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Depression and sickness behavior are Janus-faced responses to shared inflammatory pathways

BMC Medicine volume 10, Article number: 66 (2012) Cite this article

Abstract

It is of considerable translational importance whether depression is a form or a consequence of sickness behavior. Sickness behavior is a behavioral complex induced by infections and immune trauma and mediated by pro-inflammatory cytokines. It is an adaptive response that enhances recovery by conserving energy to combat acute inflammation. There are considerable phenomenological similarities between sickness behavior and depression, for example, behavioral inhibition, anorexia and weight loss, and melancholic (anhedonia), physio-somatic (fatigue, hyperalgesia, malaise), anxiety and neurocognitive symptoms. In clinical depression, however, a transition occurs to sensitization of immuno-inflammatory pathways, progressive damage by oxidative and nitrosative stress to lipids, proteins, and DNA, and autoimmune responses directed against self-epitopes. The latter mechanisms are the substrate of a neuroprogressive process, whereby multiple depressive episodes cause neural tissue damage and consequent functional and cognitive sequelae. Thus, shared immuno-inflammatory pathways underpin the physiology of sickness behavior and the pathophysiology of clinical depression explaining their partially overlapping phenomenology. Inflammation may provoke a Janus-faced response with a good, acute side, generating protective inflammation through sickness behavior and a bad, chronic side, for example, clinical depression, a lifelong disorder with positive feedback loops between (neuro)inflammation and (neuro)degenerative processes following less well defined triggers.

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Introduction

The first inkling that there are phenomenological similarities between clinical depression and sickness behavior and that both conditions may share common pathways, that is, activation of the inflammatory responses system (IRS) was published in 1993 [1, 2]. Sickness behavior is a behavioral complex that is typically induced by acute infections and tissue injury in many mammalian species. The characteristic behavioral pattern consists of malaise, hyperalgesia, pyrexia, listlessness and disinterest in social interactions with the environment, lethargy, behavioral inhibition, reduction of locomotor activity, exploration and grooming, reduction of reproductive performance, anhedonia, somnolence and sleepiness, anorexia and weight loss, failure to concentrate, and anxiety. There is evidence that sickness behavior is mediated through the effects of pro-inflammatory cytokines (PICs), such as IL-1, TNFα and IL-6 [310]. In this context, there is abundant evidence that clinical depression is an immuno-inflammatory disorder characterized by among other things increased levels of PICs and acute phase proteins, including C-reactive protein and haptoglobin [1120].

Characteristic symptoms of major depression include anorexia, weight loss, fatigue, lethargy, sleep disorders, hyperalgesia, reduction of locomotor activity, and failure to concentrate (American Psychiatric Association). Moreover, 'vegetative symptoms' of depression, such as anorexia, weight loss, and psychomotor retardation, are significantly associated with inflammatory markers in clinical depression, such as increased levels of plasma haptoglobin, an acute phase protein, synthesis of which is induced by the three abovementioned PICs [1, 2].

Thus, it may be concluded that there are striking behavioral and inflammatory similarities between both sickness behavior and clinical depression [1, 2, 11]. Therefore, some authors regard clinical depression as a form of sickness behavior and/or as a consequence of the sickness behavioral response [9]. Figure 1 shows the theory - principally derived from inflammatory translational models - that inflammatory triggers cause IRS activation and induce the production of PICs, which in turn may provoke sickness behavior and depression, thus explaining the phenomenological overlap between these conditions.

Figure 1
figure 1

Inflammation causes sickness and depression. This Figure shows the theory that acute triggers cause inflammation and increased production of pro-inflammatory cytokines (PICs), which is associated with the onset of sickness behavior and clinical depression.

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The main aims of this paper are to delineate: a) the symptomatic and behavioral similarities and dissimilarities between both clinical depression and sickness behavior; b) the staging of depression versus the course of sickness behavior; c) the shared immuno-inflammatory pathways that both underpin clinical depression and sickness behavior and may discriminate them; and d) the etiologic factors in both conditions.

The nature of sickness behavior

Inflammatory inducers, for example acute viral and bacterial infections and inflammatory trauma, are detected by sentinels (for example, receptors on the innate immune system) and activate inflammatory mediators, for example, PICs which target the immune cells in the inflamed tissues [21]. Adaptive inflammatory responses are terminated once the triggers are eliminated and damaged tissues are repaired, a phenomenon known as resolution of inflammation. As we will explain in this section PIC-induced sickness behavior plays an important role in the resolution of inflammation and increased energy demands during inflammation.

Sickness and energy consumption

Combating pathogen threats consumes large amounts of energy and, therefore, rations available energy [22]. PIC signals, for example, TNFα signals, modulate the balance between this increased energy demand and energy supply and control food intake, energy expenditure and substrate utilization [23, 24]. PICs play a key role in this highly increased energy request characterized by a negative energy balance (increased lipolysis, loss of tissue proteins and lowered muscle protein synthesis, gluconeogenesis) and decreased voluntary energy utilization [22]. The central nervous system (CNS) receives neural and humoral signals about the peripheral inflammatory response through PIC-induced activation of afferent vagal signals, effects of TNFα at the sensory nuclei of the solitary tract, and all three PICs entering the brain though different pathways [22, 25]. These PICs, in turn, will shut off energy-consuming processes, such as locomotor, neurocognitive and reproductive activity. Thus, metabolic energy is withdrawn from the brain and some peripheral organs and redirected to counteract the adverse effects of the invading pathogens. The energy saved by this process contributes to pyrexia and to the enhancement of the inflammatory state of immune cells [22]. Many of the sickness behavior symptoms, such as anergia, malaise, somnolence, psychomotor retardation, cognitive deficits and loss of libido serve to limit motor, sexual and brain activity and thereby direct metabolic energy to combating the primary infection [4, 7, 22, 26]. Immune responses are highly calorie dependent and increase resting energy expenditure, while sickness behavior responses, for example, motor inhibition, may conserve critical energy [27].

Sickness behavior and pyrexia

Mild to moderate pyrexia (in contrast to high fever) is a positive adaptive response as it strengthens the host defenses and resistance to infection, for example, by enhancing the phagocytosis and mobility of polymorphonuclear leukocytes and killing of bacteria and preventing viral replication [2830]. In addition, PICs and cytokines, such as IFNs are more active during fever [31]. The relative balance of pyrogenic IL-1 and non-pyrogenic IL-18, and their endogenous inhibitory factors in different CNS sites, may contribute to the presence and degree of pyrexia [32]. In the past, fevers were even induced in patients to combat infections.

Sickness behavior and anorexia and weight loss

Inflammation-induced anorexia is directly proportional to the magnitude of the insult and is also inversely related to body weight prior to the insult [33]. It is suggested that anorexia may limit the intake of iron, which otherwise would activate bacterial production [34]. Iron is one of the nutrients employed by bacteria for bacterial growth. This reasoning is, however, highly speculative as only less than 1% of dietary iron is absorbed and iron status changes slowly over time. A more plausible adaptive function is that anorexia through calorie restriction attenuates different intracellular signaling pathways leading to inflammation and even sickness behavior [35, 36]. Thus, a two-week calorie restriction period significantly reduces inflammatory pathways, including IL-6 [37]. Calorie-restriction results in a dose-dependent suppression of lipopolysaccharide (LPS)-induced sickness behavior by inducing an anti-inflammatory state [36]. Motor inhibition and anorexia can lead to lean body mass loss, increased protein catabolism and loss of body protein and fat mass, which together may explain inflammation-induced weight loss and eventually cachexia. In the short-term, weight reduction, but not the composition of the diet, attenuates the inflammatory response, for example, by lowering inflammatory PICs, such as IL-6 and TNF [3840] and increasing plasma levels of adiponectin, an adipose-derived anti-inflammatory protein [41].

Figure 2 shows the different functions of acute inflammation-induced sickness behavior. Thus, sickness behavior is a short-term response to acute inflammatory triggers and is an adaptive motivational state induced to cope with these triggers and the consequent negative energy balance [4, 7]. This homeostatic adaptive behavioral response is conserved across species through evolution and occurs in a predictable form cross-culturally [26].

Figure 2
figure 2

This figure shows the functions of acute inflammation-induced sickness behavior: a) energy saving by protecting the organism from the energy consuming effects of inflammation (through somnolence, lethargy, sleepiness, hyperalgesia, reduction of motor activity, exploration and grooming, cognitive deficits, loss of libido, anhedonia, disinterest in social interactions with the environment, and anxiety); b) anti-inflammatory effects (through anorexia, weight loss); and c) pathogen-directed effects (through pyrexia).

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Symptomatic/behavioral similarities and dissimilarities between depression and sickness behavior

The Diagnostic and Statistical Manual of Mental Disorders (DSM IV-TR, American Psychiatric Association), one of the most commonly used diagnostic systems for psychiatric disorders, considers that the diagnosis of clinical depression can be made when at least five out of nine basic symptoms sare present for at least two weeks. Table 1 lists these nine basic symptoms and also three partially overlapping symptom dimensions that may superimpose on these basic symptoms, that is: 1) melancholic; 2) anxiety; and 3) physio-somatic dimensions [15]. It should be stressed that multivariate statistical analyses (pattern recognition methods) have confirmed and validated the basic symptoms of clinical depression and also the three symptom dimensions [4244]. These three dimensions delineate specific depressive subgroups, for example, depression with melancholic, anxiety or physio-somatic features, which were externally validated by biomarkers.

Table 1 Characteristics of depression and sickness behavior.
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Table 1 compares the symptoms of clinical depression with the characteristics of sickness behavior. Basic symptoms/behaviors of clinical depression are also observed in sickness behavior, for example, anorexia, weight loss, reduction of locomotor activity and exploration, fatigue, sleepiness, and failure to concentrate. Moreover, symptoms belonging to the three dimensions, for example, melancholia (a failure to react to pleasurable stimuli, and excessive psychomotor retardation and weight loss) anxiety, and physio-somatic symptoms (malaise and hyperalgesia) also occur during sickness behavior. An apparent difference between depression and sickness behavior is pyrexia. There are, however, some reports that major depressed patients have increased body temperature as compared to normal volunteers, that is 98.38 ± 0.61 degrees F versus 98.13 ± 0.59 degrees F, respectively (mean ± SD) (that is, 36.88°C versus 36.74°C [45]. Increased body temperature in clinical depression is also shown by Szuba et al. [46]. However, there is by no means conclusive evidence of significant pyrexia in patients with clinical depression.

Obvious differences are suicidal ideation, feelings of guilt and worthlessness, symptoms indicating a distinctive existential state of depression [26]. In this context, it is important to note that Charlton proposed the malaise theory of depression, that is, malaise, the key symptom of sickness behavior, should be considered the core 'emotion' of depression. Indeed, a flu-like malaise or the subjective feeling of infection together with other physio-somatic symptoms is an important symptom dimension in clinical depression [44]. The malaise theory regards lowered mood and the more distinctive existential state of depression as a product of malaise. Thus, humans who suffer from sickness behavior and do not know they are ill, may interpret their lack of energy and neurocognitive disorders as a personal failure, causing feelings of guilt and unworthiness [26]. By inference, this theory considers depression not primary as an affective disorder but as a somatic disorder related to sickness behavior. Nevertheless, multivariate statistical analyses show that only some depressed patients suffer from physio-somatic symptoms, including malaise [44]. These findings contrast with the view that malaise is a core emotion of depression.

Staging of depression versus the course of sickness behavior

Although some patients may suffer from one depressive episode only, longitudinal studies performed within the last two decades have shown that clinical depression is typically an episodic or lifelong disease [4749]. Although depression was classically considered to be a self-limiting disorder with a short duration (six to nine months), the course of depression varies considerably. It may take the form of prolonged episodes (chronic depression), and depressive episodes may frequently return (recurrent depression). Moreover, up to 15% of depressed patients may develop treatment resistance, defined as a failure to respond to at least two adequate antidepressant trials [50]. A subgroup of depressed patients additionally suffer from hypomanic or manic episodes (bipolar depression), including abnormally elevated mood, energy and cognition; or from a mixed state with depressive and (hypo)manic symptoms occurring together. It should be underscored that the brain is one of the most metabolically active tissues, and energy and mood are intertwined. Depression is linked to reductions in brain energy generation and mania to increased energy expenditure [51], while sickness behavior is a behavioral response, which conserves energy.

Both unipolar and bipolar depression have characteristics of a progressive illness: they both follow stages, often commencing with mild or non-specific symptoms, progressing to prodromal features of subthreshold symptoms, then an acute episode, recurrence or a chronic form of persistent, unremitting illness [16, 17, 48]. An earlier onset of depression and increased length and number of episodes are associated with increased vulnerability to further relapses and a less favorable outcome [16, 17, 52]. This progressive course is associated with a functional deterioration, including neurocognitive decline [53, 54]. This 'waxing and waning' pattern is similarly characteristic of autoimmune, progressive or degenerative disorders that combine an insidious onset with recurrent episodes or a chronic course and increased risk for functional deficits [11]. Moreover, there is evidence that sensitization offers a model for episode recurrence [55]. Sensitization indicates that repeated exposure to stressors, either psychological or organic, causes time-dependent, progressive increases in susceptibility to re-exposure to any of these stressors [56, 57]. McEwen's allostatic load model has similarly been adapted to describe this progressive pattern [58]. Moreover, a seasonal variation is often found in unipolar and bipolar depression and depressive subgroups, including postpartum depression, with, for example, peak occurrences in spring [59, 60]. There is also a seasonal variation in severity of depression and depressive symptoms, including suicide [61].

In contrast, sickness behavior is an acute, short-term state most often with an acute onset that is biologically appropriate to combat acute infections/trauma and thus enhances recovery. Evidently, (hypo)manic symptoms, the progressive deterioration over time, and seasonal variation are not characteristics of sickness behavior. Sickness behavior may be prolonged or inappropriately activated. Such a prolonged sickness behavior complex is likely to be dysfunctional [26] as is the case in more chronic infections and (auto)immune disorders. Motor and activity deficits are typically associated with sickness behavior [62, 63] and form part of the fatigue - depression - sleep disorder cluster occurring during acute and chronic illnesses including heart disease, rheumatoid arthritis, and cancer [64]. In some individuals these symptoms can persist years after hospitalization, for example, post ICU and post-administration of radioactive substances. The question arises as to whether this condition should be regarded as sickness behavior given it is no longer beneficial? The following sections will address this question.

