Skip to main content
  • Research article
  • Open access
  • Published:

Chronic kidney disease in gout in a managed care setting

Abstract

Background

To study the prevalence of chronic kidney disease (CKD) and its impact on allopurinol dosing and uric acid control among patients with gout.

Methods

This was a retrospective study using data from a large US health plan. Claims and laboratory data were analyzed for enrollees from the health plan database from January 2002 through December 2005. Patients with gout were identified from pharmacy and medical claims data based on the presence of codes for gout medication or gout diagnosis. Severity of CKD was determined using the estimated glomerular filtration rate (eGFR). Allopurinol titration was defined as a change in average daily dose from first prescription to last prescription of ≥ 50 mg.

Results

A total of 3,929 patients were identified for inclusion in this study, 39% of whom had CKD (based on having an eGFR < 90 mL/min/1.73 m2). Subjects with CKD were older (p < 0.01) and more likely to be women (p < 0.01), had a greater number of comorbid conditions (p < 0.01), and were more likely to be prescribed allopurinol (p < 0.01) compared to those with no CKD. The average starting dose of allopurinol was lower among those with CKD, and it decreased with worsening kidney function. Among the 3,122 gout patients who used allopurinol, only 25.6% without CKD and 22.2% with CKD achieved a serum uric acid concentration of < 6.0 mg/dL (p = 0.0409). Also, only 15% of allopurinol users had an upward dose titration (by ≥50 mg), but the average increase in dose did not differ significantly between those with and without CKD.

Conclusions

About two out of every five patients with gout in this population had CKD. Allopurinol doses were not adjusted in the majority of CKD patients. Serum uric acid control in gout was poor among patients without CKD and even worse among those with CKD.

Peer Review reports

Background

Gouty arthritis (gout) is relatively common in the general population, with an estimated prevalence of 4%, and it is associated with approximately 3.9 million ambulatory care visits per year [1, 2]. Chronic kidney disease (CKD) is also common, affecting approximately 26 million adults in the United States over the age of 20 [3, 4]. Specific lifestyles choices can influence the risk of gout, but lifestyle changes may not be sufficient to manage disease after the onset of gout [5].

Gout patients typically exhibit increased levels of serum uric acid. It is recommended that serum uric acid levels be lowered to a target of < 6 mg/dL to better manage gout symptoms, and to reduce synovial MSU crystals and acute gout attacks [6]. Uric acid is excreted primarily through the kidney, and any impairment of kidney function can result in hyperuricemia. Even among individuals with normal renal function, the presence of hyperuricemia has been correlated with future incidence of renal impairment and increased healthcare utilization and costs [7, 8]. Treatment of gout in patients with CKD is complicated because full dosing of allopurinol, the uric acid-reducing medicine, requires adequate renal function to clear oxypurinol, its active metabolite [9]. It is recommended that patients with renal impairment should receive reduced doses of allopurinol, as they may be at increased risk for allopurinol-related toxicity [9]. However, suboptimal uric acid control has been associated with worsening renal function [1012].

Studies suggest that the prevalence of both gout and CKD are likely to increase over time [3, 4]. Although the vast majority of patients with gout in the United States seek treatment from primary care physicians [2], most studies of CKD in gout patients have been performed in other settings such as rheumatology clinics [1215], dialysis databases [16], and renal transplant centers [17, 18]. In the present study, a retrospective analysis was performed using a large US health plan database (and associated lab data) containing detailed information on gout diagnosis, urate-lowering therapy usage, and serum uric acid (sUA) levels. The objectives of this study were to determine the prevalence of CKD among a general population of gout patients in a normal practice setting, and to investigate the impact of CKD on allopurinol dosing and uric acid control.

Methods

Data source and study design

This was a retrospective analysis of medical and pharmacy claims data from a large managed health care plan in the United States affiliated with OptumInsight. Additional laboratory data for patients was also obtained for some analyses. During the period of this study (January 1, 2002 through December 31, 2005), the health plan covered approximately 14 million individuals, mainly in the United States. The data were used in a de-identified format that complied with the requirements of the Health Insurance Portability and Accountability Act (HIPAA).

