Introduction
Fibromyalgia (FM) is a syndrome defined by widespread pain for longer than 3 months and by the presence of ≥11 of 18 tender points
Researchers have suggested that many of the symptoms reported by women with silicone gel-filled breast implants appear to be similar to those observed in patients with FM
Because of the suggested similarities between FM and reported symptoms by patients with silicone gel-filled breast implants, one of us examined the association of APA and FM and found that 47% of patients in a general rheumatological setting in the United States were seropositive for the presence of APA
In light of these results, we examined the APA levels in a cohort of Italian FM patients and investigated their association with disease severity and cytokine levels. To determine whether APA results from a generalized autoimmune response, the APA seroreactivity was evaluated also in several autoimmune disease noncase groups including rheumatoid arthritis, Sjögren's syndrome, systemic sclerosis, systemic lupus erythematosus and undifferentiated connective-tissue disease.
Materials and methods
Patients
We recruited 285 consecutive patients (270 females, 15 males) affected by primary FM as assessed by the 1990 American College of Rheumatology criteria
For each patient the tenderness at tender points was evaluated by means of the Fischer dolorimeter
To estimate the impact of FM on the quality of life, all patients and control individuals received a Fibromyalgia Impact Questionnaire
All patients were asked whether they had frequently suffered any of the following symptoms
We arbitrarily classified the FM severity on the basis of the tender point count: the presence of 11 tender points was considered mild severity, the presence of 14–16 tender points as moderate and the presence of more than 16 tender points was designated severe.
Antipolymer antibody and interleukin assay
APA levels were determined on serum samples by an indirect ELISA kit that detects IgG APA (Corgenix, Westminster, CO, USA), according to the manufacturer's instructions. Diluted serum samples, calibrator and control samples were incubated in polymer-coated microwells. After the removal of unbound proteins by washing, specific antibodies for human IgG labelled with horseradish peroxidase were added, forming complexes with the polymer-bound antibodies. The bound enzyme–antibody conjugate was assayed by the addition of a single solution containing tetramethylbenzidine and hydrogen peroxide as the chromogenic substrate. Colour develops in the wells at an intensity proportional to the concentration of APA. Results were obtained by reading the optical density at 450 nm. The measure of the optical density was converted in the sample unit using a conversion factor. All the samples were tested in duplicate, and a result of more 30 U was considered positive, as suggested by the manufacturer.
Cytokines (IL-1, IL-6, IL-8, IL-10 and TNFα) were measured by ELISA in plasma (Bender MedSystem, Austria, Vienna). A polyclonal antibody-coating antibody is adsorbed onto microwells, and the cytokine present in the samples or standards binds to antibodies adsorbed to the microwells. A biotin-conjugated monoclonal antibody directed to cytokine is added and binds to cytokine captured by the first antibody. Streptavidin–horseradish peroxidase is added and binds to the biotin-conjugated cytokine. Unbound streptavidin–horseradish peroxidase is removed during a washing step, and substrate solution reactive with horseradish peroxidase is added to the wells. A coloured product is formed in proportion to the amount of cytokine present in the sample. The reaction is terminated by addition of acid and the absorbance is measured at 450 nm. A standard curve is prepared from seven cytokine standard dilutions and the cytokine sample concentration is determined.
Statistical analysis
Data were analysed by means of nonparametric statistical methods using Kruskal–Wallis analysis of variance, Spearman's correlation, Student's
Results
Demographic and clinical data of the 285 FM patients are presented in Table
Demographic characteristics, clinical characteristics and antipolymer antibody (APA) levels of 285 fibromyalgia patients.
All fibromyalgia patients
Patients with APA >30 U
Patients with APA <30 U
Gender (females/males)
270/15
57/3
213/12
Age (years) (median (range))
54 (19–82)
46 (19–74)
56 (20–82)
Tender points
14.29 ± 0.29
13.88 ± 0.83
14.30 ± 0.34
Tender Point Index
2.17 ± 0.04
2.17 ± 0.12
2.19 ± 0.04
Onset disease
9.19 ± 0.60
8.77 ± 1.19
10.11 ± 0.67
Fibromyalgia Impact Questionnaire
58.21 ± 1.22
55.89 ± 2.59
58.46 ± 1.39
Tiredness
6.96 ± 0.17
7.16 ± 0.41
6.88 ± 0.19
Pain
6.80 ± 0.17
6.31 ± 0.42
6.87 ± 0.18
Results expressed as the mean ± standard error of the mean. The Tender Point Index was calculated as the sum of each positive tender point score divided by the total number of tender points.