Pathways underpinning clinical depression and sickness behavior

Inflammation and cell-mediated immunity

Studies in humans and rodents have defined PICs as central mediators of sickness behavior [5, 6, 6567]. Inflammatory triggers induce 'neuraxes', that is, ascending neural pathways, which convey information about metabolic, gastro-intestinal and cardiovascular challenges to brain regions that mediate stress-related behaviors [68, 69]. For example, infection and immune activation activate bottom-up, inflammatory pathways, mediated by PICs, from the periphery to the dorsal vagal complex, and ventrolateral medulla of the caudal medulla [9, 7072]. These inflammatory challenges to internal bodily functions are translated into the brain via viscerosensory pathways that subsequently drive sickness behavior, and depressive- and anxiety-like behaviors [72]. Moreover, PICs are actively transported to the brain by endothelial cell transporters or may diffuse through blood-brain-barrier deficient areas [25, 72]. This may explain why systemic inflammation provokes neuroinflammation and microglial activation. For example, administration of LPS, a component of the bacterial wall of gram negative bacteria, causes neuroinflammation and microglial activation, characterized by increased levels of TNFα, which may remain elevated for months and are associated with the onset of sickness behavior [8]. Moreover, the same pathways may activate brain regions, for example, the bed nucleus of the stria terminalis, that mediate threat-related information and infection-induced anxiety [71, 7375]. Studies investigating the mechanisms of these behavioral deficits in acute illness models have shown that peripheral inflammation leads to activation of a 'danger pathway' that originates in the caudal brainstem and signals the presence of physiological stressors to regulatory brain regions including the hypothalamus. Activation of this danger pathway leads to the suppression of hypothalamic arousal systems, notably the tuberomammillary histaminergic system, associated with behavioral activity [68]. When activation of the danger pathway is prevented, motor aspects of sickness behavior are absent following acute inflammatory challenge [69]. Thus, reduction in behavior associated with sickness is concomitant with an active inhibition of arousal systems [76]. The danger pathway also provides input to other brainstem areas involved in the regulation of arousal including the serotonergic dorsal raphe nucleus [68, 69], and in this way may serve as a link between peripheral inflammation and brain functions regulating and/or influenced by alterations in arousal states.

As reviewed previously, clinical depression and sickness behavior share the involvement of key pathways, the predominant one being the role of inflammation [15]. In clinical depression there is evidence of a chronic, low grade inflammatory process and cell-mediated immune (CMI) activation characterized by a T helper (Th1)-like response with activation of IFNγ-related pathways [77, 78]. Recent meta-analyses and recent publications have confirmed increased levels of PICs in human depression particularly IL-6, TNFα, and IL-1, and CMI activation, evidenced by higher levels of neopterin and soluble IL-2 receptors (sIL-2Rs) [1820, 79, 80]. Increased neopterin is a marker of increased IFNγ mediated macrophage activation. In humans, IFNα-based immunotherapy induces physio-somatic and depressive symptoms in many patients with hepatitis C virus. The onset of depressive symptoms during IFNα-based immunotherapy is strongly associated with induction of the cytokine network, including elevations in monocytic cytokines, Th-1-like and Th-2-like cytokines [18, 81, 82].

Elevated PICs and CMI cytokines are capable of producing depressive symptoms and administration of cytokines provides a robust experimental model of the acute phase of depression. Studies in the rodent [15] provide strong evidence that PICs, for example IL-1, IL-6, and TNFα, and CMI cytokines, for example IL-2 and IFNγ, all at around 50 μg/kg, may induce: a) sickness behavior; b) depressive-like symptoms (including loss of motivated behavior, reduction of social investigation, anorexia, weight loss, decreased spontaneous locomotor activity, increased locomotion, memory impairment, impaired spatial memory, and enhancement of the amnesic effect of scopolamine); c) melancholic symptoms (including anhedonia as indicated by reduced preference for a solution of sucrose or chocolate milk in comparison to water, and changes in the circadian clock through effects at the suprachiasmatic nucleus); d) anxiety (including anxiogenic effects in the elevated plus maze and elevation of conditioned fear memory); and e) physio-somatic symptoms (including fatigue, hyperalgesia, and autonomic symptoms). Administration of LPS elicits not only sickness behavior but also depressive- (suppression of social interaction and activity in the open-field test, food consumption and body weight, memory dysfunction), anxiety-like and physio-somatic behaviors [15]. Cytokines such as IL-1 not only have potent primary signaling effects, but also modulate many neurotransmitters intimately involved in mood regulation such as serotonin and noradrenaline [83]. Recently, the inflammatory processes were linked with the neurocircuitry hypothesis of depression [84]. Thus, PICs modulate cortical-striatal-limbic circuits, which process reward-based and affective information and are responsible for core depressive symptoms [84].

Certainly, it is difficult to determine whether the depressogenic and anxiogenic effects of LPS and other inflammatory triggers are genuine or related to sickness behavior [85]. Since cytokine- and LPS-based models are accompanied by depressive-like and sickness behaviors it was often difficult to delineate which of these models are characteristic for acute depressive-like behaviors or for sickness behavior. Nevertheless, some groups have apparently separated initial sickness behavior from depressive-like behaviors. Dissociation between LPS-induced depressive-like behaviors and sickness behavior could be established by testing mice at different time points following administration of LPS [86]. Lacosta et al. (1999) [87] showed that systemic administration of IL-2 to mice induces reductions in exploration and impaired performance in the Morris water-maze that are not related to sickness behavior. Administration of intracerebroventricular (icv) IL-1β induces a sickness behavioral response (as indicated by reduced locomotor activity, lethargy, and reduced body weight) and a stress- or anxiety-like response [88].

Activation of the IRS is controlled at different levels whereby regulatory mechanisms specifically target selected control points, such as the production of pro-inflammatory mediators or the effects of mediators on the target tissues [21, 89]. This regulation of the IRS response is an adapted compartmentalized regulatory response characterized by reflex inhibition that tends to silence an overzealous IRS [90]. Examples of inflammatory reflex inhibition are inflammation-induced increases in IL-10, a negative immunoregulatory cytokine, and transforming growth factor (TGF)β, an antiproliferative factor [21]. PIC-induced changes in neural pathways also participate in inhibiting acute inflammation, for example, enhanced production of glucocorticoids and catecholamines, and activation of cholinergic pathways [91]. For example, counter regulatory mechanisms are initiated to limit an infectious (sepsis) and non-infectious systemic inflammatory response syndrome [90, 92, 93]. This counter anti-inflammatory response syndrome is an adaptive response of the immune status that dampens an overzealous inflammatory response caused by pathogens or immune trauma [90, 92, 93].

The existence of comparable counter regulatory processes, in particular reflex inhibition, has been described in clinical depression [11, 78]: increased synthesis of the IL-1 receptor antagonist (IL-1RA), which inhibits the function of IL-1; PIC-induced activation of the cortisol-axis and the consequent immunosuppressive activities of glucocorticoids; increased IL-6 production, which is protective by increasing the production of IL-10, IL-1RA and glucocorticoids; increased IL-2R levels which induce a state of IL-2 starvation by binding their ligand and limiting the amount of IL-2 needed for immune cell proliferation; increased production of some acute phase proteins, for example, haptoglobin, which act as immunosuppressive factors; increased prostaglandin production, which may suppress lymphoproliferative responses; and lowered plasma tryptophan levels (see next section). These counter anti-inflammatory response syndrome mechanisms may explain why the immune-inflammatory response in clinical depression is accompanied by signs of immunosuppression, such as decreased ex vivo natural killer cell activity and mitogen-induced lymphoproliferative disorders [11]. In analogy with the term counter anti-inflammatory response syndrome, which is typically coined as a counter-regulatory response to sepsis/systemic inflammatory response syndrome, we would propose to label this compensatory reflex system as 'compensatory (anti)inflammatory reflex system' (CIRS).

Sickness behavior supports the protective inflammatory response (helps to eradicate the trigger and redirects energy to inflammatory cells), protects against possible detrimental effects of inflammation (for example, negative energy balance), while at the same time acting as an anti-inflammatory reflex (anti-inflammatory effects of calorie restriction and weight loss). Therefore, sickness behavior itself should be regarded as a CIRS response to acute inflammation. Thus, while clinical depression is accompanied by a CIRS that downregulates the immuno-inflammatory response, sickness behavior is part of a CIRS.

The TRYCAT (tryptophan catabolite) pathway

Recently, a new pathway associated with inflammation has been established in some individuals with depression, that is, activation of the tryptophan catabolite (TRYCAT) pathway [9497]. The first and rate-limiting enzyme of this pathway is indoleamine 2,3-dioxygenase (IDO; EC 1.13.11.52) [98]. IDO is activated by IFNγ and by PICs, such as IL-1 and TNFα, thereby inducing the catabolism of tryptophan leading to tryptophan depletion and increased synthesis of TRYCATs, for example, kynurenine, kynurenic acid, xanthurenic acid, and quinolinic acid. IDO is expressed in many organs, for example, kidney, lung, spleen, and duodenum, immune cells, and the brain, for example, astroglia and microglia [99, 100]. Lowered plasma tryptophan frequently occurs in clinical depression and is strongly associated with biomarkers of inflammation (acute phase reactants, increased cytokine levels) and CMI activation (increased serum neopterin and sIL-2Rs) [9496]. During IFNα-based immunotherapy the onset of depressive symptoms is strongly associated with IDO activation, as assessed by means of the kynurenine/tryptophan ratio [101]. Likewise, in the postnatal period lowered tryptophan and increased IDO activity are related to anxiety and depressive symptoms [102]. Acute tryptophan depletion causes a robust increase in depressive symptoms in vulnerable individuals [103].

Recent studies have shown that IDO activation may separate sickness behavior and depressive-like behaviors in the rodent [104]. Thus, in Wild type (WT) mice, inoculation with bacille Calmette-Guérin (BCG), an attenuated form of Mycobacterium bovis, elicits IDO activation and consequent elevations in PICs and CMI-cytokines, such as IFNγ, IL-1β and TNFα [104]. Inoculation with BCG caused an initial acute episode of sickness behavior that was followed by a chronic state of depressive-like symptoms starting one week after BCG administration. Sickness behavior was equally induced in WT and IFNγR(-/-) mice, whereas IFNγ and TNFα together are necessary to cause IDO activation in microglia and consequent depressive-like behaviors. Moreover, IDO-deficient mice are resistant to the depressogenic effects of BCG, while they show a normal inflammatory response following BCG administration [104].

These TRYCAT data obtained in animal experiments are, however, difficult to extrapolate to clinical depression, because the clinical results are controversial. Thus, initial research showed no changes in urinary excretion of TRYCATs, such as xanthurenic acid and kynurenine, after tryptophan loading in depressed patients [105108]. Nevertheless, higher xanthurenic excretion rates were related to anxiety and a lowered availability of plasma tryptophan [105, 108]. The latter findings show that a 'TRYCAT shunt' through activation of IDO lowered plasma tryptophan in individuals with depression. In a recent study [109], lower levels of kynurenic acid and consequently a relatively increased kynurenine/kynurenic acid ratio were observed in depression. This ratio might be important for the pathophysiology of depression as kynurenine and some of its catabolites, for example, quinolinic acid, are depressogenic, anxiogenic, excitotoxic and neurotoxic, whereas kynurenic acid is neuroprotective [96]. One study shows increased TRYCATs in adolescents with melancholic depression [110] and another study increased quinolinic acid in microglia of depressed suicide victims [111]. Sublette et al. [112] detected increased plasma kynurenine levels in suicide attempters with major depression. Recent data shows that aberrations in the TRYCAT pathway, classically seen as a hallmark of depression, may be more germane to somatization, suggesting that the classically labeled psychosomatic symptoms of somatization may be more appropriately termed physio-somatic symptoms [113]. Thus, in a study comparing depression, comorbid depression + somatization, somatization alone, and controls, plasma tryptophan was even lower in somatization than in depression, while the kynurenine/kynurenic acid ratio and the kynurenine/tryptophan ratio were significantly higher in patients with somatization than depression [113]. Plasma tryptophan was negatively, and both ratios were positively, correlated with severity of physio-somatic symptoms. In summary, although in acute inflammatory states (for example, during IFNα-based immunotherapy) IDO activation is strongly related to the onset of depressive-like behaviors, this appears not to be the case in clinical depression since only some of those individuals, that is, those with physio-somatic symptoms or suicidal behavior, show relative increases in TRYCAT levels.

IDO activation has protective CIRS functions: IDO-induced reductions in plasma tryptophan and increased TRYCAT formation may attenuate the primary immuno-inflammatory response, for example, by attenuating T cell activation and proliferation [11, 15]. This reflex inhibition could, therefore, be involved in spontaneous remissions of clinical depression, consistent with the observation that depression is sometimes a self-limiting disorder [96]. This CIRS mechanisms may also explain the contradictory findings on the TRYCAT pathway in acute depressive states (for example, IFNα-induced depression where there is a strong association between TRYCAT aberrations and the onset of depression) and major depression (DSM-IV-TR criteria), where these associations are much weaker probably because lowered tryptophan and increased TRYCATs have attenuated the initial immune-inflammatory response. Nevertheless, increased levels of TRYCATs, for example, quinolinic acid, in the anterior cingulate gyrus may be detrimental and play a role in clinical depression.

Detrimental immuno-inflammatory pathways that discriminate depression from sickness behavior

Although there is some evidence that shared immuno-inflammatory pathways may underpin sickness behavior and clinical depression, they have divergent effects in both conditions. Thus, the inflammatory response in sickness behavior has a beneficial CIRS effect on the organism, whereas inflammatory pathways and their sequelae have detrimental effects in depression and in particular in recurrent and chronic depression.

Transition to sensitization and autoimmunity

There is evidence that immuno-inflammatory responses are sensitized by recurrent depressive episodes. Thus, neopterin, a biomarker of CMI activation, is significantly increased in depressed patients who have experienced two or more depressive episodes than in patients who suffered only one depressive episode [18, 114]. Likewise, plasma IL-1 and TNFα are significantly increased in depressed patients who suffered from three or more depressive episodes [18]. Women with a lifetime history of depression have increased inflammatory biomarkers, including IL-6 and sIL-1RA, in the early puerperium as compared to women who have never suffered from depression [115]. Increased C-reactive protein (CRP) levels in depressed men predict not only severity of the current depressive episode, but also recurrent depression [116]. It is known that PICs mediate central sensitization, for example, behavioral responses to maternal separation [117, 118]. This suggests that recurrent depressive episodes amplify the pathophysiological responses of depressogenic cytokines, potentially enhancing inflammation-induced behavioral responses. Since it is known that increased numbers of episodes increase the risk of recurrence and treatment resistance [17], the findings suggest that sensitization of immuno-inflammatory pathways increases vulnerability to develop new depressive episodes.