Patient identification

This study included commercial health plan members at least 18 years of age. Ideally, a gout diagnosis would be based on the demonstration of intracellular urate crystals in an appropriate clinical setting, or on clinical or survey criteria published by the American College of Rheumatology [19, 20]. However, these approaches are not feasible in large retrospective studies such as this one. In this study, patients were considered to have gout and were selected for the study if they had a minimum of 2 qualifying claims (as described below) during the time period from January 2002 through December 2005. The first qualifying claim must have been a prescription claim for a gout medication (allopurinol, probenecid, colchicine, and/or sulfinpyrazone). The second qualifying claim may have been either a prescription claim for a gout medication or a medical claim with an International Classification of Diseases, Ninth Revision, Clinical Modification (ICD-9-CM) diagnosis code of 274.0. Patients were also required to have at least 1 serum creatinine laboratory result during the first 12 months of their follow-up period for study inclusion. Patients with evidence of dialysis, kidney transplant, and/or cancer during the study period were excluded from the analysis. To qualify patients were also required to be enrolled in the health plan for ≥ 365 days during a baseline period and for ≥ 365 days during a follow-up period.

Measurements of kidney function and uric acid

The Modification of Diet in Renal Disease (MDRD) study equation was applied to patients' serum creatinine levels to estimate the glomerular filtration rate (eGFR) [21]. The definition and stages of CKD used for the study are based on staging described by the National Kidney Foundation Kidney Disease Outcomes Quality Initiative (NKF KDOQI™, as found at http://www.kidney.org/professionals/kdoqi/guidelines_ckd/toc.htm), with modifications as described below. All patients with eGFR ≥90 were defined as having no CKD (information on kidney damage in the presence of normal eGFR was unavailable, so NKF Stage 1 disease was rolled into the "no CKD category"). Patients with NKF Stage 2 disease (eGFR 60-89), NKF Stage 3 disease (eGFR 30-59), or NKF Stage 4 disease (eGFR 15-29) were defined as having CKD and assigned to the Stage 2 (mild disease) category, the Stage 3 (moderate disease) category, or the Stage 4 (severe disease) category, respectively. Patients with NKF Stage 5 disease (kidney failure, eGFR < 15) were rolled into the Stage 4 (severe disease) category, due to small sample size. As some patients may have had more than one eGFR value, determination of CKD stage was based on the last eGFR value in the follow-up period. Follow-up eGFR was used instead of baseline eGFR because not all patients had a baseline GFR, and as renal function deteriorates over time, the follow-up eGFR was expected to classify patients by their most severe disease indicator.

Patients' serum uric acid levels were obtained from laboratory data. In accordance with available guidelines, a serum uric acid concentration < 6 mg/dL (< 0.36 mmol/L) was designated as the desirable goal for gout patients receiving urate reduction therapy [22]. Patients were stratified by CKD stage, and the proportion of patients at goal was determined.

Patient demographic and clinical characteristics

Patient demographic variables including age, gender, and geographic location were identified from the enrollment data. ICD-9-CM codes from medical claims were used to calculate scores for the Charlson-Deyo Comorbidity Index, a validated index of severity of comorbidity [23]. A validated comorbidity classification developed by Elixhauser and adopted by the US Agency for Healthcare Research and Quality (AHRQ) was used to examine gout-kidney disease relationships across comorbidity groups [24].

In a subset analysis, the proportion of gout patients receiving allopurinol prescriptions (medication fill rate) was evaluated. In addition, the allopurinol average daily dose was calculated at the time of initial observed dose and at the time of last observation. Patients were considered to have titrated their allopurinol dose if the absolute change in average daily dose from first prescription to last prescription was ≥ 50 mg. Additional analyses were conducted using a threshold of change in allopurinol dose of ≥100 mg to define therapy titration. Other medications for gout such as probenecid, colchicine, and sulfinpyrazone were used too infrequently in the study sample for meaningful analysis.

