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Objectives
- Tumor necrosis factor-alpha (TNF-α) inhibitors may improve insulin sensitivity and thus would be expected to reduce the risk of diabetes mellitus (diabetes) in patients with rheumatoid arthritis (RA).
- This study examined the association of TNF-α inhibitor use and the risk of developing diabetes in an RA inception cohort in a tertiary health system using Electronic Health Records (EHR).
Methods
- All adult individuals diagnosed with RA between 1/1/2001 – 3/31/2008 were identified (n=1539). RA was defined as ICD-9 code 714.0 at >e; 2 outpatient encounters with a rheumatologist, and diagnosis was validated against the American College of Rheumatology criteria by manual review of 100 random charts (97% concordance).
- Prevalentcasesof diabetes,definedas1ormoreoutpatientvisits with ICD-9 250, a non-fasting blood glucose >e; 200 mg/dl, hemoglobin A1C≥7,orahypoglycemicmedicationorder, wereexcluded(n=252).
- Information on demographic data, medical history, body mass index (BMI), laboratory measures and medications were collected at office visits TNF-α inhibitor use was modeled as time-varying but for descriptive comparison purposes classified into ever or never usage.
- The outcome was incident diabetes, defined by the 2010 American Diabetes Association criteria.
- Time-varying Cox Proportional Hazard regression models were used to adjust for gender, age, race, hypertension, BMI, positive rheumatoid factor (RF) and anti-cyclic citrullinated peptide antibodies (anti-CCP), erythrocyte sedimentation rate, C- reactive protein (CRP), non-steroidal anti-inflammatory drugs (NSAID), glucocorticoid, hydroxychloroquine and methotrexate use. Medication use was considered continuous for lapses <e; 90 days.
Results
- 1287 non-diabetic incident RA patients were included in the analysis. Patients were predominantly women (73%), and 97% were Caucasian, with median age of 61 years and BMI 28.6 kg/m2. RF and anti-CCP were positive in 80% and 53%, respectively.
- Patients in the ever TNF-α inhibitor use group (n=403) had a lower median age but higher median BMI and CRP levels and were more likely to have positive anti-CCP antibodies and to have taken NSAIDs, glucocorticoids or methotrexate and less likey to have been on hydroxychloroquine.
- Median follow-up time (last visit or diabetes diagnosis date) for the ever- and never-TNF-α inhibitor users was 36.3 months and 23.9 months, respectively (p < .001). The median duration of TNF-α inhibitor exposure was 35.2 months.
- Of the 56 cases developing diabetes during observation, 15 were ever and 41 were never TNF-α inhibitor users, yielding incidence rates of 10.5 and 22.0 per 1000 person-years (p=0.020), respectively.
- Adjusting for covariates, the hazard ratio for incident diabetes for TNF-α inhibitor usage was 0.40 (95% confidence interval 0.16-0.99, p=0.046) compared to non-use.
Characteristics of RA Patients by TNF-α Inhibitor Usage
|
Overall
n=1287 |
Never users of TNF-α Inhibitor
n=884 |
Ever Users of TNF-α Inhibitor
n=403 |
P-value |
| Age (median) |
61
(51-73) |
64
(53-76) |
57
(48-65) |
<.001 |
| Female gender |
942
(73%) |
655
(74%) |
287
(71%) |
.280 |
| White race |
1247
(97%) |
863
(98%) |
384
(95%) |
.025 |
| BMI (median) |
228.6
(24.8-32.8) |
228.1
(24.7-32.0) |
229.4
(25.5-34.7) |
.001 |
| Hypertension |
613
(48%) |
434
(49%) |
179
(44%) |
.119 |
| Hyperlipidemia |
295
(23%) |
221
(25%) |
74
(18%) |
.009 |
| RF positive |
653
(80%) |
426
(78%) |
227
(84%) |
.062 |
| CCP positive |
240
(53%) |
149
(50%) |
91
(60%) |
.044 |
| Max ESR (median) |
29
(14-48) |
28
(14-47) |
30
(14-49) |
.181 |
| Max CRP (median) |
8.1
(2.8-21) |
7.0
(2.3-19.1) |
9.2
(3.4-23) |
.045 |
| NSAIDs |
971
(76%) |
652
(74%) |
319
(79%) |
0.037 |
| Glucocorticoids |
1117
(87%) |
739
(84%) |
378
(94%) |
<0.001 |
| Methotrexate |
768
(60%) |
475
(54%) |
293
(73%) |
<0.001 |
| Hydroxychloroquine |
432
(34%) |
315
(36%) |
117
(29%) |
0.020 |
Conclusion
- In this inception RA cohort, the use of TNF-α inhibitors was associated with a 60% reduction in risk of developing diabetes after adjusting for confounders.
- These novel findings have important implications in the treatment of this group of patients at high risk for cardiovascular disease.
References
- Gonzalez-Gay MA et al. Anti-tumor necrosis factor-alpha blockade improvesinsulin resistance in patients with rheumatoid arthritis. Clin Exp Rheumatol 2006;24(1):83-6.
- Seriolo B et al Effects of etanercept or infliximab treatment on lipid profile and insulin resistance in patients with refractory rheumatoid arthritis. Clin Rheumatol 2007;26(10):1799-800
- Rosenvinge A et al. Insulin resistance inpatients with rheumatoid arthritis: effect of anti-TNFalpha therapy. Scand J Rheumatol 2007;36(2):91-6
- Kiortsis DNet al. Effects of infliximab treatment on insulin resistance in patients with rheumatoid arthritis and ankylosing spondylitis. Ann Rheum Dis 2005; 64(5):765-6
- Tam LS et al. Impact of TNF inhibition on insulin resistance and lipids levels in patients with rheumatoid arthritis. Clin Rheumatol 2007;26(9):1495-8.
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