Immuno-inflammatory mechanisms may also explain the high degree of anti-5-hydroxytryptamine (5-HT) antibody activity in clinical depression (54.1%), and in melancholia (82.9%) as compared to normal controls (5.7%) [119]. This autoimmune activity directed against 5-HT is significantly associated with biomarkers of inflammation (increased IL-1 and TNFα) and CMI activation (increased neopterin). In this respect, administration of pro-inflammatory and CMI-related stimuli, including LPS, IFNγ, and TNFα, reduces the survival of 5-HT neurons in the dorsal raphe nucleus, an effect that is not related to IDO activation [120]. The autoimmune activity directed against 5-HT is additionally associated with the number of previous depressive episodes, suggesting that exposure to previous depressive episodes increases anti-5-HT antibody activity, which, in turn, could confer increased risk to develop new depressive episodes.

Moreover, increased IL-6 and TNFα and lower serum zinc levels are associated with risk for depression and treatment-resistant depression [121125]. This suggests that the immuno-inflammatory response in clinical depression may confer increased risk towards treatment resistance [126]. There is also evidence that immuno-inflammatory processes underpin the pathophysiology not only of unipolar and bipolar depression, but also mania [127, 128]. Acute mania is accompanied by increased sIL-6R and sIL-2R levels, and increases in acute phase reactants [127, 128], increased sCD4, sCD8, and sIL-1R antagonist levels [129], and elevated total immunoglobulin (Ig) G1, complement proteins C3, C6 and factor B [130]. Recently, it was argued that immuno-inflammatory processes play a role in the progressive shortening of the inter-episode interval with each recurrence when bipolar depression progresses [16, 17]. All in all, the aforementioned findings suggest that sensitization (kindling) and progression of depression and bipolar disorder are, in part, caused by progressive inflammatory, CMI and autoimmune responses.

Transition to damage by O&NS processes

As with many inflammatory conditions, clinical depression is accompanied by activation of oxidative and nitrosative stress (O&NS) pathways [131]. The latter are likely amplified by reduced antioxidant levels, for example, coenzyme Q10, zinc and glutathione, and by the immuno-inflammatory responses in depression, perpetuating a vicious cycle between reduced antioxidants, inflammation and activated O&NS pathways [131]. There are no reports whether O&NS pathways play a role in adaptive sickness behavior. Nevertheless, these pathways have detrimental effects in clinical depression and additionally play a role in chronic depression. There is abundant evidence that depression is characterized not only by increased reactive oxygen and nitrogen species (ROS/RNS), but also by O&NS damage to lipids, proteins, DNA, and mitochondria [131]. In these processes O&NS pathways may alter the chemical structure of membrane fatty acids and functional proteins. When these modified fatty acids and proteins become immunogenic, an autoimmune response may be mounted directed against these 'neoepitopes' thereby further damaging the function or chemical structure of these epitopes [132, 133]. Many depressed patients show increased IgM-mediated autoimmune responses directed against neoepitopes, such as the three anchorage molecules, palmitic and myristic acid and L-farnesyl S-cysteine, as well as acetylcholine, phosphatidylinositol, oleic acid, and NO-adducts, including NO-tryptophan and NO-tyrosine [133]. These autoimmune responses may interfere with cellular functions including intracellular signaling, apoptosis, and cellular differentiation. For example, the autoimmune reactions directed against the anchorage molecules may interfere with palmitoylation, myristoylation and farnesylation, and, therefore, with the binding and function of hundreds of proteins to the membrane [133]. Some of these IgM-mediated autoimmune responses are significantly higher in chronically depressed patients than in non-chronically depressed patients, suggesting that this O&NS damage may increase risk to develop chronic depression for example by activating neuroprogressive pathways [16, 17, 52, 133]. These O&NS-related processes together with the effects of inflammatory mediators at 5-HT neurons [120] may explain the transition from inflammation and CMI activation to damage by O&NS and autoimmune reactions, which both may aggravate the preexisting inflammation and are involved in the process of chronic depression.

Transition to neuroprogression

Another immuno-inflammation-related pathway, which has detrimental effects in clinical depression and is not germane in sickness behavior, is neuroprogression, that is the stage related and potentially progressive process of neurodegeneration, reduced neurogenesis and neuronal plasticity, and apoptosis [15, 17, 123, 126, 134137]. Many, but not all depressed individuals show features suggestive of a neuroprogressive illness. As discussed above, people who have a longer duration of illness and suffered from more frequent depressive episodes have a greater risk to develop subsequent relapses. Treatment response appears to reduce with more recurrent mood episodes [15, 17, 52]. Recurrent depressive episodes are correlated with increased cognitive disabilities, for example, decreased memory performance which is lowered by 2% to 3% following each depressive episode [138]. Depressive episodes are additionally associated with an increased risk of dementia [54]. Likewise, more depressive episodes are associated with underlying brain alterations, for example, reductions in volume of orbitofrontal and subgenual prefrontal cortex, hippocampus, and basal ganglia [52]. The duration of illness, for example, is negatively correlated with the volume of cerebral grey matter [139]. Meta-analysis showed that in patients with chronic depression (> 2 years) or recurrent depression hippocampal volume is significantly decreased and that the latter is related to the number of episodes [140, 141]. In some studies, decreased hippocampal volumes in patients with recurrent depression are associated with neurocognitive decline [142]. Treatment resistance and the duration of illness are related to decreased right caudate and left putamen volume [52, 143]. This effect may in part be related to a decrease in soma size of some cell types [144]. There is also evidence that in depression the abovementioned neuroprogression is at least partially caused by inflammatory and O&NS pathways [15, 17, 126]. PICs, such as IL-1 and TNFα, and CMI cytokines, for example, IFNγ and IL-2, TRYCATs, such as quinolinic acid, and damage by O&NS to structural fatty acids, anchorage molecules, functional proteins, DNA and mitochondria all may contribute to neuroprogression [15, 17, 126]. Further, both immune challenge and depression influence a constellation of brain regions that process viscerosensory and regulation of emotion in humans [145147] and rodents [148]. These regions include parts of the medial prefrontal cortex (anterior cingulate) and basal forebrain (nucleus accumbens). Intriguingly, the CIRS seems to weaken with progression of the illness, and this failure to dampen inflammatory activation might play a role in the process of neuroprogression seen with multiple episodes [149].

All in all, the abovementioned findings show that clinical depression is accompanied by chronic inflammatory and O&NS responses and/or its sequelae, including sensitization, autoimmunity, damage by O&NS and neuroprogression. As a consequence, the inflammatory experiments described in the previous sections do not provide mechanistic explanations as to how PICs and CMI cytokines cause progressive clinical depression, as defined by its progressive course and progressive immuno-inflammatory pathophysiology. These experiments nevertheless support the view that PICs and CMI cytokines are associated with the onset of depressive-like behaviors and the physio-somatic, melancholic, and anxiety symptomatic clusters. However, most of these LPS- and cytokine-induced models did not separate sickness behavior from depression. In addition, these experiments are very limited because they select only one or two aspects of the symptom dimensions of depression, for example, reduced intake of sweetened milk as a model for anhedonia and thus melancholia [150]. More adequate animal models of clinical depression should be constructed to model not only the symptomatic dimensions, but also the typical course (self-limiting versus waxing and waning or progressive course) and the progressive pathophysiology (with sensitization and a transition to oxidative damage, autoimmunity and neuroprogression) of clinical depression.

Etiologic factors in depression and sickness behavior

Etiologically, sickness behavior is conceptualized as an acute phase of adaptive CIRS behavior in response to acute infections and inflammatory trauma [4, 7, 26]. When the resolution phase, however, is not induced, for example, when the IRS was unable to eradicate the pathogen, inflammation may persist despite the CIRS thus causing a chronic inflammatory state [21]. Chronic inflammation may result from a failure to eradicate the acute inflammatory trigger (for example, pyogenic bacteria), innately chronic irritants (for example, fungi, sarcoidosis), or autoimmune responses [151]. Acute and chronic inflammation are distinguished in terms of immune response patterns and time course. The time point of transition of acute inflammation to chronic inflammation is also related to the time when the energy stores become empty and this is estimated to be around 19 to 43 days depending on the nature of the energy store [152]. This transition is related to a number of inflammatory sequelae, including cachexia, insulin resistance, anemia, osteopenia and hypertension [152]. Sickness behavior thus plays a critical role in preventing the transition from acute to chronic inflammation following an acute trigger by compensating for the negative energy balance, redirecting energy to the activated immune cells, and so on [152]. Clinical depression, on the other hand, is accompanied by chronic inflammatory processes and is associated with less well defined trigger factors, as will be explained in this section.

In many chronic disorders, including degenerative (for example, diabetes, atherosclerosis) and neurodegenerative (for example, Parkinson's disorder) disorders the initiating trigger is not well defined, while the chronic state appears to consist of positive feedback loops connecting chronic inflammation and its pathophysiological process [21]. For example, Parkinson's disease (PD) is characterized by a vicious cycle between microglial activation and dopaminergic neuron degeneration, caused by detrimental effects of PICs, O&NS, and so on [25]. A similar pattern is observed in clinical depression: a chronic inflammatory process appears to be associated with transition to progressive autoimmune and neuroprogressive processes.

In contrast to sickness behavior, pathogens do not play a major role in clinical depression although some authors have attempted to make links between pathogens such as herpes simplex type 2 and toxoplasma gondii and psychopathology [153, 154]. In a previous review, we concluded that there is no good quality evidence that acute infections and infections with Epstein-Barr Virus (EBV) may act as trigger factors associated with the onset of clinical depression [155]. Only some types of chronic infection are frequently associated with clinical depression, for example, HIV infection [156] and increased translocation of gram negative bacteria [157]. Some chronic infections, such as Lyme's disease can cause prominent neuropsychiatric sequelae [158, 159]. Thus, while sickness behavior is an adaptive CIRS response to acute infections, only a few chronic pathogenic conditions appear to be associated with the onset of clinical depression. However, it cannot be excluded that reactivated dormant infected states and consequent infection-induced molecular pathways may be important in clinical depression. Viral infections of the brain, for example, cause neurologic and psychiatric dysfunction more often than appreciated [160].

Multiple trigger factors may provoke depressive behaviors, for example, psychosocial stressors, various medical disorders, and conditions as different as hemodialysis, IFNα-based immunotherapy, and the postnatal period [25, 65, 80]. Psychosocial stressors in humans may induce inflammatory, Th1-like and O&NS responses, including lipid peroxidation and DNA damage, while in the rodent different types of stressors induce peripheral and central activation of inflammatory, O&NS and neuroprogressive pathways [25, 65, 80, 161]. For example, in the rodent, social defeat stress increases the reactivity of microglia to LPS, suggesting a role for social stress factors in the regulation of microglia responses [162]. Therefore, it may be concluded that psycho-traumatic and psychosocial stressors may cause depression and depressive-like behaviors through activation of immuno-inflammatory, O&NS and neuroprogressive pathways.

Many different medical disorders and conditions, which are associated with immuno-inflammatory and O&NS pathways, show a high comorbidity with depression: a) medical disorders, such as chronic obstructive pulmonary disease (COPD), cardiovascular disorder (CVD), chronic fatigue syndrome, obesity and the metabolic syndrome, rheumatoid arthritis (RA), systemic lupus erythematosus (SLE), inflammatory bowel disease (IBD), psoriasis, osteoporosis, and diabetes type 1 and 2; b) neurodegenerative or neuroinflammatory disorders, such as Alzheimer's (AD), PD and Huntington's disease, multiple sclerosis (MS) and stroke; and c) conditions, such as hemodialysis, IFNα-based immunotherapy, and the postnatal period [25, 163]. We have argued that these disorders/conditions are all accompanied by activation of immuno-inflammatory and O&NS pathways and therefore may cause the basic immune/inflammatory state which may lead to comorbid depression [25]. Likewise, the same pathways could induce sickness behavior, which is experienced as feeling unwell, aches and pains, fatigue, and so on. However, while sickness behavior, per definition, is an adaptive response, comorbid depression worsens the aforementioned medical conditions [25]. Concomitant depression lowers the quality of life and increases disability and mortality in individuals with COPD, CVD, RA, SLE, IBD, psoriasis and diabetes type 1 and 2. Comorbid depression also contributes to lowered quality of life in individuals with MS, PD, AD, and stroke, negatively influences recovery from neurological defects, and predicts a higher morbidity and mortality in individuals with those neurological disorders. These negative effects of comorbid depression may be explained by increases in (neuro)inflammatory burden, including TRYCAT production, damage by O&NS, transition to autoimmunity and neuroprogression, which all together may drive the (neuro)inflammatory progression of the abovementioned medical conditions. During IFNα-based immunotherapy the incidence of depression was highest on the 12th week of treatment, when more than 20% of patients with Hepatitis C Virus had moderate/severe depressive symptoms [164]. Physio-somatic symptoms, including fatigue, increased in the first week of treatment, and predicted cognitive-depressive symptoms some weeks to months later [165]. Thus, IFNα-based immunotherapy is probably one of the only trigger factors of depression that is characterized by transition from an acute inflammatory state (accompanied by sickness behavior) to a chronic inflammatory state (accompanied by depression).

Another factor that discriminates sickness behavior from depression is that the former is a response to a specific immune trigger, whereas the association between depressogenic triggers and depression is not always present. For example, as depressed people suffer from recurrent depressive episodes, it is less likely that stressful triggers are required to manifest depression. Following more than nine previous episodes, the trigger - depression association is muted and episodes appear autonomously, disconnected from triggers [166]. Also this effect may be explained by the knowledge that depression is a progressive disorder and that depressive episodes become sensitized [17].

The above suggests that chronic animal models such as the chronic mild stress and olfactory bulbectomized rat model are superior to the acute cytokine or LPS-induced models in that they: a) are less 'contaminated' with sickness behavior; and b) more accurately represent the psychosocial etiology, and/or (neuro)inflammatory and (neuro)progressive pathophysiology of clinical depression. Thus, the chronic mild stress model in the rodent shows that psychosocial triggers may cause depression-like behaviors in association with systemic and central inflammation and neuroprogression including decreased neurogenesis and neuronal cell damage [65]. The chronic mild stress model also mediates some of its effects from the differential regulation of the TRYCATs in different parts of the CNS [167]. A differential increase in quinolinic acid in the amygdala and striatum, with a trend increase in kynurenic acid in the frontal cortex following chronic mild stress would suggest an important role for variable TRYCAT pathway activation in mediating the changes associated with more psychosocial type stressors. Such differential TRYCAT pathway activation in different areas in the CNS may be relevant in differentiating sickness behaviors from clinical depression. Also, the olfactory bulbectomized rodent model of depression reflects the (neuro)inflammatory and neuroprogressive phenomena observed in clinical depression [66, 67, 168, 169].

Is prolonged, exaggerated or maladaptive sickness behavior depression?