Data analysis

For univariate and bivariate analyses, Student's t-test and Pearson's chi-squared test, respectively, were used. For multivariable analyses designed to determine factors associated with changes in allopurinol dose, a logistic regression with occurrence of a dose change of ≥50 mg/day was used as the dependent variable. Independent variables included severity of CKD, age, gender, region of plan membership, thiazide use, preexisting comorbid conditions, and length of allopurinol therapy. All analyses were conducted using the SAS (version 9.0) software program (SAS Institute, Inc., Cary, North Carolina).

Results

Patient selection and characteristics

A total of 220,763 patients were initially identified from the health plan database, based on the presence of at least 1 medical claim for gout or 1 fill for gout medication between 1/1/02 and 12/31/05 (Figure 1). After application of age criteria, continuous enrollment criteria, and criteria requiring no cancer during baseline, 41,290 patients remained. Of these 41,290 patients, 19,828 met the study criteria for having gout. The sample was further reduced to only include patients with available serum creatinine results during the first 12 months of follow-up. After application of all inclusion and exclusion criteria, a final sample of 3,929 patients was selected for the study.

Figure 1
figure 1

Patient selection. A total of 220,763 patients with at least 1 medical claim for gout or 1 fill for gout medication between 1/1/02 and 12/31/05 were initially identified from the health plan database. After application of all inclusion and exclusion criteria, a final sample of 3,929 patients was selected for the study.

Of the 3,929 patients who met the inclusion criteria, 1,536 (39%) were identified as having CKD. In a sensitivity analysis using the first serum creatinine measurement during the first 12 months (rather than the last measurement), subject distribution among CKD stages was similar. More than half (67.2%) of the subjects with CKD had Stage 2 CKD, 23.2% had Stage 3 CKD, and 9.6% had Stage 4 CKD (Table 1). CKD subjects were older (p < 0.0001) and more likely to be female (p = 0.0082) than those without CKD (Table 1). CKD patients had a greater number of comorbid conditions (p < 0.0001) and a higher Charlson-Deyo Comorbidity Index score (p < 0.0001) as compared to subjects without CKD. The five most common comorbid conditions observed in both patients with CKD and those without CKD were hypertension (67.6% of CKD patients vs. 48.5% of non-CKD patients); dyslipidemia (54.2% vs. 45.1%); non-gout arthropathies (35.4% vs. 34.4%); cardiovascular diseases (32.5% vs. 25.6%); and diabetes mellitus (25.8% vs. 16.4%). There was not a statistically significant difference in the length of follow-up between patients with CKD and those without CKD.

Table 1 Patient characteristics at baseline

Serum uric acid levels and allopurinol use

A total of 3,122 gout patients used allopurinol at least once during the study period (79% of the study population). Only 77.5% of patients without CKD were prescribed allopurinol, compared to 80.0% of patients with Stage 2 CKD, 87.4% of patients with Stage 3 CKD, and 87.8% of patients with Stage 4 CKD. However, the mean follow-up serum uric acid level among allopurinol users with CKD was significantly higher than for allopurinol users without CKD (7.11 mg/dL vs. 6.75 mg/dL; p < 0.0001) (Table 2). Further, 25.6% of allopurinol users without CKD as compared to only 22.2% of allopurinol users with CKD reached the serum uric acid goal of < 6.0 mg/dL during the follow-up period (p = 0.0409).

Table 2 Serum uric acid lab results

The mean initial dose of allopurinol decreased significantly with increasing severity of CKD (Table 3). Patients with Stage 2 CKD had a mean initial allopurinol dose of 249.0 mg/day, compared to 233.8 mg/day for patients with Stage 3 CKD and 217.6 mg/day for patients with Stage 4 CKD. The majority of patients who used allopurinol did not titrate their medication dose during the study period. Only about 14.6% of patients without CKD and 15.6% of patients with CKD had a dose titration. Although there was no significant difference in likelihood of dose titration between all patients with CKD vs. those without CKD (p = 0.45), patients with Stage 4 CKD were significantly more likely to have a dose titration compared to patients without CKD (p < 0.0001). Titration of dose upwards was more common than titration of dose downwards, both among patients with CKD and those without CKD (Table 3). We compared initial daily dose of allopurinol to the maintenance doses recommended by Hande et al. [9] using eGFR as a surrogate for creatinine clearance (Table 4). We found that 95.6% of subjects with an eGFR 100 or higher had an initial dose that did not exceed the recommended maintenance dose; however, this percentage was only 33.3% for eGFR 20-99, and 1.2% for eGFR0-19.