Antipolymer antibody levels in fibromyalgia patients and in control individuals
Antipolymer antibody levels in fibromyalgia patients and in control individuals. Antipolymer antibody (APA) levels in fibromyalgia (FM) patients (all patients and patients separated according to disease severity) and in control individuals. SEM, standard error of the mean.
Considering a cut-off value of 30 U, APA-positive values were detected in 60 FM patients (21.05%) and in 15 healthy control individuals (15.00%) without significant differences in seropositivity among them.
Patients with moderate (19.17 ± 4.44) and severe symptoms (25.05 ± 4.42) had slightly higher APA levels with respect to patients with mild symptoms (13.18 ± 2.01) (Figure
A negative correlation between APA levels and age was found both in FM patients (
Considering the subset of FM patients with positive APA, significant correlations were found between APA levels versus the Fibromyalgia Impact Questionnaire (
Patients with positive APA levels showed a lower percentage of constipation (26% versus 42%,
No differences in cytokine levels were detected between FM patients with mild, moderate or severe symptoms or between those FM patients with APA-positive/negative values. A significant correlation was found, however, between APA levels and IL-1 values within the subset of patients with positive APA (
Correlation between antipolymer antibody and IL-1 levels
Correlation between antipolymer antibody and IL-1 levels. Correlation between antipolymer antibody (APA) and IL-1 levels in the subgroup of fibromyalgia patients with APA >30 U.
APA seroreactivity results were low (7.7%) in the autoimmune noncase group.
Discussion
The production of APA antibodies may result from an immunological response to self-antigens or to environmental agents, such as medications, silicone, or other chemicals, which results in the formation of antibodies cross-reacting with partially polymerized acrylamide. Because it has been shown that APA antibodies are present in about 50% of patients with silicone breast implants, and the highest prevalence of APA is found in implant patients with severe symptoms of a FM-like syndrome
Our objective was to examine the presence of APA seropositivity in 285 nonimplanted FM patients and to verify whether APA levels correlate with disease severity and with cytokine levels.
We did not find differences of seropositivity between FM patients and control individuals but did observe that patients with moderate and severe symptoms exhibited qualitatively higher levels of APA, even if not statistically significant, with respect to patients with mild symptoms. Lee and colleagues
Wilson and colleagues
Interestingly, in our study the APA levels correlated with Fibromyalgia Impact Questionnaire estimates and tiredness results in the subset of seropositive patients, so APA correlated with the severity of the disease only when it is positive. This is the first study reporting an association between APA seropositivity and the Fibromyalgia Impact Questionnaire.
Like other reports
We found a low prevalence of APA seroactivity in the noncase group that is about one-half of that found in FM patients. This result is in accordance with a precedent work
Conclusion
We have shown that APA cannot be considered a marker of disease in Italian FM patients. Its presence, however, might permit the identification of a subset of FM patients with more severe symptoms and who may respond differently to different therapeutic strategies. APA seroactivity is also not a general marker for autoimmune disease processes.
Abbreviations
APA = antipolymer antibody; ELISA = enzyme-linked immunosorbent assay; FM = fibromyalgia; IL = interleukin; TNF = tumour necrosis factor.
Competing interests
The authors declare that they have no competing interests.
Authors' contributions
LB conceived of the study, its design and coordination, evaluated the clinical parameters and helped to draft the manuscript. CG, FDF and TG performed the laboratory assays. AR performed the statistical analysis and drafted the manuscript. MD and CT participated in the evaluation of clinical parameters. RBW provided the kit and helped to draft the manuscript. SB participated in the design of the study. All authors read and approved the final manuscript.