There is recent literature describing new concepts, such as prolonged, exaggerated and maladaptive sickness behavior [170, 171]. In translational models, exaggerated inflammatory and neuro-immune responses are associated with so-called 'prolonge'" sickness behavior, including memory deficits. Such an exaggerated response is observed in aged as compared to adult mice [170]. This age-dependent prolonged sickness behavior is accompanied by oxidative damage to mitochondrial DNA (mtDNA) in microglia, increased intracellular ROS and activation of nuclear factor kappa B [170]. Subchronic administration of IL-1β significantly impairs spatial and learning memory, which is correlated with dysfunction of neurotrophins and their receptors [172]. Furthermore, the release of neurotransmitters, including acetylcholine, was significantly lower during memory retrieval. In hippocampal neurons, IL-1β administration significantly induced cell apoptosis, reduced αa-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptors, but increased N-methyl-D-aspartate receptor changes similar to those observed in AD [173]. It thus seems unlikely that depression is a maladaptive syndrome that results from prolonged 'sickness behavior' but rather the consequence of a chronic underlying immuno-inflammatory and degenerative process. These findings also show that there was no resolution to acutely triggered inflammation and consequently that transition towards chronic inflammatory pathology had occurred. By inference, this condition cannot be termed 'prolonged' sickness behavior, because the latter term indicates a short-term adaptive response to inflammatory trauma. Nevertheless, a valid conclusion is that shared pathways, for example, increased levels of PIC, explain the partially overlapping phenomenology of sickness behavior and clinical depression.

There is also a new hypothesis that associates depression as an evolutionary product of sickness behavior with protection from infection. As such depression is regarded as an evolutionary behavioral response that helps the immune system to fight pathogens and to avoid new pathogen exposure [26, 174, 175]. These hypotheses, however, did not take into account that clinical depression is not a simple behavioral response, but a progressive disorder driven by a cascading neurobiology leading to a progressive course and pathophysiology. Moreover, acute lethargy, hyperalgesia, loss of interest, anxiety, and anhedonia are beneficial behaviors, but when chronic the same symptoms are typically not beneficial, but pathological and maladaptive: they may further isolate the depressed patient from social contacts creating a state of demotivation and demoralization and negative anticipation of the future [26]. Chronic illness, furthermore, requires a person to use coping and adaptive strategies to integrate the consequences of a disorder. There is a wide diversity of coping styles and beliefs on the nature of depression, some of which are adaptive while others are maladaptive [176].

Antidepressive treatments

Antidepressants have significant immunoregulatory and immunosuppressive effects in normal volunteers and animal models. Tricyclic antidepressants (TCAs) and selective 5-HT reuptake inhibitors (SSRIs) attenuate the production of PICs, for example, IL-1β, TNFα and IL-6, and Th1-like cytokines, including IL-2 and IFNγ [177]. Most antidepressants, that is, TCAs, SSRIs, reversible inhibitors of monoamine oxidase A, 5-HT and noradrenaline reuptake inhibitors, and atypical antidepressants (for example, tianeptine) all increase the production of IL-10, a negative immunoregulatory cytokine and/or lower the production of IFNγ, resulting in a decreased IFNγ/IL-10 production ratio [178]. There is also evidence that SSRIs and TCAs inhibit the production of IL-1β, TNF-α, and IL-6 in brain cell cultures [65]. Also, in animal models antidepressants have antiinflammatory effects [65]. Mice challenged with a lethal dose of LPS are protected by bupropion administration, which significantly reduces the production of IFNγ, TNFα and IL-1β [179]. There is also evidence that antidepressants may attenuate inflammation-induced sickness behaviors. For example, tianeptine may reduce sickness behaviors induced by peripheral (but not central) administration of LPS and IL-1β [180]. Treatments that target inflammation, for example, etanercept that blocks TNFα functions, may attenuate IL-1β-induced sickness behaviors [181].

In depressed patients, on the other hand, the in vivo effects of antidepressants are less clear. Subchronic treatments with antidepressants do not consistently attenuate inflammatory signs in depressed patients [182, 183]. Accordingly, a recent meta-analysis showed that antidepressant subclasses other than SSRIs did not attenuate the concentrations of pro-inflammatory cytokines [184]. Thus, despite the well-established immunoregulatory effects of antidepressants targeting inflammation (attenuate), Th1 (downregulate) and T regulatory (upregulate) functions, clinical remission in depression is not associated with normalization of immuno-inflammatory pathways [182184]. Thus, clinical depression appears to be accompanied by a 'resistance' to the immunosuppressive effects of antidepressants [183]. This may suggest that the immuno-inflammatory pathways are continuously activated by processes that cannot be blocked by antidepressants, for example, by the autoimmune responses directed against neoantigenic determinants [133] and increased translocation of gram negative bacteria [157]. There is also evidence that antidepressants target O&NS (attenuate), antioxidants (increase) and neuroprogressive processes (attenuate) [183]. Despite these effects, increased activity and sensitization of immuno-inflammatory pathways, O&NS pathways, autoimmune responses, and neuroprogression determine in part the staging of depression, for example, treatment resistance and recurrence of depression [52]. Thus, these pathways may in part explain why in many trials the clinical efficacy of antidepressants does not outperform placebo [185] and why, despite being treated with antidepressants, depressed patients show high relapse rates [186]. Therefore, new combinatorial treatment strategies are being developed in clinical depression with drugs that target inflammation, Th1 activation, O&NS and lowered antioxidant levels, and/or neuroprogression, for example, statins, acetylsalicylic acid, minocycline, zinc, N-acelyl cysteine, curcumin, ω3 polyunsaturated fatty acids, and so on [183].

Conclusions

Figure 3 compares sickness behavior with clinical depression. Sickness behavior helps to eradicate the trigger, has anti-inflammatory effects and is energy saving. As such sickness behavior enhances recovery and should be considered as part of a CIRS, which limits an overzealous immuno-inflammatory response to acute triggers. Cross-sectionally, there are phenomenological similarities between sickness behavior and the basic symptoms and melancholic, physio-somatic and anxiety symptom dimensions of clinical depression. Major differences, however, are that malaise, a core symptom of sickness behavior, occurs in some depressed patients only, whereas significant pyrexia is confined to sickness behavior. Moreover, depression is often accompanied not by anorexia and weight loss but by hyperphagia and weight gain. In most individuals, depression is a lifelong disease with a tendency towards recurrent episodes (waxing and waning), a chronic course, seasonal variation, and occasionally (hypo)manic symptoms. Moreover, sensitization and a potentially progressive deteriorating pattern characterize the course of depression. This contrasts with sickness behavior, which is defined as an acute, short lasting (19 to 43 days) behavioral pattern.

Figure 3
figure 3

This figure compares sickness behavior with clinical depression. Sickness behavior is energy saving, helps to eradicate the trigger, and has anti-inflammatory effects and as such enhances recovery and is part of a compensatory (anti)-inflammatory reflex system (CIRS). Increases in pro-inflammatory cytokines (PICs) underpin both sickness behavior and clinical depression and thus may explain the partial phenomenological overlap. Depression, however, is a chronic disorder with a specific course and pathophysiology and the presence of a CIRS that downregulates the primary inflammatory response. Disorders in tryptophan catabolites (TRYCATs), cell-mediated immune (CMI) activation, and oxidative and nitrosative stress (O&NS), and, in particular, their sequelae (O&NS damage, sensitization, autoimmunity and neuroprogression) are the specific organic substrates of depression. While sickness behavior is a behavioral response to acute triggers, the onset of depression is associated with multiple less-well defined trigger factors, for example, brain disorders, such as Alzheimer (AD), Huntington (HD), and Parkinson (PD) disorder, stroke and multiple sclerosis (MS); systemic disorders, such as cardio-vascular disorder (CVD), chronic obstructive pulmonary disorder (COPD), rheumatoid arthritis (RA), systemic lupus erythematosus (SLE), inflammatory bowel disorder (IBD), diabetes, metabolic syndrome, HIV infection, cancer, bacterial translocation; and conditions, such as postpartum period, hemodialysis, and interferon-(IFN)α based immunotherapy.

Full size image

Translational studies show that inflammatory pathways may account for sickness behavior as well as clinical depression and, therefore, may explain the partial phenomenological overlap between both conditions. Clinical depression is accompanied by a CIRS that downregulates the primary immuno-inflammatory response and by a transition from inflammation and ROS/RNS overproduction to sensitization in inflammatory and CMI responses, progressive O&NS damage and autoimmune responses. The latter pathways appear to be the substrate of a neuroprogressive process, whereby multiple depressive episodes cause neural tissue damage and its functional and cognitive sequelae. Sickness behavior is also induced by immuno-inflammatory pathways, but in contrast to clinical depression, the sickness behavioral complex has beneficial CIRS effects enhancing recovery from the primary trigger. When there is no resolution of the acute inflammatory phase within 19 to 43 days, chronic inflammation may ensue causing transition to chronic inflammatory pathology. Sickness behavior plays a critical role in preventing this transition by compensating for the negative energy balance and redirecting energy to the activated immune cells.

Whereas acute infections typically elicit sickness behavior, there is not much evidence that acute pathogens play a major role in clinical depression. While traumatic life events can induce an inflammatory state often leading to clinical depression, no association between psychosocial stressors and sickness behavior has been described. Comorbid depression increases morbidity and mortality in patients with (auto)immune and (neuro)inflammatory disorders, whereas sickness behavior, when present, would tend to dampen the inflammatory pathways.

All in all, while sickness behavior is a beneficial CIRS response, clinical depression is a disabling, progressive disorder. Inflammation thus provokes a Janus-faced response with a good 'acute' protective inflammatory side, involving CIRS responses, such as sickness behavior, and a bad 'chronic' side, that can lead to clinical depression, a chronic disorder with positive feedback loops between (neuro)inflammation and (neuro)degenerative processes following less well-defined triggers. This Janus face also represents the transition of an inflammation-induced adaptive behavioral response that is conserved through evolution to an inflammation-related chronic progressive disorder, which is increasing in prevalence in industrialized societies [187].

Abbreviations

AD:

Alzheimer disease

BCG:

bacille Calmette-Guérin

CMI:

cell-mediated immune

COPD:

chronic obstructive pulmonary disease

CRP:

C-reactive protein

CVD:

cardiovascular disorder

DSM IV TR:

The Diagnostic and Statistical Manual of Mental Disorders, fourth edition, text revision

IBD:

inflammatory bowel disease

IDO:

indoleamine 2,3-dioxygenase

IFN:

interferon

IL-1:

interleukin-1

IL-1RA:

IL-1 receptor antagonist

IRS:

inflammatory responses system

LPS:

lipopolysaccharide

mtDNA:

mitochondrial DNA

O&NS:

oxidative and nitrosative stress

PD:

Parkinson disease

PICs:

pro-inflammatory cytokines

RA:

rheumatoid arthritis

ROS/RNS:

reactive oxygen and nitrogen species

sIL-2R:

soluble IL-2 receptor

SLE:

systemic lupus erythematosus

SSRIs:

selective 5-HT reuptake inhibitors

TCAs:

tricyclic antidepressants

TNF:

tumor necrosis factor

TGF:

transforming growth factor

Th:

T helper

TRYCAT:

tryptophan catabolite.

References

  1. Maes M: A review on the acute phase response in major depression. Rev Neurosci. 1993, 4: 407-416.

    CAS  PubMed  Google Scholar 

  2. Maes M, Meltzer HY, Scharpe S, Cooreman W, Uyttenbroeck W, Suy E, Vandervorst C, Calabrese J, Raus J, Cosyns P: Psychomotor retardation, anorexia, weight loss, sleep disturbances, and loss of energy: psychopathological correlates of hyperhaptoglobinemia during major depression. Psychiatry Res. 1993, 47: 229-241. 10.1016/0165-1781(93)90081-Q.

    CAS  PubMed  Google Scholar 

  3. Holmes JE, Miller NE: Effects of bacterial endotoxin on water intake, food intake, and body temperature in the albino rat. J Exp Med. 1963, 118: 649-658. 10.1084/jem.118.4.649.

    CAS  PubMed  PubMed Central  Google Scholar 

  4. Hart BL: Biological basis of the behavior of sick animals. Neurosci Biobehav Rev. 1988, 12: 123-137. 10.1016/S0149-7634(88)80004-6.

    CAS  PubMed  Google Scholar 

  5. Maier SF, Wiertelak EP, Martin D, Watkins LR: Interleukin-1 mediates the behavioral hyperalgesia produced by lithium chloride and endotoxin. Brain Res. 1993, 623: 321-324. 10.1016/0006-8993(93)91446-Y.

    CAS  PubMed  Google Scholar 

  6. Yirmiya R: Endotoxin produces a depressive-like episode in rats. Brain Res. 1996, 711: 163-174. 10.1016/0006-8993(95)01415-2.

    CAS  PubMed  Google Scholar 

  7. Johnson RW: The concept of sickness behavior: a brief chronological account of four key discoveries. Vet Immunol Immunopathol. 2002, 87: 443-450. 10.1016/S0165-2427(02)00069-7.

    CAS  PubMed  Google Scholar 

  8. Qin L, Wu X, Block ML, Liu Y, Breese GR, Hong JS, Knapp DJ, Crews FT: Systemic LPS causes chronic neuroinflammation and progressive neurodegeneration. Glia. 2007, 55: 453-462. 10.1002/glia.20467.

    PubMed  PubMed Central  Google Scholar 

  9. Dantzer R, O'Connor JC, Freund GG, Johnson RW, Kelley KW: From inflammation to sickness and depression: when the immune system subjugates the brain. Nat Rev Neurosci. 2008, 9: 46-56. 10.1038/nrn2297.

    CAS  PubMed  PubMed Central  Google Scholar 

  10. Burton MD, Sparkman NL, Johnson RW: Inhibition of interleukin-6 trans-signaling in the brain facilitates recovery from lipopolysaccharide-induced sickness behavior. J Neuroinflammation. 2011, 8: 54-10.1186/1742-2094-8-54.

    CAS  PubMed  PubMed Central  Google Scholar 

  11. Maes M: Evidence for an immune response in major depression: a review and hypothesis. Prog Neuropsychopharmacol Biol Psychiatry. 1995, 19: 11-38. 10.1016/0278-5846(94)00101-M.

    CAS  PubMed  Google Scholar 

  12. Maes M, Bosmans E, Suy E, Vandervorst C, DeJonckheere C, Raus J: Depression-related disturbances in mitogen-induced lymphocyte responses and interleukin-1 beta and soluble interleukin-2 receptor production. Acta Psychiatr Scand. 1991, 84: 379-386. 10.1111/j.1600-0447.1991.tb03163.x.

    CAS  PubMed  Google Scholar 

  13. Maes M, Scharpe S, Bosmans E, Vandewoude M, Suy E, Uyttenbroeck W, Cooreman W, Vandervorst C, Raus J: Disturbances in acute phase plasma proteins during melancholia: additional evidence for the presence of an inflammatory process during that illness. Prog Neuropsychopharmacol Biol Psychiatry. 1992, 16: 501-515. 10.1016/0278-5846(92)90056-K.