Table 3 Allopurinol use
Table 4 Adherence to allopurinol dosing guidelines

Multivariable logistic regression analysis was used to assess factors associated with titration (Table 5). Adjusting for covariates, patients with severe CKD had a significantly higher likelihood of dose titration compared to allopurinol users without CKD (odds ratio [OR] 2.130, 95% confidence interval [95% CI]: 1.380 - 3.289). Other factors associated with dose titration were thiazide use during follow-up (OR 1.301, 95% CI 1.035 - 1.635) and a higher pre-index Charlson-Deyo Comorbidity Index score (OR 1.164, 95% CI 1.059 - 1.279). Increased age was associated with a decreased odds of dose titration (OR 0.973, 95% CI 0.962 - 0.985). Results using a threshold for titration of ≥100 mg were similar.

Table 5 Multivariate models predicting an average allopurinol dose change ≥50 mg/day

Discussion

The prevalence of CKD in the US general population is approximately 13% [3]. This retrospective study reveals a very high prevalence of CKD (approximately 40%) among gout patients in the US. A previous smaller study of gout patients in New Zealand found a level of CKD prevalence similar to what is reported here [25]. In the present study, gout patients with severe renal disease were somewhat older and more likely to be female and to have a greater overall comorbidity burden. As expected, serum uric acid concentrations were higher among those with worse renal disease. Although individuals with CKD were treated more frequently, they received lower initial doses of allopurinol. Over time, the average allopurinol dose among patients with gout increased regardless of the presence or severity of renal disease. The magnitude of increase among those with renal disease was smaller but statistically indistinguishable from those with normal renal function. Thus, the treatment received by those with normal renal function was not substantially more aggressive than the treatment received by those with impaired renal function.

Within each cohort, patients who used allopurinol had lower serum uric acid levels than patients who did not use allopurinol. However, a significant finding of this study was the relatively low proportion of patients treated with allopurinol who achieved a serum uric acid concentration of < 6 mg/dL (25.6% of patients without CKD, 23.3% of those with Stage 2 CKD, 20.2% of those with Stage 3 CKD, and 18.8% of those with Stage 4 CKD). Although goal attainment was low among all patient cohorts, presence of CKD decreased the likelihood of meeting this benchmark even further. Further, a low percentage of patients with CKD (only about 16%) had their allopurinol dosage titrated. These findings highlight the therapeutic challenge of balancing the risks and benefits of administering allopurinol to patients with impaired renal function.

Appropriate dosing of allopurinol when CKD is present is an important yet controversial topic. The US Food and Drug Administration has approved the following dosing regimen for gout without concurrent renal disease [26]: Start with a dose of 100 mg/day and increase by 100 mg/day at weekly intervals until the desired therapeutic response is achieved. A maximum dose of 800 mg/day is permitted. However, in a Japanese study, patients achieved a therapeutic serum concentration of oxypurinol (> 4.6 mcg/mL) and a clinical response rate of > 90% at an allopurinol dose of just 100-200 mg/day [27]. Dosing in this study was based on levels of serum creatinine, not on eGFR. Others have raised concerns about the safety of higher doses of allopurinol, and using serum creatinine as an index for allopurinol dosing has been shown to be less safe than using eGFR [28]. Adhering to the current guidelines for dosing allopurinol based on eGFR, on the other hand, does not necessarily result in desired uric acid control [9, 29, 30]. The results of the managed care analysis performed here reflect this therapeutic challenge.

