Diabetes and Other Comorbidities in Rheumatoid Arthritis Patients Starting a Biologic DMARD: A Multi-Database Cohort Study

Seoyoung C. Kim^1,2, Yinzhu Jin³, Gregory Brill⁴, Jennifer Lewey^4,5, Nam-Kyong Choi³, Elisabetta Patorno⁴ and Rishi J. Desai³, ¹Rheumatology, Immunology and Allergy and Pharmacoepidemiology and Pharmacoeconomics, Brigham and Women’s Hospital, Boston, MA, ²Pharmacoepidemiology and Pharmacoeconomics, Brigham and Women’s Hospital, Boston, MA, ³Division of Pharmacoepidemiology and Pharmacoeconomics, Brigham and Women’s Hospital, Boston, MA, ⁴Division of Pharmacoepidemiology and Pharmacoeconomics, Brigham and Women’s Hospital/Harvard Medical School, Boston, MA, ⁵Division of Cardiology, Columbia University Medical Center, New York, NY

Meeting: 2016 ACR/ARHP Annual Meeting

Date of first publication: September 28, 2016

Keywords: diabetes and rheumatoid arthritis (RA), DMARDs

Session Information

Date: Sunday, November 13, 2016

Title: Epidemiology and Public Health - Poster I

Session Type: ACR Poster Session A

Session Time: 9:00AM-11:00AM

Background/Purpose: Patients with rheumatoid arthritis (RA) are known to have an increased comorbidity burden. Presence of diabetes or other comorbidities such as cardiovascular disease (CVD) may affect the treatment decisions for RA. Limited information is available regarding biologic initiation patterns in RA patients with various comorbid conditions. We aimed to compare the frequency of diabetes and other comorbidities in RA patients starting different classes of biologic DMARDs.

Methods: Using longitudinal claims data from Medicaid (2000-2010), Medicare (2008-2013) and a commercial health plan (MarketScan 2006-2015), we conducted a cohort study that included RA patients who initiated a biologic DMARD. We included 3 categories of biologic DMARDs: 1) TNF inhibitors (TNFi), 2) abatacept and 3) other biologics including rituximab, tocilizumab and tofacitinib. Patients were required to be naive to all biologic DMARDs for at least 365 days prior to the date of the 1^st biologic drug dispensing (i.e., index date). We assessed the prevalence of diabetes and other comorbidities in the 365-day period prior to the index date in each data source.

Results: There were a total of 148,584 biologic DMARD initiators: 25,878 in Medicaid, 40,663 in Medicare and 81,831 in MarketScan. Mean age (SD) in years was 46.8 (12.0) in Medicaid, 73.1 (6.3) in Medicare and 53.7 (13.0) in MarketScan. Over 75% were female. Across all three databases, 115,903 (78%) started a TNFi, 13,547 (9%) abatacept and 18,922 (13%) other biologics. Diabetes was common, affecting 22.8% in Medicaid, 35.3% in Medicare and 17.7% in MarketScan. Hypertension (36.1-78.6%), hyperlipidemia (21.3-67.7%), coronary heart disease (8.3-30.0%), heart failure (2.7-14.7%) and other cardiovascular comorbidities were common in all three databases. Compared to abatacept or other biologic initiators, TNFi initiators were younger and had a lower proportion of CV comorbidities including coronary heart disease, heart failure, stroke, and atrial fibrillation and malignancy at baseline. Differences in diabetes prevalence across treatment groups were less pronounced (Table).

Conclusion: Diabetes and CV comorbidities were common in RA patients starting a biologic DMARD across all three databases. Cardiovascular comorbidity profile was different in TNFi initiators compared to initiators of abatacept or other biologics. Our findings highlight the need for future research accounting for these differences appropriately in comparative effectiveness and safety studies of biologic DMARDs in multimorbid RA patients to inform treatment decisions.

Table. Baseline characteristics of different biologic starters
		TNFi	Abatacept	Other biologics
N
	Medicaid	24,647	498	733
	Medicare	25,792	6,107	8,764
	MarketScan	65,464	6,942	9,425
Age, years
	Medicaid	46.8±11.9	48.7±12.0*	48.1±12.6*
	Medicare	72.6±6.1	73.8±6.3*	74.2±6.6*
	MarketScan	52.8±12.9	56.9±13.0*	57.9±13.1*
Diabetes
	Medicaid	22.6%	24.1%	30.0%*
	Medicare	35.5%	34.8%	35.3%
	MarketScan	16.9%	19.8%*	21.7%*
Coronary heart disease
	Medicaid	8.8%	11.2%	12.8%*
	Medicare	28.2%	31.6%*	34.2%*
	MarketScan	7.3%	12.3%*	12.6%*
Heart failure
	Medicaid	4.2%	6.0%*	10.8%*
	Medicare	12.7%	17.4%*	18.8%*
	MarketScan	2.0%	5.2%*	6.2%*
Stroke
	Medicaid	2.2%	3.8%*	4.1%*
	Medicare	6.7%	7.2%	7.9%*
	MarketScan	1.7%	2.7%*	3.3%*
Atrial fibrillation
	Medicaid	1.1%	2.2%*	2.7%*
	Medicare	10.3%	14.1%*	15.4%*
	MarketScan	2.2%	4.4%*	5.4%*
Hypertension
	Medicaid	35.6%	41.2%*	50.0%*
	Medicare	78.2%	80.3%*	78.9%
	MarketScan	36.5%	44.2%*	48.0%*
Hyperlipidemia
	Medicaid	21.1%	23.7%	26.1%*
	Medicare	67.3%	69.3%*	68.0%
	MarketScan	29.9%	34.3%*	36.4%*
Malignancy
	Medicaid	3.5%	3.6%	26.9%*
	Medicare	14.6%	16.9%*	48.3%*
	MarketScan	5.6%	9.2%*	24.4%*
*p<0.05 compared to TNFi

Disclosure: S. C. Kim, Pfizer, Lilly, Genentech, AstraZeneca, and Bristol-Myers Squibb, 2; Y. Jin, None; G. Brill, None; J. Lewey, None; N. K. Choi, National Research Foundation of Korea (NRF-2014R1A1A2058601 and NRF-2015K2A1A2070210), 2; E. Patorno, None; R. J. Desai, None.

To cite this abstract in AMA style:

Kim SC, Jin Y, Brill G, Lewey J, Choi NK, Patorno E, Desai RJ. Diabetes and Other Comorbidities in Rheumatoid Arthritis Patients Starting a Biologic DMARD: A Multi-Database Cohort Study [abstract]. Arthritis Rheumatol. 2016; 68 (suppl 10). https://acrabstracts.org/abstract/diabetes-and-other-comorbidities-in-rheumatoid-arthritis-patients-starting-a-biologic-dmard-a-multi-database-cohort-study/. Accessed .

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