    CAS  PubMed  Google Scholar 

  14. Song C, Dinan T, Leonard BE: Changes in immunoglobulin, complement and acute phase protein levels in the depressed patients and normal controls. J Affect Disord. 1994, 30: 283-288. 10.1016/0165-0327(94)90135-X.

    CAS  PubMed  Google Scholar 

  15. Leonard B, Maes M: Mechanistic explanations how cell-mediated immune activation, inflammation and oxidative and nitrosative stress pathways and their sequels and concomitants play a role in the pathophysiology of unipolar depression. Neurosci Biobehav Rev. 2012, 36: 764-785. 10.1016/j.neubiorev.2011.12.005.

    CAS  PubMed  Google Scholar 

  16. Berk M, Brnabic A, Dodd S, Kelin K, Tohen M, Malhi GS, Berk L, Conus P, McGorry PD: Does stage of illness impact treatment response in bipolar disorder? Empirical treatment data and their implication for the staging model and early intervention. Bipolar Disord. 2011, 13: 87-98. 10.1111/j.1399-5618.2011.00889.x.

    PubMed  Google Scholar 

  17. Berk M, Kapczinski F, Andreazza AC, Dean OM, Giorlando F, Maes M, Yücel M, Gama CS, Dodd S, Dean B, Magalhaes PV, Amminger P, McGorry P, Malhi GS: Pathways underlying neuroprogression in bipolar disorder: focus on inflammation, oxidative stress and neurotrophic factors. Neurosci Biobehav Rev. 2011, 35: 804-817. 10.1016/j.neubiorev.2010.10.001.

    CAS  PubMed  Google Scholar 

  18. Maes M, Mihaylova I, Kubera M, Ringel K: Activation of cell-mediated immunity in depression: association with inflammation, melancholia, clinical staging and the fatigue and somatic symptom cluster of depression. Prog Neuropsychopharmacol Biol Psychiatry. 2012, 36: 169-175. 10.1016/j.pnpbp.2011.09.006.

    PubMed  Google Scholar 

  19. Dowlati Y, Herrmann N, Swardfager W, Liu H, Sham L, Reim EK, Lanctôt KL: A meta-analysis of cytokines in major depression. Biol Psychiatry. 2010, 67: 446-457. 10.1016/j.biopsych.2009.09.033.

    CAS  PubMed  Google Scholar 

  20. Liu Y, Ho RC, Mak A: Interleukin (IL)-6, tumour necrosis factor alpha (TNF-αa) and soluble interleukin-2 receptors (sIL-2R) are elevated in patients with major depressive disorder: a meta-analysis and meta-regression. J Affect Disord. 2012, 139: 230-239. 10.1016/j.jad.2011.08.003.

    CAS  PubMed  Google Scholar 

  21. Medzhitov R: Inflammation 2010: new adventures of an old flame. Cell. 2010, 140: 771-776. 10.1016/j.cell.2010.03.006.

    CAS  PubMed  Google Scholar 

  22. Peters A: The energy request of inflammation. Endocrinology. 2006, 147: 4550-4552. 10.1210/en.2006-0815.

    CAS  PubMed  Google Scholar 

  23. Steinberg GR, Watt MJ, Febbraio MA: Cytokine regulation of AMPK signalling. Front Biosci. 2009, 14: 1902-1916.

    CAS  Google Scholar 

  24. Roubenoff R, Roubenoff RA, Cannon JG, Kehayias JJ, Zhuang H, Dawson-Hughes B, Dinarello CA, Rosenberg IH: Rheumatoid cachexia: cytokine-driven hypermetabolism accompanying reduced body cell mass in chronic inflammation. J Clin Invest. 1994, 93: 2379-2386. 10.1172/JCI117244.

    CAS  PubMed  PubMed Central  Google Scholar 

  25. Maes M, Kubera M, Obuchowiczwa E, Goehler L, Brzeszcz J: Depression's multiple comorbidities explained by (neuro)inflammatory and oxidative & nitrosative stress pathways. Neuro Endocrinol Lett. 2011, 32: 7-24.

    CAS  PubMed  Google Scholar 

  26. Charlton BG: The malaise theory of depression: major depressive disorder is sickness behavior and antidepressants are analgesic. Med Hypotheses. 2000, 54: 126-30. 10.1054/mehy.1999.0986.

    CAS  PubMed  Google Scholar 

  27. Cunningham-Rundles S, McNeeley DF, Moon A: Mechanisms of nutrient modulation of the immune response. J Allergy Clin Immunol. 2005, 115: 1119-1128. 10.1016/j.jaci.2005.04.036.

    CAS  PubMed  Google Scholar 

  28. Kluger MJ: Fever. Pediatrics. 1980, 66: 720-724.

    CAS  PubMed  Google Scholar 

  29. Schaffner A: Fever--useful or noxious symptom that should be treated?. Ther Umsch. 2006, 63: 185-188. 10.1024/0040-5930.63.3.185.

    CAS  PubMed  Google Scholar 

  30. Rantala S, Vuopio-Varkila J, Vuento R, Huhtala H, Syrjänen J: Predictors of mortality in beta-hemolytic streptococcal bacteremia: a population-based study. J Infect. 2009, 58: 266-272. 10.1016/j.jinf.2009.01.015.

    PubMed  Google Scholar 

  31. El-Radhi AS: The role of fever in the past and present. Med J Islamic World Acad Sci. 2011, 19: 9-14.

    Google Scholar 

  32. Harden LM, du Plessis I, Roth J, Loram LC, Poole S, Laburn HP: Differences in the relative involvement of peripherally released interleukin (IL)-6, brain IL-1β and prostanoids in mediating lipopolysaccharide-induced fever and sickness behavior. Psychoneuroendocrinology. 2011, 36: 608-622. 10.1016/j.psyneuen.2010.09.003.

    CAS  PubMed  Google Scholar 

  33. Lennie TA: Relationship of body energy status to inflammation-induced anorexia and weight loss. Physiol Behav. 1998, 64: 475-481. 10.1016/S0031-9384(98)00103-6.

    CAS  PubMed  Google Scholar 

  34. Kluger MJ, Rothenburg BA: Fever and reduced iron: their interaction as a host defense response to bacterial infection. Science. 1979, 203: 374-376. 10.1126/science.760197.

    CAS  PubMed  Google Scholar 

  35. Jung KJ, Lee EK, Kim JY, Zou Y, Sung B, Heo HS, Kim MK, Lee J, Kim ND, Yu BP, Chung HY: Effect of short term calorie restriction on pro-inflammatory NF-kB and AP-1 in aged rat kidney. Inflamm Res. 2009, 58: 143-150. 10.1007/s00011-008-7227-2.

    CAS  PubMed  Google Scholar 

  36. MacDonald L, Radler M, Paolini AG, Kent S: Calorie restriction attenuates LPS-induced sickness behavior and shifts hypothalamic signaling pathways to an anti-inflammatory bias. Am J Physiol Regul Integr Comp Physiol. 2011, 301: R172-184. 10.1152/ajpregu.00057.2011.

    CAS  PubMed  Google Scholar 

  37. Bosutti A, Malaponte G, Zanetti M, Castellino P, Heer M, Guarnieri G, Biolo G: Calorie restriction modulates inactivity-induced changes in the inflammatory markers C-reactive protein and pentraxin-3. J Clin Endocrinol Metab. 2008, 93: 3226-3229. 10.1210/jc.2007-1684.

    CAS  PubMed  Google Scholar 

  38. Kopp HP, Kopp CW, Festa A, Krzyzanowska K, Kriwanek S, Minar E, Roka R, Schernthaner G: Impact of weight loss on inflammatory proteins and their association with the insulin resistance syndrome in morbidly obese patients. Arterioscler Thromb Vasc Biol. 2003, 23: 1042-1047. 10.1161/01.ATV.0000073313.16135.21.

    CAS  PubMed  Google Scholar 

  39. Jellema A, Plat J, Mensink RP: Weight reduction, but not a moderate intake of fish oil, lowers concentrations of inflammatory markers and PAI-1 antigen in obese men during the fasting and postprandial state. Eur J Clin Invest. 2004, 34: 766-773. 10.1111/j.1365-2362.2004.01414.x.

    CAS  PubMed  Google Scholar 

  40. Sharman MJ, Volek JS: Weight loss leads to reductions in inflammatory biomarkers after a very-low-carbohydrate diet and a low-fat diet in overweight men. Clin Sci (Lond). 2004, 107: 365-369. 10.1042/CS20040111.

    CAS  Google Scholar 

  41. Yang WS, Lee WJ, Funahashi T, Tanaka S, Matsuzawa Y, Chao CL, Chen CL, Tai TY, Chuang LM: Weight reduction increases plasma levels of an adipose-derived anti-inflammatory protein, adiponectin. J Clin Endocrinol Metab. 2002, 86: 3815-3819.

    Google Scholar 

  42. Maes M, Maes L, Schotte C, Vandewoude M, Martin M, D'Hondt P, Blockx P, Scharpé S, Cosyns P: Clinical subtypes of unipolar depression: part III. quantitative differences in various biological markers between the cluster-analytically generated nonvital and vital depression classes. Psychiatry Res. 1990, 34: 59-75. 10.1016/0165-1781(90)90058-D.

    CAS  PubMed  Google Scholar 

  43. Maes M, Meltzer HY, Cosyns P, Schotte C: Evidence for the existence of major depression with and without anxiety features. Psychopathology. 1994, 27: 1-13. 10.1159/000284842.

    CAS  PubMed  Google Scholar 

  44. Maes M: "Functional" or "psychosomatic" symptoms, for example a flu-like malaise, aches and pain and fatigue, are major features of major and in particular of melancholic depression. Neuro Endocrinol Lett. 2009, 30: 564-573.

    PubMed  Google Scholar 

  45. Rausch JL, Johnson ME, Corley KM, Hobby HM, Shendarkar N, Fei Y, Ganapathy V, Leibach FH: Depressed patients have higher body temperature: 5-HT transporter long promoter region effects. Neuropsychobiology. 2003, 47: 120-127. 10.1159/000070579.

    CAS  PubMed  Google Scholar 

  46. Szuba MP, Guze BH, Baxter LR: Electroconvulsive therapy increases circadian amplitude and lowers core body temperature in depressed subjects. Biol Psychiatry. 1997, 42: 1130-1137. 10.1016/S0006-3223(97)00046-2.

    CAS  PubMed  Google Scholar 

  47. Boland RJ, Keller MB: The course of depression. Neuropsychopharmacology, the 5th Generation of Progress. Edited by: Davis KL, Charney D, Coyle JT, Nemeroff C. 2002, New York: American College of Neuropsychopharmacology, 1009-1015.

    Google Scholar 

  48. Berk M, Conus P, Lucas N, Hallam K, Malhi GS, Dodd S, Yatham LN, Yung A, McGorry P: Setting the stage: from prodrome to treatment resistance in bipolar disorder. Bipolar Disord. 2007, 9: 671-678. 10.1111/j.1399-5618.2007.00484.x.

    PubMed  Google Scholar 

  49. Berk M, Hallam KT, McGorry PD: The potential utility of a staging model as a course specifier: a bipolar disorder perspective. J Affect Disord. 2007, 100: 279-281. 10.1016/j.jad.2007.03.007.

    PubMed  Google Scholar 

  50. Berlim MT, Turecki G: What is the meaning of treatment resistant/refractory major depression (TRD)? A systematic review of current randomized trials. Eur Neuropsychopharmacol. 2007, 17: 696-707. 10.1016/j.euroneuro.2007.03.009.

    CAS  PubMed  Google Scholar 

  51. Caliyurt O, Altiay G: Resting energy expenditure in manic episode. Bipolar Disord. 2009, 11: 102-106. 10.1111/j.1399-5618.2008.00649.x.

    PubMed  Google Scholar 

  52. Moylan S, Maes M, Wray NR, Berk M: The neuroprogressive nature of Major Depressive Disorder: pathways to disease evolution and resistance, and therapeutic implications. Mol Psychiatry.

  53. Kessing LV: Severity of depressive episodes during the course of depressive disorder. Brit J Psychiatry. 2008, 192: 290-293. 10.1192/bjp.bp.107.038935.

    Google Scholar 

  54. Kessing LV, Andersen PK: Does the risk of developing dementia increase with the number of episodes in patients with depressive disorder and in patients with bipolar disorder?. J Neurol Neurosurg Psychiatry. 2004, 75: 1662-1666. 10.1136/jnnp.2003.031773.

    CAS  PubMed  PubMed Central  Google Scholar 

  55. Post RM, Rubinow DR, Ballenger JC: Conditioning and sensitisation in the longitudinal course of affective illness. Br J Psychiatry. 1986, 149: 191-201. 10.1192/bjp.149.2.191.

    CAS  PubMed  Google Scholar 

  56. Antelman SM, Levine J, Gershon S: Time-dependent sensitization: the odyssey of a scientific heresy from the laboratory to the door of the clinic. Mol Psychiatry. 2000, 5: 350-356. 10.1038/sj.mp.4000721.

    CAS  PubMed  Google Scholar 

  57. Bell IR, Hardin EE, Baldwin CM, Schwartz GE: Increased limbic system symptomatology and sensitizability of young adults with chemical and noise sensitivities. Environ Res. 1995, 70: 84-97. 10.1006/enrs.1995.1052.

    CAS  PubMed  Google Scholar 

  58. Kapczinski F, Vieta E, Andreazza AC, Frey BN, Gomes FA, Tramontina J, Kauer-Sant'anna M, Grassi-Oliveira R, Post RM: Allostatic load in bipolar disorder: implications for pathophysiology and treatment. Neurosci Biobehav Rev. 2008, 32: 675-692. 10.1016/j.neubiorev.2007.10.005.

    PubMed  Google Scholar 

  59. Sato T, Bottlender R, Sievers M, Möller HJ: Distinct seasonality of depressive episodes differentiates unipolar depressive patients with and without depressive mixed states. J Affect Disord. 2006, 90: 1-5. 10.1016/j.jad.2005.09.009.

    PubMed  Google Scholar 

  60. Sylvén SM, Papadopoulos FC, Olovsson M, Ekselius L, Poromaa IS, Skalkidou A: Seasonality patterns in postpartum depression. Am J Obstet Gynecol. 2011, 204: 413.e1-6. 10.1016/j.ajog.2011.01.022.

    Google Scholar 

  61. Maes M, Cosyns P, Meltzer HY, De Meyer F, Peeters D: Seasonality in violent suicide but not in nonviolent suicide or homicide. Am J Psychiatry. 1993, 150: 1380-1385.