Our findings do not indicate that initial daily dose of allopurinol is prescribed in a manner that correlates with published guidelines sensitive to renal function. The original guidelines for allopurinol dosing were based on an extensive review of severe adverse reactions to allopurinol and a small de novo study of 40 patients [9]. That study calculated that renal clearance of oxypurinol was directly proportional to the creatinine clearance, which was calculated using the Cockroft-Gault formula. The recommended dosing levels were based on achieving a target serum oxypurinol level of 30-100 mmol/L and not on avoiding any toxicity threshold. In another study based on data from a rheumatology practice, there were modest correlations between allopurinol doses and plasma oxypurinol concentrations, and between creatinine clearance and plasma oxypurinol [30]. However, there was no correlation between plasma oxypurinol and plasma uric acid, and only 50% of patients within the therapeutic range of plasma oxypurinol had a plasma uric acid level < 0.42 mmol/L [30]. Collectively, these findings suggest that there is considerable heterogeneity in drug handling, and future studies need to test the underlying assumption that oxypurinol is the sole active metabolite responsible for therapeutic efficacy and toxicity. Concerns regarding adverse events in particular may influence the aggressiveness of current treatment regimens. Cutaneous adverse reactions to allopurinol occur in approximately 7.7 per 1000 recipients [31], and the incidence of allopurinol hypersensitivity syndrome is about 2-3 times higher among renally impaired patients compared to non-renally impaired patients [32]. However, the relationship between adverse events and allopurinol dosing is still not fully understood. Previous studies have shown that patients receiving doses of allopurinol above the recommended dose (as based on the creatinine clearance rate) did not exhibit increased toxicity [33, 34]. Other studies have indicated that specific genetic markers may influence the risk of experiencing severe cutaneous adverse reactions following allopurinol treatment [35].

A few caveats must be considered when interpreting the results of the present study: (1) The approach used to identify gout patients from claims data is subject to misclassification errors. This problem was addressed by performing sensitivity analyses that specified different combinations of coding, medications, and laboratory criteria as alternate selection criteria. The resulting patient populations varied in terms of size and other characteristics, but the fundamental findings in this analysis held. (2) Because of the requirement of availability of a serum creatinine test, the current study population may have been less renally healthy than other populations of gout patients. This factor could reduce the generalizability of the findings. (3) The authors studied patients with gout seeking medical care, thereby potentially selecting those with more severe or frequent flare-ups of gout; this, in turn, may have overestimated the prevalence of CKD among gout patients. (4) The multivariate model examining allopurinol dose change did not distinguish between dose increases or decreases. This would be a valuable direction for future research. (5) A limitation of claims analysis is that we are only able to measure prescribed doses, which may differ from the dose that a patient actually took.

Conclusion

In this study a high prevalence of CKD was observed among gout patients. Serum uric acid goal attainment was low among patients treated with allopurinol, and poorest among those with CKD. The findings suggest that poor outcomes among gout patients with CKD are partly due to clinicians' reluctance to prescribe higher doses of allopurinol to patients with impaired renal function. The benefits and risks of allopurinol treatment must be weighed carefully in patients with CKD, and alternate treatment approaches are needed to improve the prognosis of these patients. Future research should address at least three additional issues: (1) the role of non-oxypurinol metabolites of allopurinol in efficacy and toxicity, (2) more sophisticated pharmacogenomics-based studies of allopurinol dosing in the presence of CKD, and (3) development of urate-lowering drugs that are not renally cleared. Additionally, our results suggest a need to raise awareness among physicians regarding the importance of titrating therapy to reach uric acid goals.

Abbreviations

AHRQ:

Agency for Healthcare Research and Quality

CKD:

chronic kidney disease

eGFR:

glomerular filtration rate

HIPAA:

Health Insurance Portability and Accountability Act

ICD-9-CM:

International Classification of Diseases, Ninth Revision, Clinical Modification

MDRD:

Modification of Diet in Renal Disease

NKF KDOQI:

National Kidney Foundation Kidney Disease Outcomes Quality Initiative

sUA:

serum uric acid

References

  1. Mikuls TR, Saag KG: New insights into gout epidemiology. Curr Opin Rheumatol. 2006, 18: 199-203. 10.1097/01.bor.0000209435.89720.7c.

    Article  PubMed  Google Scholar 

  2. Krishnan E, Lienesch D, Kwoh CK: Gout in ambulatory care settings in the United States. J Rheumatol. 2008, 35: 498-501.

    PubMed  Google Scholar 

  3. Coresh J, Selvin E, Stevens LA, Manzi J, Kusak JW, Eggers P, Van Lente F, Levey AS: Prevalence of chronic kidney disease in the United States. JAMA. 2007, 298: 2038-47. 10.1001/jama.298.17.2038.

