Risk of hospitalised infection in rheumatoid arthritis patients receiving biologics following a previous infection while on treatment with anti-TNF therapy
作者: Huifeng Yun , Fenglong Xie , Elizabeth Delzell , Lang Chen , Emily B Levitan
DOI: 10.1136/ANNRHEUMDIS-2013-204011
关键词: Sepsis 、 Adalimumab 、 Rheumatoid arthritis 、 Infliximab 、 Surgery 、 Abatacept 、 Internal medicine 、 Medicine 、 Respiratory tract infections 、 Rituximab 、 Etanercept 、 Immunology 、 General Biochemistry, Genetics and Molecular Biology 、 Immunology and Allergy 、 Rheumatology
摘要: BackgroundThe risk of subsequent infections in rheumatoid arthritis (RA) patients who receive biologic therapy after a serious infection is unclear.ObjectiveTo compare the subsequent risk of hospitalised infections associated with specific biologic agents among RA patients previously hospitalised for infection while receiving anti-tumour necrosis factor (anti-TNF) therapy.MethodsUsing 2006–2010 Medicare data for 100% of beneficiaries with RA enrolled in Medicare, we identified patients hospitalised with an infection while on anti-TNF agents. Follow-up began 61 days after hospital discharge and ended at the earliest of: next infection, loss of Medicare coverage or 18 months after start of follow-up. We calculated the incidence rate of subsequent hospitalised infection for each biologic and used Cox regression to control for potential confounders.Results10 794 eligible hospitalised infections among 10183 unique RA patients who contributed at least 1 day of biologic exposure during follow-up. We identified 7807 person-years of exposure to selected biologics—333 abatacept, 133 rituximab and 7341 anti-TNFs (1797 etanercept, 1405 adalimumab, 4139 infliximab)—and 2666 associated infections. Mean age across biologic exposure cohorts was 64–69 years. The crude incidence rate of subsequent hospitalised infection ranged from 27.1 to 34.6 per 100 person-years. After multivariable adjustment, abatacept (HR: 0.80, 95% CI 0.64 to 0.99) and etanercept (HR: 0.83, 95% CI 0.72 to 0.96) users had significantly lower risks of subsequent infection compared to infliximab users.ConclusionsAmong RA patients who experienced a hospitalised infection while on anti-TNF therapy, abatacept and etanercept were associated with the lowest risk of subsequent infection compared to other biologic therapies.
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highwire.org参考文章(27)
Robert J. Glynn, Joshua J. Gagne, Sebastian Schneeweiss, Role of disease risk scores in comparative effectiveness research with emerging therapies. Pharmacoepidemiology and Drug Safety. ,vol. 21, pp. 138- 147 ,(2012) , 10.1002/PDS.3231
Jasvinder A Singh, Daniel E Furst, Aseem Bharat, Jeffrey R Curtis, Arthur F Kavanaugh, Joel M Kremer, Larry W Moreland, James O'Dell, Kevin L Winthrop, Timothy Beukelman, S Louis Bridges Jr, W Winn Chatham, Harold E Paulus, Maria Suarez‐Almazor, Claire Bombardier, Maxime Dougados, Dinesh Khanna, Charles M King, Amye L Leong, Eric L Matteson, John T Schousboe, Eileen Moynihan, Karen S Kolba, Archana Jain, Elizabeth R Volkmann, Harsh Agrawal, Sangmee Bae, Amy S Mudano, Nivedita M Patkar, Kenneth G Saag, None, 2012 Update of the 2008 American College of Rheumatology recommendations for the use of disease‐modifying antirheumatic drugs and biologic agents in the treatment of rheumatoid arthritis Arthritis Care and Research. ,vol. 64, pp. 625- 639 ,(2012) , 10.1002/ACR.21641
Sebastian Schneeweiss, Soko Setoguchi, Michael E. Weinblatt, Jeffrey N. Katz, Jerry Avorn, Paul E. Sax, Raisa Levin, Daniel H. Solomon, Anti–tumor necrosis factor α therapy and the risk of serious bacterial infections in elderly patients with rheumatoid arthritis Arthritis & Rheumatism. ,vol. 56, pp. 1754- 1764 ,(2007) , 10.1002/ART.22600
Jeffrey R. Curtis, Nivedita Patkar, Aiyuan Xie, Carolyn Martin, Jeroan J. Allison, Michael Saag, Deborah Shatin, Kenneth G. Saag, Risk of serious bacterial infections among rheumatoid arthritis patients exposed to tumor necrosis factor alpha antagonists. Arthritis & Rheumatism. ,vol. 56, pp. 1125- 1133 ,(2007) , 10.1002/ART.22504
Jeffrey R. Curtis, Juan Xi, Nivedita Patkar, Aiyuan Xie, Kenneth G. Saag, Carolyn Martin, Drug-specific and time-dependent risks of bacterial infection among patients with rheumatoid arthritis who were exposed to tumor necrosis factor α antagonists Arthritis & Rheumatism. ,vol. 56, pp. 4226- 4227 ,(2007) , 10.1002/ART.23050
Daniel E. Furst, The Risk of Infections with Biologic Therapies for Rheumatoid Arthritis Seminars in Arthritis and Rheumatism. ,vol. 39, pp. 327- 346 ,(2010) , 10.1016/J.SEMARTHRIT.2008.10.002
D. Y. Lin, L. J. Wei, The Robust Inference for the Cox Proportional Hazards Model Journal of the American Statistical Association. ,vol. 84, pp. 1074- 1078 ,(1989) , 10.1080/01621459.1989.10478874
Carlos G. Grijalva, Lang Chen, Elizabeth Delzell, John W. Baddley, Timothy Beukelman, Kevin L. Winthrop, Marie R. Griffin, Lisa J. Herrinton, Liyan Liu, Rita Ouellet-Hellstrom, Nivedita M. Patkar, Daniel H. Solomon, James D. Lewis, Fenglong Xie, Kenneth G. Saag, Jeffrey R. Curtis, Initiation of tumor necrosis factor-α antagonists and the risk of hospitalization for infection in patients with autoimmune diseases JAMA. ,vol. 306, pp. 2331- 2339 ,(2011) , 10.1001/JAMA.2011.1692
Kimme L. Hyrich, Mark Lunt, Kath D. Watson, Deborah P. M. Symmons, Alan J. Silman, , Outcomes after switching from one anti-tumor necrosis factor alpha agent to a second anti-tumor necrosis factor alpha agent in patients with rheumatoid arthritis: results from a large UK national cohort study. Arthritis & Rheumatism. ,vol. 56, pp. 13- 20 ,(2007) , 10.1002/ART.22331
Ahmed Fathy, Ahmed M. Dewedar, Medhat A. Shalaby, Sulaiman Al-Homaid, Ahmed M. Mahfouz, Osama A. Shams, Lack of adverse effect of anti-tumor necrosis factor-α biologics in treatment of rheumatoid arthritis: 5 years follow-up. International Journal of Rheumatic Diseases. ,vol. 15, pp. 330- 335 ,(2012) , 10.1111/J.1756-185X.2012.01715.X