    CAS  PubMed  Google Scholar 

  62. Stone EA, Lehmann ML, Lin Y, Quartermain D: Depressive behavior in mice due to immune stimulation is accompanied by reduced neural activity in brain regions involved in positively motivated behavior. Biol Psychiatry. 2006, 60: 803-811. 10.1016/j.biopsych.2006.04.020.

    CAS  PubMed  Google Scholar 

  63. Gaykema RPA, Park S-M, McKibbin CR, Goehler LE: Lipopolysaccharide suppresses activation of the tuberomammillary histaminergic system concomitant with behavior: a novel target of immune-sensory pathways. Neuroscience. 2008, 152: 273-287. 10.1016/j.neuroscience.2007.10.042.

    CAS  PubMed  PubMed Central  Google Scholar 

  64. Bower JE, Ganz PA, Aziz N, Fahey JL: Fatigue and proinflammatory cytokine activity in breast cancer survivors. Psychosom Med. 2002, 64: 604-611.

    PubMed  Google Scholar 

  65. Kubera M, Obuchowicz E, Goehler L, Brzeszcz J, Maes M: In animal models, psychosocial stress-induced (neuro)inflammation, apoptosis and reduced neurogenesis are associated to the onset of depression. Prog Neuropsychopharmacol Biol Psychiatry. 2011, 35: 744-759. 10.1016/j.pnpbp.2010.08.026.

    CAS  PubMed  Google Scholar 

  66. Leonard BE, Song C: Changes in the immune system in rodent models of depression. Int J Neuropsychopharmacol. 2002, 5: 345-356. 10.1017/S1461145702003140.

    CAS  PubMed  Google Scholar 

  67. Song C, Leonard BE: The olfactory bulbectomised rat as a model of depression. Neurosci Biobehav Rev. 2005, 29: 627-647. 10.1016/j.neubiorev.2005.03.010.

    PubMed  Google Scholar 

  68. Gaykema RPA, Goehler LE: Lipopolysaccharide challenge-induced suppression of Fos in hypothalamic orexin neurons: their potential role in sickness behavior. Brain Behav Immun. 2009, 23: 926-930. 10.1016/j.bbi.2009.03.005.

    CAS  PubMed  PubMed Central  Google Scholar 

  69. Gaykema RPA, Goehler LE: Ascending caudal medullary catecholamine pathways drive sickness-induced deficits in exploratory behavior: brain substrates for fatigue?. Brain Behav Immun. 2011, 25: 443-460. 10.1016/j.bbi.2010.11.005.

    CAS  PubMed  Google Scholar 

  70. Anisman H, Merali Z: Anhedonic and anxiogenic effects of cytokine exposure. Adv Exp Med Biol. 1999, 461: 199-233. 10.1007/978-0-585-37970-8_12.

    CAS  PubMed  Google Scholar 

  71. Lyte M, Li W, Opitz N, Gaykema RP, Goehler LE: Induction of anxiety-like behavior in mice during the initial stages of infection with the agent of murine colonic hyperplasia Citrobacter rodentium. Physiol Behav. 2006, 89: 350-357. 10.1016/j.physbeh.2006.06.019.

    CAS  PubMed  Google Scholar 

  72. Goehler LE, Lyte M, Gaykema RP: Infection-induced viscerosensory signals from the gut enhance anxiety: implications for psychoneuroimmunology. Brain Behav Immun. 2007, 21: 721-726. 10.1016/j.bbi.2007.02.005.

    CAS  PubMed  PubMed Central  Google Scholar 

  73. Castex N, Fioramonti J, Fargeas MJ, Bueno L: c-fos expression in specific rat brain nuclei after intestinal anaphylaxis: involvement of 5-HT3 receptors and vagal afferent fibers. Brain Res. 1995, 688: 149-160. 10.1016/0006-8993(95)00526-V.

    CAS  PubMed  Google Scholar 

  74. Rossi-George A, Urbach D, Colas D, Goldfarb Y, Kusnecov AW: Neuronal, endocrine, and anorexic responses to the T-cell superantigen staphylococcal enterotoxin A: dependence on tumor necrosis factor-alpha. J Neurosci. 2005, 25: 5314-5322. 10.1523/JNEUROSCI.0687-05.2005.

    CAS  PubMed  Google Scholar 

  75. Goehler LE, Gaykema RP, Opitz N, Reddaway R, Badr N, Lyte M: Activation in vagal afferents and central autonomic pathways: early responses to intestinal infection with Campylobacter jejuni. Brain Behav Immun. 2005, 19: 334-344. 10.1016/j.bbi.2004.09.002.

    PubMed  Google Scholar 

  76. Grossberg AJ, Zhu X, Leinninger GM, Levasseur PR, Braun TP, Myers MG, Marks DL: Inflammation-induced lethargy is mediated by suppression of orexin neuron activity. J Neurosci. 2011, 31: 11376-11386. 10.1523/JNEUROSCI.2311-11.2011.

    CAS  PubMed  PubMed Central  Google Scholar 

  77. Maes M, Bosmans E, Suy E, Vandervorst C, De Jonckheere C, Raus J: Immune disturbances during major depression: upregulated expression of interleukin-2 receptors. Neuropsychobiology. 1990, 24: 115-120. 10.1159/000119472.

    PubMed  Google Scholar 

  78. Maes M: Depression is an inflammatory disease, but cell-mediated immune activation is the key component of depression. Prog Neuropsychopharmacol Biol Psychiatry. 2011, 35: 664-675. 10.1016/j.pnpbp.2010.06.014.

    CAS  PubMed  Google Scholar 

  79. Howren MB, Lamkin DM, Suls J: Associations of depression with C-reactive protein, IL-1, and IL-6: a meta-analysis. Psychosom Med. 2009, 71: 171-186. 10.1097/PSY.0b013e3181907c1b.

    CAS  PubMed  Google Scholar 

  80. Maes M, Lin AH, Delmeire L, Van Gastel A, Kenis G, De Jongh R, Bosmans E: Elevated serum interleukin-6 (IL-6) and IL-6 receptor concentrations in posttraumatic stress disorder following accidental man-made traumatic events. Biol Psychiatry. 1999, 45: 833-839. 10.1016/S0006-3223(98)00131-0.

    CAS  PubMed  Google Scholar 

  81. Bonaccorso S, Puzella A, Marino V, Pasquini M, Biondi M, Artini M, Almerighi C, Levrero M, Egyed B, Bosmans E, Meltzer HY, Maes M: Immunotherapy with interferon-alpha in patients affected by chronic hepatitis C induces an intercorrelated stimulation of the cytokine network and an increase in depressive and anxiety symptoms. Psychiatry Res. 2001, 105: 45-55. 10.1016/S0165-1781(01)00315-8.

    CAS  PubMed  Google Scholar 

  82. Wichers MC, Kenis G, Koek GH, Robaeys G, Nicolson NA, Maes M: Interferon-alpha-induced depressive symptoms are related to changes in the cytokine network but not to cortisol. J Psychosom Res. 2007, 62: 207-214. 10.1016/j.jpsychores.2006.09.007.

    PubMed  Google Scholar 

  83. Anisman H: Cascading effects of stressors and inflammatory immune system activation: implications for major depressive disorder. J Psychiatry Neurosci. 2009, 34: 4-20.

    PubMed  PubMed Central  Google Scholar 

  84. Piser TM: Linking the cytokine and neurocircuitry hypotheses of depression: a translational framework for discovery and development of novel anti-depressants. Brain Behav Immun. 2010, 24: 515-524. 10.1016/j.bbi.2010.02.006.

    CAS  PubMed  Google Scholar 

  85. Swiergiel AH, Dunn AJ: Effects of interleukin-1beta and lipopolysaccharide on behavior of mice in the elevated plus-maze and open field tests. Pharmacol Biochem Behav. 2007, 86: 651-659. 10.1016/j.pbb.2007.02.010.

    CAS  PubMed  PubMed Central  Google Scholar 

  86. Frenois F, Moreau M, O'Connor J, Lawson M, Micon C, Lestage J, Kelley KW, Dantzer R, Castanon N: Lipopolysaccharide induces delayed FosB/DeltaFosB immunostaining within the mouse extended amygdala, hippocampus and hypothalamus, that parallel the expression of depressive-like behavior. Psychoneuroendocrinol. 2007, 32: 516-531. 10.1016/j.psyneuen.2007.03.005.

    CAS  Google Scholar 

  87. Lacosta S, Merali Z, Anisman H: Influence of acute and repeated interleukin-2 administration on spatial learning, locomotor activity, exploratory behaviors, and anxiety. Behav Neurosci. 1999, 113: 1030-1041.

    CAS  PubMed  Google Scholar 

  88. Song C, Phillips AG, Leonard B: Interleukin 1 beta enhances conditioned fear memory in rats: possible involvement of glucocorticoids. Eur J Neurosci. 2003, 18: 1739-1743. 10.1046/j.1460-9568.2003.02886.x.

    PubMed  Google Scholar 

  89. Nathan C: Points of control in inflammation. Nature. 2002, 420: 846-852. 10.1038/nature01320.

    CAS  PubMed  Google Scholar 

  90. Adib-Conquy M, Cavaillon JM: Compensatory anti-inflammatory response syndrome. Thromb Haemost. 2009, 101: 36-47.

    CAS  PubMed  Google Scholar 

  91. Tracey KJ: The inflammatory reflex. Nature. 2002, 420: 853-859. 10.1038/nature01321. Review

    CAS  PubMed  Google Scholar 

  92. Bone RC: Important new findings in sepsis. JAMA. 1997, 278: 249-10.1001/jama.1997.03550030089042.

    CAS  PubMed  Google Scholar 

  93. Burdette SD, Parilo MA, Kaplan LJ, Bailey H: Systemic inflammatory response syndrome. Medscape, eMedicine. 2010, updated April 11, 2012, [http://emedicine.medscape.com/article/168943]

    Google Scholar 

  94. Maes M, Meltzer HY, Scharpé S, Bosmans E, Suy E, De Meester I, Calabrese J, Cosyns P: Relationships between lower plasma L-tryptophan levels and immune-inflammatory variables in depression. Psychiatry Res. 1993, 49: 151-165. 10.1016/0165-1781(93)90102-M.

    CAS  PubMed  Google Scholar 

  95. Maes M, Scharpé S, Meltzer HY, Okayli G, Bosmans E, D'Hondt P, Vanden Bossche BV, Cosyns P: Increased neopterin and interferon-gamma secretion and lower availability of L-tryptophan in major depression: further evidence for an immune response. Psychiatry Res. 1994, 54: 143-160. 10.1016/0165-1781(94)90003-5.

    CAS  PubMed  Google Scholar 

  96. Maes M, Leonard BE, Myint AM, Kubera M, Verkerk R: The new '5-HT' hypothesis of depression: cell-mediated immune activation induces indoleamine 2,3-dioxygenase, which leads to lower plasma tryptophan and an increased synthesis of detrimental tryptophan catabolites (TRYCATs), both of which contribute to the onset of depression. Prog Neuropsychopharmacol Biol Psychiatry. 2011, 35: 702-721. 10.1016/j.pnpbp.2010.12.017.

    CAS  PubMed  Google Scholar 

  97. Song C, Lin A, Bonaccorso S, Heide C, Verkerk R, Kenis G, Bosmans E, Scharpe S, Whelan A, Cosyns P, de Jongh R, Maes M: The inflammatory response system and the availability of plasma tryptophan in patients with primary sleep disorders and major depression. J Affect Disord. 1998, 49: 211-219. 10.1016/S0165-0327(98)00025-1.

    CAS  PubMed  Google Scholar 

  98. Werner-Felmayer G, Werner ER, Fuchs D, Hausen A, Reibnegger G, Wachter H: Tumour necrosis factor-alpha and lipopolysaccharide enhance interferon-induced tryptophan degradation and pteridine synthesis in human cells. Biol Chem Hoppe Seyler. 1989, 370: 1063-1069. 10.1515/bchm3.1989.370.2.1063.

    CAS  PubMed  Google Scholar 

  99. Takikawa O, Yoshida R, Yasui H, Hayaishi O: The relationship between plasma kynurenine and indoleamine 2,3-dioxygenase activity in the extrahepatic tissues. Progress in Tryptophan and Serotonin Research. Edited by: Schlossberger HG, Kochen W, Linzen B, Steinhart H. 1984, Berlin-New York: Walter de Gruyter and Co, 517-520.

    Google Scholar 

  100. Moroni F, Russi P, Gallo-Mezo MA, Moneti G, Pellicciari R: Modulation of quinolinic and kynurenic acid content in the rat brain: effects of endotoxins and nicotinylalanine. J Neurochem. 1991, 57: 1630-1635. 10.1111/j.1471-4159.1991.tb06361.x.

    CAS  PubMed  Google Scholar 

  101. Bonaccorso S, Marino V, Puzella A, Pasquini M, Biondi M, Artini M, Almerighi C, Verkerk R, Meltzer H, Maes M: Increased depressive ratings in patients with hepatitis C receiving interferon-alpha-based immunotherapy are related to interferon-alpha-induced changes in the serotonergic system. J Clin Psychopharmacol. 2002, 22: 86-90. 10.1097/00004714-200202000-00014.

    CAS  PubMed  Google Scholar 

  102. Maes M, Verkerk R, Bonaccorso S, Ombelet W, Bosmans E, Scharpé S: Depressive and anxiety symptoms in the early puerperium are related to increased degradation of tryptophan into kynurenine, a phenomenon which is related to immune activation. Life Sci. 2002, 71: 1837-1848. 10.1016/S0024-3205(02)01853-2.

    CAS  PubMed  Google Scholar 

  103. Toker L, Amar S, Bersudsky Y, Benjamin J, Klein E: The biology of tryptophan depletion and mood disorders. Isr J Psychiatry Relat Sci. 2010, 47: 46-55.

    PubMed  Google Scholar 

  104. O'Connor JC, André C, Wang Y, Lawson MA, Szegedi SS, Lestage J, Castanon N, Kelley KW, Dantzer R: Interferon-gamma and tumor necrosis factor-alpha mediate the upregulation of indoleamine 2,3-dioxygenase and the induction of depressive-like behavior in mice in response to bacillus Calmette-Guerin. J Neurosci. 2009, 29: 4200-4209. 10.1523/JNEUROSCI.5032-08.2009.

    PubMed  PubMed Central  Google Scholar 

  105. Hoes MJ: The clinical significance of an elevated excretion of xanthurenic acid in psychiatric patients. Acta Psychiatr Belg. 1979, 79: 638-646.

    CAS  PubMed  Google Scholar 

  106. Møller SE, Kirk L, Honoré P: Tryptophan tolerance and metabolism in endogenous depression. Psychopharmacology (Berl). 1982, 76: 79-83. 10.1007/BF00430761.