    Article  CAS  PubMed  Google Scholar 

  4. Wallace KL, Riedel AA, Joseph-Ridge N, Wortmann R: Increasing prevalence of gout and hyperuricemia over 10 years among older adults in a managed care population. J Rheumatol. 2004, 31: 1582-7.

    PubMed  Google Scholar 

  5. Choi HK, Curhan G: Gout: epidemiology and lifestyle choices. Curr Opin Rheumatol. 2005, 17: 341-5.

    Article  PubMed  Google Scholar 

  6. Shoji A, Yamanaka H, Kamatani N: A retrospective study of the relationship between serum urate level and recurrent attacks of gouty arthritis: evidence for reduction of recurrent gouty arthritis with antihyperuricemic therapy. Arthritis Rheum. 2004, 51: 321-325. 10.1002/art.20405.

    Article  CAS  PubMed  Google Scholar 

  7. Avram Z, Krishnan E: Hyperuricaemia--where nephrology meets rheumatology. Rheumatology (Oxford). 2008, 47: 960-964. 10.1093/rheumatology/ken070.

    Article  CAS  Google Scholar 

  8. Wu EQ, Patel PA, Yu AP, Mody RR, Cahill KE, Tang J, Krishnan E: Disease-related and all-cause health care costs of elderly patients with gout. J Manag Care Pharm. 2008, 14: 164-75.

    PubMed  Google Scholar 

  9. Hande KR, Noone RM, Stone WJ: Severe allopurinol toxicity: Description and guidelines for prevention in patients with renal insufficiency. Am J Med. 1984, 76: 47-56.

    Article  CAS  PubMed  Google Scholar 

  10. Chonchol M, Shlipak MG, Katz R, Sarnak MJ, Newman AB, Siscovick DS, Kestenbaum B, Carney JK, Fried LF: Relationship of uric acid with progression of kidney disease. Am J Kidney Dis. 2007, 50: 239-47. 10.1053/j.ajkd.2007.05.013.

    Article  CAS  PubMed  Google Scholar 

  11. Weiner DE, Tighiouart H, Elsayed EF, Griffith JL, Salem DN, Levey AS: Uric acid and incident kidney disease in the community. J Am Soc Nephrol. 2008, 19: 1204-11. 10.1681/ASN.2007101075.

    Article  CAS  PubMed  PubMed Central  Google Scholar 

  12. Gibson T, Rodgers V, Potter C, Simmonds HA: Allopurinol treatment and its effect on renal function in gout: a controlled study. Ann Rheum Dis. 1982, 41: 59-65. 10.1136/ard.41.1.59.

    Article  CAS  PubMed  PubMed Central  Google Scholar 

  13. Perez-Ruiz F, Calabozo M, Herrero-Beites AM, García-Erauskin G, Pijoan JI: Improvement of renal function in patients with chronic gout after proper control of hyperuricemia and gouty bouts. Nephron. 2000, 86: 287-91. 10.1159/000045783.

    Article  CAS  PubMed  Google Scholar 

  14. Alvarez-Nemegyei J, Cen-Piste JC, Medina-Escobedo M, Villanueva-Jorge S: Factors associated with musculoskeletal disability, and chronic renal failure in clinically diagnosed primary gout. J Rheumatol. 2005, 32: 1923-7.

    PubMed  Google Scholar 

  15. Vecchio PC, Emmerson BT: Gout due to renal disease. Br J Rheumatol. 1992, 31: 63-5. 10.1093/rheumatology/31.1.63.

    Article  CAS  PubMed  Google Scholar 

  16. Cohen SD, Kimmel PL, Neff R, Agodoa L, Abbott KC: Association of incident gout and mortality in dialysis patients. J Am Soc Nephrol. 2008, 19: 2204-10. 10.1681/ASN.2007111256.

    Article  PubMed  PubMed Central  Google Scholar 

  17. Sparta G, Kemper MJ, Neuhaus TJ: Hyperuricemia and gout following pediatric renal transplantation. Pediatr Nephrol. 2006, 21: 1884-8. 10.1007/s00467-006-0257-5.