    Google Scholar 

  107. Maes M, De Ruyter M, Suy E: Xanthurenic acid flow in 24-hour urine following L-tryptophan loading in depressive patients. Acta Psychiatr Belg. 1986, 86: 120-130.

    CAS  PubMed  Google Scholar 

  108. Maes M, De Ruyter M, Suy E: The renal excretion of xanthurenic acid following L-tryptophan loading in depressed patients. Hum Psychopharmacol Clin Exp. 1987, 2: 231-235. 10.1002/hup.470020406.

    Google Scholar 

  109. Myint AM, Kim YK, Verkerk R, Scharpé S, Steinbusch H, Leonard B: Kynurenine pathway in major depression: evidence of impaired neuroprotection. J Affect Disord. 2007, 98: 143-151. 10.1016/j.jad.2006.07.013.

    CAS  PubMed  Google Scholar 

  110. Gabbay V, Klein RG, Katz Y, Mendoza S, Guttman LE, Alonso CM, Babb JS, Hirsch GS, Liebes L: The possible role of the kynurenine pathway in adolescent depression with melancholic features. J Child Psychol Psychiatry. 2010, 51: 935-943. 10.1111/j.1469-7610.2010.02245.x.

    PubMed  PubMed Central  Google Scholar 

  111. Steiner J, Walter M, Gos T, Guillemin GJ, Bernstein HG, Sarnyai Z, Mawrin C, Brisch R, Bielau H, Meyer zu Schwabedissen L, Bogerts B, Myint AM: Severe depression is associated with increased microglial quinolinic acid in subregions of the anterior cingulate gyrus: evidence for an immune-modulated glutamatergic neurotransmission?. J Neuroinflammation. 2011, 8: 94-10.1186/1742-2094-8-94.

    CAS  PubMed  PubMed Central  Google Scholar 

  112. Sublette ME, Galfalvy HC, Fuchs D, Lapidus M, Grunebaum MF, Oquendo MA, Mann JJ, Postolache TT: Plasma kynurenine levels are elevated in suicide attempters with major depressive disorder. Brain Behav Immun. 2011, 25: 1272-1278. 10.1016/j.bbi.2011.05.002.

    CAS  PubMed  PubMed Central  Google Scholar 

  113. Anderson G, Maes M, Berk M: Biological underpinnings of the commonalities in depression, somatization, and chronic fatigue syndrome. Med Hypotheses. 2012, 78: 752-756. 10.1016/j.mehy.2012.02.023.

    PubMed  Google Scholar 

  114. Celik C, Erdem M, Cayci T, Ozdemir B, Ozgur Akgul E, Kurt YG, Yaman H, Isintas M, Ozgen F, Ozsahin A: The association between serum levels of neopterin and number of depressive episodes of major depression. Prog Neuropsychopharmacol Biol Psychiatry. 2010, 34: 372-375. 10.1016/j.pnpbp.2010.01.002.

    CAS  PubMed  Google Scholar 

  115. Maes M, Ombelet W, De Jongh R, Kenis G, Bosmans E: The inflammatory response following delivery is amplified in women who previously suffered from major depression, suggesting that major depression is accompanied by a sensitization of the inflammatory response system. J Affect Disord. 2001, 63: 85-92. 10.1016/S0165-0327(00)00156-7.

    CAS  PubMed  Google Scholar 

  116. Liukkonen T, Silvennoinen-Kassinen S, Jokelainen J, Räsänen P, Leinonen M, Meyer-Rochow VB, Timonen M: The association between C-reactive protein levels and depression: results from the northern Finland 1966 birth cohort study. Biol Psychiatry. 2006, 60: 825-830. 10.1016/j.biopsych.2006.02.016.

    CAS  PubMed  Google Scholar 

  117. Hennessy MB, Paik KD, Caraway JD, Schiml PA, Deak T: Proinflammatory activity and the sensitization of depressive-like behavior during maternal separation. Behav Neurosci. 2011, 125: 426-433.

    PubMed  PubMed Central  Google Scholar 

  118. Kawasaki Y, Zhang L, Cheng JK, Ji RR: Cytokine mechanisms of central sensitization: distinct and overlapping role of interleukin-1beta, interleukin-6, and tumor necrosis factor-alpha in regulating synaptic and neuronal activity in the superficial spinal cord. J Neurosci. 2008, 28: 5189-5194. 10.1523/JNEUROSCI.3338-07.2008.

    CAS  PubMed  PubMed Central  Google Scholar 

  119. Maes M, Ringel K, Kubera M, Berk M, Rybakowski J: Increased autoimmune activity against 5-HT: a key component of depression that is associated with inflammation and activation of cell-mediated immunity, and with severity and staging of depression. J Affect Disord. 2012, 136: 386-392. 10.1016/j.jad.2011.11.016.

    CAS  PubMed  Google Scholar 

  120. Hochstrasser T, Ullrich C, Sperner-Unterweger B, Humpel C: Inflammatory stimuli reduce survival of serotonergic neurons and induce neuronal expression of indoleamine 2,3-dioxygenase in rat dorsal raphe nucleus organotypic brain slices. Neuroscience. 2011, 184: 128-138.

    CAS  PubMed  Google Scholar 

  121. Maes M, Bosmans E, De Jongh R, Kenis G, Vandoolaeghe E, Neels H: Increased serum IL-6 and IL-1 receptor antagonist concentrations in major depression and treatment resistant depression. Cytokine. 1997, 9: 853-858. 10.1006/cyto.1997.0238.

    CAS  PubMed  Google Scholar 

  122. Maes M, Vandoolaeghe E, Neels H, Demedts P, Wauters A, Meltzer HY, Altamura C, Desnyder R: Lower serum zinc in major depression is a sensitive marker of treatment resistance and of the immune/inflammatory response in that illness. Biol Psychiatry. 1997, 42: 349-358. 10.1016/S0006-3223(96)00365-4.

    CAS  PubMed  Google Scholar 

  123. Kubera M, Van Bockstaele D, Maes M: Leukocyte subsets in treatment-resistant major depression. Pol J Pharmacol. 1999, 51: 547-549.

    CAS  PubMed  Google Scholar 

  124. O'Brien SM, Scully P, Fitzgerald P, Scott LV, Dinan TG: Plasma cytokine profiles in depressed patients who fail to respond to selective serotonin reuptake inhibitor therapy. J Psychiatr Res. 2007, 41: 326-331. 10.1016/j.jpsychires.2006.05.013.

    PubMed  Google Scholar 

  125. Jacka FN, Maes M, Pasco JA, Williams LJ, Berk M: Nutrient intakes and the common mental disorders in women. J Affect Disord.

  126. Maes M, Yirmyia R, Noraberg J, Brene S, Hibbeln J, Perini G, Kubera M, Bob P, Lerer B, Maj M: The inflammatory & neurodegenerative (I&ND) hypothesis of depression: leads for future research and new drug developments in depression. Metab Brain Dis. 2009, 24: 27-53. 10.1007/s11011-008-9118-1.

    CAS  PubMed  Google Scholar 

  127. Maes M, Bosmans E, Calabrese J, Smith R, Meltzer HY: Interleukin-2 and interleukin-6 in schizophrenia and mania: effects of neuroleptics and mood stabilizers. J Psychiatr Res. 1995, 29: 141-152. 10.1016/0022-3956(94)00049-W.

    CAS  PubMed  Google Scholar 

  128. Maes M, Delange J, Ranjan R, Meltzer HY, Desnyder R, Cooremans W, Scharpé S: Acute phase proteins in schizophrenia, mania and major depression: modulation by psychotropic drugs. Psychiatry Res. 1997, 66: 1-11. 10.1016/S0165-1781(96)02915-0.

    CAS  PubMed  Google Scholar 

  129. Liu HC, Yang YY, Chou YM, Chen KP, Shen WW, Leu SJ: Immunologic variables in acute mania of bipolar disorder. J Neuroimmunol. 2004, 150: 116-122. 10.1016/j.jneuroim.2004.01.006.

    CAS  PubMed  Google Scholar 

  130. Wadee AA, Kuschke RH, Wood LA, Berk M, Ichim L, Maes M: Serological observations in patients suffering from acute manic episodes. Hum Psychopharmacol. 2002, 17: 175-179. 10.1002/hup.390.

    PubMed  Google Scholar 

  131. Maes M, Galecki P, Chang YS, Berk M: A review on the oxidative and nitrosative stress (O&NS) pathways in major depression and their possible contribution to the (neuro)degenerative processes in that illness. Prog Neuropsychopharmacol Biol Psychiatry. 2011, 35: 676-692. 10.1016/j.pnpbp.2010.05.004.

    CAS  PubMed  Google Scholar 

  132. Maes M, Mihaylova I, Leunis JC: Increased serum IgM antibodies directed against phosphatidyl inositol (Pi) in chronic fatigue syndrome (CFS) and major depression: evidence that an IgM-mediated immune response against Pi is one factor underpinning the comorbidity between both CFS and depression. Neuro Endocrinol Lett. 2007, 28: 861-867.

    PubMed  Google Scholar 

  133. Maes M, Mihaylova I, Kubera M, Leunis JC, Geffard M: IgM-mediated autoimmune responses directed against multiple neoepitopes in depression: new pathways that underpin the inflammatory and neuroprogressive pathophysiology. J Affect Disord. 2012, 135: 414-418.

    Google Scholar 

  134. Wichers MC, Koek GH, Robaeys G, Praamstra AJ, Maes M: Early increase in vegetative symptoms predicts IFN-alpha-induced cognitive-depressive changes. Psychol Med. 2005, 35: 433-441. 10.1017/S0033291704003526.

    CAS  PubMed  Google Scholar 

  135. Leonard BE, Myint A: Inflammation and depression: is there a causal connection with dementia?. Neurotox Res. 2006, 10: 149-160. 10.1007/BF03033243.

    CAS  PubMed  Google Scholar 

  136. Song C, Wang H: Cytokines mediated inflammation and decreased neurogenesis in animal models of depression. Prog Neuropsychopharmacol Biol Psychiatry. 2011, 35: 760-768. 10.1016/j.pnpbp.2010.06.020.

    CAS  PubMed  Google Scholar 

  137. Catena-Dell'Osso M, Bellantuono C, Consoli G, Baroni S, Rotella F, Marazziti D: Inflammatory and neurodegenerative pathways in depression: a new avenue for antidepressant development?. Curr Med Chem. 2011, 18: 245-255. 10.2174/092986711794088353.

    PubMed  Google Scholar 

  138. Gorwood P, Corruble E, Falissard B, Goodwin GM: Toxic effects of depression on brain function: impairment of delayed recall and the cumulative length of depressive disorder in a large sample of depressed outpatients. Am J Psychiatry. 2008, 165: 731-739. 10.1176/appi.ajp.2008.07040574.

    PubMed  Google Scholar 

  139. Lampe IK, Hulshoff Pol HE, Janssen J, Schnack HG, Kahn RS, Heeren TJ: Association of depression duration with reduction of global cerebral gray matter volume in female patients with recurrent major depressive disorder. Am J Psychiatry. 2003, 160: 2052-2054. 10.1176/appi.ajp.160.11.2052.

    PubMed  Google Scholar 

  140. McKinnon MC, Yucel K, Nazarov A, MacQueen GM: A meta-analysis examining clinical predictors of hippocampal volume in patients with major depressive disorder. J Psychiatry Neurosci. 2009, 34: 41-54.

    PubMed  PubMed Central  Google Scholar 

  141. Videbech P, Ravnkilde B: Hippocampal volume and depression: a meta-analysis of MRI studies. Am J Psychiatry. 2004, 161: 1957-1966. 10.1176/appi.ajp.161.11.1957.

    PubMed  Google Scholar 

  142. MacQueen GM, Campbell S, McEwen BS, Macdonald K, Amano S, Joffe RT, Nahmias C, Young LT: Course of illness, hippocampal function, and hippocampal volume in major depression. Proc Natl Acad Sci USA. 2003, 100: 1387-1392. 10.1073/pnas.0337481100.

    CAS  PubMed  PubMed Central  Google Scholar 

  143. Lacerda AL, Nicoletti MA, Brambilla P, Sassi RB, Mallinger AG, Frank E, Kupfer DJ, Keshavan MS, Soares JC: Anatomical MRI study of basal ganglia in major depressive disorder. Psychiatry Res. 2003, 124: 129-140. 10.1016/S0925-4927(03)00123-9.

    PubMed  Google Scholar 

  144. Stockmeier CA, Mahajan GJ, Konick LC, Overholser JC, Jurjus GJ, Meltzer HY, Uylings HB, Friedman L, Rajkowska G: Cellular changes in the postmortem hippocampus in major depression. Biol Psychiatry. 2004, 56: 640-650. 10.1016/j.biopsych.2004.08.022.

    PubMed  PubMed Central  Google Scholar 

  145. Drevets WC, Price JL, Furey ML: Brain structural and functional abnormalities in mood disorders: implications for neurocircuitry models of depression. Brain Struct Funct. 2008, 213: 93-118. 10.1007/s00429-008-0189-x.

    PubMed  PubMed Central  Google Scholar 

  146. Harrison NA, Brydon L, Walker C, Gray MA, Steptoe A, Critchley HD: Inflammation causes mood changes through alterations in subgenual cingulate activity and mesolimbic connectivity. Biol Psychiatry. 2009, 66: 407-414. 10.1016/j.biopsych.2009.03.015.

    PubMed  PubMed Central  Google Scholar 

  147. Koenigs M, Grafman J: The functional neuroanatomy of depression: distinct roles for ventromedial and dorsolateral prefrontal cortex. Behav Brain Res. 2009, 201: 239-243. 10.1016/j.bbr.2009.03.004.

    PubMed  PubMed Central  Google Scholar 

  148. Park S-M, Gaykema RPA, Goehler LE: How does immune challenge inhibit ingestion of palatable food? Systemic lipopolysaccharide modulates key nodal points of feeding neurocircuitry. Brain Behav Immun. 2008, 22: 1160-1172. 10.1016/j.bbi.2008.05.001.

    CAS  PubMed  PubMed Central  Google Scholar 

  149. Kauer-Sant'Anna M, Kapczinski F, Andreazza AC, Bond DJ, Lam RW, Young LT, Yatham LN: Brain-derived neurotrophic factor and inflammatory markers in patients with early- vs. late-stage bipolar disorder. Int J Neuropsychopharmacol. 2009, 12: 447-458. 10.1017/S1461145708009310.

    PubMed  Google Scholar 

  150. Jancsár SM, Leonard BE: The effects of antidepressant drugs on conditioned taste aversion learning of the olfactory bulbectomized rat. Neuropharmacology. 1981, 20: 1341-1345.