    Article  PubMed  Google Scholar 

  18. Stamp L, Ha L, Searle M, O'Donnel J, Frampton C, Chapman P: Gout in renal transplant recipients. Nephrology (Carlton). 2006, 11: 367-71. 10.1111/j.1440-1797.2006.00577.x.

    Article  CAS  Google Scholar 

  19. Wallace SL, Robinson H, Masi AT, Decker JL, McCarty DJ, Yü TF: Preliminary criteria for the classification of the acute arthritis of primary gout. Arthritis Rheum. 1977, 20: 895-900. 10.1002/art.1780200320.

    Article  CAS  PubMed  Google Scholar 

  20. Harrold LR, Saag KG, Yood RA, Mikuls TR, Andrade SE, Fouayzi H, Davis J, Chan KA, Raebel MA, Von Worley A, Platt R: Validity of gout diagnoses in administrative data. Arthritis Rheum. 2007, 57: 103-8. 10.1002/art.22474.

    Article  PubMed  Google Scholar 

  21. Levey AS, Bosch JP, Lewis JB, Greene T, Rogers N, Roth D: A more accurate method to estimate glomerular filtration rate from serum creatinine: a new prediction equation. Modification of Diet in Renal Disease Study Group. Ann Intern Med. 1999, 130: 461-70.

    Article  CAS  PubMed  Google Scholar 

  22. Zhang W, Doherty M, Bardin T, Pascual E, Barskova V, Conaghan P, Gerster J, Jacobs J, Leeb B, Liot F, McCarthy G, Netter P, Nuki G, Perez-Ruiz F, Pignone A, Piment OJ, Punzi L, Roddy E, Uhlig T, Zimmerman-Górska I: EULAR evidence based recommendations for gout. Part II: Management. Report of a task force of the EULAR Standing Committee for International Clinical Studies Including Therapeutics (ESCISIT). Ann Rheum Dis. 2006, 65: 1312-24. 10.1136/ard.2006.055269.

    Article  CAS  PubMed  PubMed Central  Google Scholar 

  23. Charlson ME, Pompei P, Ales KL, MacKenzie CR: A new method of classifying prognostic comorbidity in longitudinal studies: Development and validation. J Chronic Dis. 1987, 40: 373-83. 10.1016/0021-9681(87)90171-8.

    Article  CAS  PubMed  Google Scholar 

  24. Elixhauser A, Steiner C, Harris DR, Coffey RM: Comorbidity measures for use with administrative data. Med Care. 1998, 36: 8-27. 10.1097/00005650-199801000-00004.

    Article  CAS  PubMed  Google Scholar 

  25. Kumar S, Gow P: A survey of indications, results and complications of surgery for tophaceous gout. N Z Med J. 2002, 115: U109-

    PubMed  Google Scholar 

  26. Anonymous: Product Monograph: Zyloprim, allopurinol tablets USP. Mississauga, ON, Canada. 2006

    Google Scholar 

  27. Takada M, Okada H, Kotake T, Kawato N, Saito M, Nakai M, Gunji T, Shibakawa M: Appropriate dosing regimen of allopurinol in Japanese patients. J Clin Pharm Ther. 2005, 30: 407-12. 10.1111/j.1365-2710.2005.00670.x.

    Article  CAS  PubMed  Google Scholar 

  28. Perez-Ruiz F, Hernando I, Villar I, Nolla JM: Correction of allopurinol dosing should be based on clearance of creatinine, but not plasma creatinine levels: another insight to allopurinol-related toxicity. J Clin Rheumatol. 2005, 11: 129-33. 10.1097/01.rhu.0000164822.98163.22.

    Article  PubMed  Google Scholar 

  29. Dalbeth N, Kumar S, Stamp L, Gow P: Dose adjustment of allopurinol according to creatinine clearance does not provide adequate control of hyperuricemia in patients with gout. J Rheumatol. 2006, 33: 1646-50.

    CAS  PubMed  Google Scholar 

  30. Stamp L, Gow P, Sharples K, Raill B: The optimal use of allopurinol: an audit of allopurinol use in South Auckland. Aust N Z J Med. 2000, 30: 567-72.