    PubMed  Google Scholar 

  151. Kumar RK, Wakefield D: Inflammation: chronic. eLS. 2010, DOI: 10.1002/9780470015902. a0000944. {ED Query: I couldn't find this ref. in PubMed so left it as is.}

    Google Scholar 

  152. Straub RH: Evolutionary medicine and chronic inflammatory state-known and new concepts in pathophysiology. J Mol Med (Berl). 2012, 90: 523-534. 10.1007/s00109-012-0861-8.

    Google Scholar 

  153. Jewkes RK, Dunkle K, Nduna M, Jama PN, Puren A: Associations between childhood adversity and depression, substance abuse and HIV and HSV2 incident infections in rural South African youth. Child Abuse Negl. 2010, 34: 833-841. 10.1016/j.chiabu.2010.05.002.

    PubMed  PubMed Central  Google Scholar 

  154. Pearce BD, Kruszon-Moran D, Jones JL: The relationship between Toxoplasma gondii infection and mood disorders in the Third National Health and Nutrition Survey. Biol Psychiatry.

  155. Maes M: An intriguing and hitherto unexplained co-occurrence: depression and chronic fatigue syndrome are manifestations of shared inflammatory, oxidative and nitrosative (IO&NS) pathways. Prog Neuropsychopharmacol Biol Psychiatry. 2011, 35: 784-794. 10.1016/j.pnpbp.2010.06.023.

    CAS  PubMed  Google Scholar 

  156. Owe-Larsson B, Säll L, Salamon E, Allgulander C: HIV infection and psychiatric illness. Afr J Psychiatry. 2009, 12: 115-128.

    CAS  Google Scholar 

  157. Maes M, Kubera M, Leunis JC, Berk M: Increased IgA and IgM responses against gut commensals in chronic depression: further evidence for increased bacterial translocation or leaky gut. J Affect Disord.

  158. Hassett AL, Radvanski DC, Buyske S, Savage SV, Sigal LH: Psychiatric comorbidity and other psychological factors in patients with "chronic Lyme disease". Am J Med. 2009, 122: 843-850. 10.1016/j.amjmed.2009.02.022.

    PubMed  PubMed Central  Google Scholar 

  159. Strijdom SC, Berk M: Lyme disease in South Africa. S Afr Med J. 1996, 86 (Suppl): 741-744.

    CAS  PubMed  Google Scholar 

  160. van den Pol AN: Viral infection leading to brain dysfunction: more prevalent than appreciated?. Neuron. 2009, 64: 17-20. 10.1016/j.neuron.2009.09.023.

    CAS  PubMed  PubMed Central  Google Scholar 

  161. Maes M, Song C, Lin A, DeJong R, Van Gastel A, Kenis G, Bosmans E, DeMeester I, Neels H, Janca A, Scharpe S, Smith RS: Immune and clinical correlates of psychological stress-induced production of interferon-γ and IL-10 in humans. Cytokines, Stress and Immunity. Edited by: Plotnikoff NP, Faith RE, Murgo AJ, Good RA. 1998, New York: Taylor and Francis, 39-50.

    Google Scholar 

  162. Wohleb ES, Hanke ML, Corona AW, Powell ND, Stiner LM, Bailey MT, Nelson RJ, Godbout JP, Sheridan JF: β-Adrenergic receptor antagonism prevents anxiety-like behavior and microglial reactivity induced by repeated social defeat. J Neurosci. 2011, 31: 6277-6288. 10.1523/JNEUROSCI.0450-11.2011.

    CAS  PubMed  PubMed Central  Google Scholar 

  163. Williams LJ, Pasco JA, Jacka FN, Henry MJ, Dodd S, Berk M: Depression and bone metabolism. A review. Psychother Psychosom. 2009, 78: 16-25. 10.1159/000162297.

    PubMed  Google Scholar 

  164. Pavlovićc Z, Delićc D, Marićc NP, Vukovićc O, Jašovićc-Gašićc M: Depressive symptoms in patients with hepatitis C treated with pegylated interferon alpha therapy: a 24-week prospective study. Psychiatr Danub. 2011, 23: 370-377.

    Google Scholar 

  165. Wichers MC, Koek GH, Robaeys G, Verkerk R, Scharpé S, Maes M: IDO and interferon-alpha-induced depressive symptoms: a shift in hypothesis from tryptophan depletion to neurotoxicity. Mol Psychiatry. 2005, 10: 538-544. 10.1038/sj.mp.4001600.

    CAS  PubMed  Google Scholar 

  166. Kendler KS, Thornton LM, Gardner CO: Genetic risk, number of previous depressive episodes, and stressful life events in predicting onset of major depression. Am J Psychiatry. 2001, 158: 582-586. 10.1176/appi.ajp.158.4.582.

    CAS  PubMed  Google Scholar 

  167. Laugeray A, Launay JM, Callebert J, Surget A, Belzung C, Barone PR: Evidence for a key role of the peripheral kynurenine pathway in the modulation of anxiety- and depression-like behaviours in mice: Focus on individual differences. Pharmacol Biochem Behav. 2011, 98: 161-168. 10.1016/j.pbb.2010.12.008.

    CAS  PubMed  Google Scholar 

  168. Wrynn AS, Mac Sweeney CP, Franconi F, Lemaire L, Pouliquen D, Herlidou S, Leonard BE, Gandon J, de Certaines JD: An in-vivo magnetic resonance imaging study of the olfactory bulbectomized rat model of depression. Brain Res. 2000, 879: 193-199. 10.1016/S0006-8993(00)02619-6.

    CAS  PubMed  Google Scholar 

  169. Wang D, Noda Y, Tsunekawa H, Zhou Y, Miyazaki M, Senzaki K, Nabeshima T: Behavioural and neurochemical features of olfactory bulbectomized rats resembling depression with comorbid anxiety. Behav Brain Res. 2007, 178: 262-273. 10.1016/j.bbr.2007.01.003.

    CAS  PubMed  Google Scholar 

  170. Huang Y, Henry CJ, Dantzer R, Johnson RW, Godbout JP: Exaggerated sickness behavior and brain proinflammatory cytokine expression in aged mice in response to intracerebroventricular lipopolysaccharide. Neurobiol Aging. 2008, 29: 1744-1753. 10.1016/j.neurobiolaging.2007.04.012.

    CAS  PubMed  Google Scholar 

  171. Nakanishi H, Hayashi Y, Wu Z: The role of microglial mtDNA damage in age-dependent prolonged LPS-induced sickness behavior. Neuron Glia Biol. 2011, 28: 1-7.

    CAS  Google Scholar 

  172. Taepavarapruk P, Song C: Reductions of acetylcholine release and nerve growth factor expression are correlated with memory impairment induced by interleukin-1beta administrations: effects of omega-3 fatty acid EPA treatment. J Neurochem. 2010, 112: 1054-1064. 10.1111/j.1471-4159.2009.06524.x.

    CAS  PubMed  Google Scholar 

  173. Lai AY, Swayze RD, El-Husseini A, Song C: Interleukin-1 beta modulates AMPA receptor expression and phosphorylation in hippocampal neurons. J Neuroimmunol. 2006, 175: 97-106. 10.1016/j.jneuroim.2006.03.001.

    CAS  PubMed  Google Scholar 

  174. Kinney DK, Tanaka M: An evolutionary hypothesis of depression and its symptoms, adaptive value, and risk factors. J Nerv Ment Dis. 1980, 97: 561-567.

    Google Scholar 

  175. Raison CL, Miller AH: The evolutionary significance of depression in Pathogen Host Defense (PATHOS-D). Mol Psychiatr. 2012, doi: 10.1038/mp.2012.2. PubMed PMID: 22290120

    Google Scholar 

  176. Olde Hartman TC, Borghuis MS, Lucassen PL, van de Laar FA, Speckens AE, van Weel C: Medically unexplained symptoms, somatisation disorder and hypochondriasis: course and prognosis. A systematic review. J Psychosom Res. 2009, 66: 363-377. 10.1016/j.jpsychores.2008.09.018.

    PubMed  Google Scholar 

  177. Xia Z, DePierre JW, Nassberger L: Tricyclic antidepressants inhibit IL-6, IL-1b and TNF-a release in human blood monocytes and IL-2 and interferon-g in T cells. Immunopharmacology. 1996, 34: 27-37. 10.1016/0162-3109(96)00111-7.

    CAS  PubMed  Google Scholar 

  178. Maes M, Song C, Lin AH, Bonaccorso S, Kenis G, De Jongh R, Bosmans E, Scharpe S: Negative immunoregulatory effects of antidepressants: inhibition of interferon-gamma and stimulation of interleukin-10 secretion. Neuropsychopharmacol. 1999, 20: 370-379. 10.1016/S0893-133X(98)00088-8.

    CAS  Google Scholar 

  179. Brustolim D, Ribeiro-dos-Santos R, Kast RE, Altschuler EL, Soares MB: A new chapter opens in anti-inflammatory treatments: the antidepressant bupropion lowers production of tumor necrosis factor-alpha and interferon-gamma in mice. Int Immunopharmacol. 2006, 6: 903-907. 10.1016/j.intimp.2005.12.007.

    CAS  PubMed  Google Scholar 

  180. Castanon N, Bluthé RM, Dantzer R: Chronic treatment with the atypical antidepressant tianeptine attenuates sickness behavior induced by peripheral but not central lipopolysaccharide and interleukin-1beta in the rat. Psychopharmacology (Berl). 2001, 154: 50-60. 10.1007/s002130000595.

    CAS  Google Scholar 

  181. Jiang Y, Deacon R, Anthony DC, Campbell SJ: Inhibition of peripheral TNF can block the malaise associated with CNS inflammatory diseases. Neurobiol Dis. 2008, 632: 125-132.

    Google Scholar 

  182. Maes M, Meltzer HY, Bosmans E, Bergmans R, Vandoolaeghe E, Ranjan R, Desnyder R: Increased plasma concentrations of interleukin-6, soluble interleukin-6, soluble interleukin-2 and transferrin receptor in major depression. J Affect Disord. 1995, 34: 301-309. 10.1016/0165-0327(95)00028-L.

    CAS  PubMed  Google Scholar 

  183. Maes M, Fišar Z, Medina M, Scapagnini G, Nowak G, Berk M: New drug targets in depression: inflammatory, cell-mediated immune, oxidative and nitrosative stress, mitochondrial, antioxidant, and neuroprogressive pathways. And new drug candidates-Nrf2 activators and GSK-3 inhibitors. Inflammopharmacology. 2012, 20: 127-150. 10.1007/s10787-011-0111-7.

    CAS  PubMed  Google Scholar 

  184. Hannestad J, DellaGioia N, Bloch M: The effect of antidepressant medication treatment on serum levels of inflammatory cytokines: a meta-analysis. Neuropsychopharmacology. 2011, 36: 2452-2459. 10.1038/npp.2011.132.

    CAS  PubMed  PubMed Central  Google Scholar 

  185. Kirsch I: Antidepressants and the placebo response. Epidemiol Psichiatr Soc. 2009, 18: 318-322.

    PubMed  Google Scholar 

  186. Tuma T: Outcome of hospital treated depression at 4.5 years. An elderly and a younger cohort compared. Br J Psychiatry. 2000, 176: 224-228. 10.1192/bjp.176.3.224.

    CAS  PubMed  Google Scholar 

  187. Twenge JM, Gentile B, DeWall CN, Ma D, Lacefield K, Schurtz DR: Birth cohort increases in psychopathology among young Americans, 1938-2007: A cross-temporal meta-analysis of the MMPI. Clin Psychol Rev. 2010, 30: 145-154. 10.1016/j.cpr.2009.10.005.

    PubMed  Google Scholar 

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Acknowledgements

The authors would like to thank Bruce Charlton for extensive discussion of the text.

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Authors and Affiliations

  1. Maes Clinics @ TRIA, Piyavate Hospital, 998 Rimklongsamsen Road, Bangkok, 10310, Thailand

    Michael Maes

  2. School of Medicine, Deakin University, Kitchener House, Ryrie Street, Geelong, Victoria, 3220, Australia

    Michael Berk

  3. Orygen Youth Health Research Centre, Centre for Youth Mental Health, 35 Poplar Road, Parkville Victoria, 3052, Parkville, Australia

    Michael Berk

  4. The Mental Health Research Institute of Victoria, Australia Kenneth Myer Building, 30 Royal Parade, Parkville, Victoria, 3052, Australia

    Michael Berk

  5. Department of Psychiatry, Melbourne University, Level 1, North Block Main Building Royal Melbourne Hospital, Parkville, Victoria, 3050, Australia

    Michael Berk

  6. Center for the Study of Complementary and Alternative Therapies, School of Nursing, University of Virginia, PO Box 800793, Charlottesville, VA, 22908, USA

    Lisa Goehler

  7. Department of Psychology and Neurosciences, Dalhousie University, 1355 Oxford Streeet, Halifax, B3H 4R2, Canada

    Cai Song

  8. Department of Pharmacology, Chinese Academy Engineering Instit ute for the Development of Endangered Medicinal Resources in Southwest China, Post Code 30023, 189 Changgang Road, Xing Ning District, Nanning, Guangxi, P.R. China

    Cai Song

  9. CRC, Rm 30, 57 Laurel street, Glasgow, G11 7QT, Scotland, UK

    George Anderson

  10. Department of Adult Psychiatry, Medical University of Łóź, Aleksandrowska 159, Łóź, 91-229, Poland

    Piotr Gałecki

  11. Department of Pharmacology, Galway University, University Road, Galway, Co.Galway, Ireland

    Brian Leonard

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Correspondence to Michael Maes.

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Competing interests

There was no financial support for this specific research.

MBk has received Grant/Research Support from the NIH, Cooperative Research Centre, Simons Autism Foundation, Cancer Council of Victoria, Stanley Medical Research Foundation, MBF, NHMRC, Beyond Blue, Geelong Medical Research Foundation, Bristol Myers Squibb, Eli Lilly, Glaxo SmithKline, Organon, Novartis, Mayne Pharma and Servier, has been a speaker for Astra Zeneca, Bristol Myers Squibb, Eli Lilly, Glaxo SmithKline, Janssen Cilag, Lundbeck, Merck, Pfizer, Sanofi Synthelabo, Servier, Solvayand Wyeth, and served as a consultant to Astra Zeneca, Bristol Myers Squibb, Eli Lilly, Glaxo SmithKline, Janssen Cilag, Lundbeck and Servier. The other authors declare that they have no competing interests.

Authors' contributions

MM and MB participated in the design of this review, while all authors helped to draft the paper. All authors contributed equally to this paper. All authors read and approved the final manuscript.

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Maes, M., Berk, M., Goehler, L. et al. Depression and sickness behavior are Janus-faced responses to shared inflammatory pathways. BMC Med 10, 66 (2012). https://doi.org/10.1186/1741-7015-10-66

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ISSN: 1741-7015

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