    Article  CAS  PubMed  Google Scholar 

  31. Bigby M, Jick S, Jick H, Arndt K: Drug-induced cutaneous reactions. A report from the Boston Collaborative Drug Surveillance Program on 15,438 consecutive inpatients, 1975 to 1982. JAMA. 1986, 256: 3358-63. 10.1001/jama.256.24.3358.

    Article  CAS  PubMed  Google Scholar 

  32. Khanna D, Pandya BJ, D'Souza AO, Meissner BL, Kamalaker R, Harikrishnan V: Incidence of allopurinol hypersensitivity syndrome (AHS) among renally impaired patients [abstract]. Arthritis Rheum. 2009, 60 (Suppl 10): 2043-

    Google Scholar 

  33. Stamp LK, O'Donnell JL, Zhang M, James J, Frampton C, Barclay ML, Chapman PT: Using allopurinol above the dose based on creatinine clearance is effective and safe in patients with chronic gout, including those with renal impairment. Arthritis Rheum. 2011, 63: 412-21. 10.1002/art.30119.

    Article  CAS  PubMed  Google Scholar 

  34. Vázquez-Mellado J, Morales EM, Pacheco-Tena C, Burgos-Vargas R: Relation between adverse events associated with allopurinol and renal function in patients with gout. Ann Rheum Dis. 2001, 60: 981-3. 10.1136/ard.60.10.981.

    Article  PubMed  PubMed Central  Google Scholar 

  35. Hung SI, Chung WH, Liou LB, Chu CC, Lin M, Huang HP, Lin YL, Lan JL, Yang LC, Hong HS, Chen MJ, Lai PC, Wu JY, Chen YT: HLA-B*5801 allele as a genetic marker for severe cutaneous adverse reactions caused by allopurinol. Proc Natl Acad Sci. 2005, 102: 4134-9. 10.1073/pnas.0409500102.

    Article  CAS  PubMed  PubMed Central  Google Scholar 

Pre-publication history

Download references

Acknowledgements

This study was sponsored by Takeda Pharmaceuticals International, Inc. Editorial assistance was provided by Manel Valdes-Cruz, Takeda Pharmaceuticals North America, Inc., and by Jesse Potash, OptumInsight.

Author information

Authors and Affiliations

Authors

Corresponding author

Correspondence to Victoria Zarotsky.

Additional information

Competing interests

This study was funded by Takeda Pharmaceuticals International, Inc. (TPI), Deerfield, IL. (TAP Pharmaceutical Products Inc. is now a part of TPI.) Dr. Krishnan has received grant support from Takeda Pharmaceuticals International, Inc. (TPI), and has held stock in Savient Pharmaceuticals. He has served as an advisor/consultant for both of these companies. Proprietary products manufactured by these companies are not named/discussed in this manuscript. Dr Krishnan is supported in part from a Research Starter Grant from the PhRMA Foundation and a career development grant from the American College of Rheumatology Research and Education Foundation. Dr. Pandya is an employee of Takeda Pharmaceuticals International, Inc., and Dr Fuldeore was previously employed by TAP Pharmaceutical Products, Inc., and now works for Abbott Laboratories. Drs Riedel and Zarotsky are employees of OptumInsight.

Authors' contributions

MF, AR, VZ, BP, OD, and EK participated in the design of the study and helped to draft the manuscript. All authors have read and approved this manuscript.

Authors’ original submitted files for images

Below are the links to the authors’ original submitted files for images.

Authors’ original file for figure 1

Rights and permissions

Open Access This article is published under license to BioMed Central Ltd. This is an Open Access article is distributed under the terms of the Creative Commons Attribution License ( https://creativecommons.org/licenses/by/2.0 ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Reprints and permissions

About this article

Cite this article

Fuldeore, M.J., Riedel, A.A., Zarotsky, V. et al. Chronic kidney disease in gout in a managed care setting. BMC Nephrol 12, 36 (2011). https://doi.org/10.1186/1471-2369-12-36

Download citation

  • Received:

  • Accepted:

  • Published:

  • DOI: https://doi.org/10.1186/1471-2369-12-36

Keywords