Regional risk of and viral hepatitis with tumor necrosis factor-alpha inhibitor treatment: A systematic review.

Front Pharmacol

Lydia Becker Institute of Immunology and Inflammation, Manchester Incubator Building, University of Manchester, Manchester, United Kingdom.

Published: January 2023

AI Article Synopsis

  • TNFα inhibitors help treat autoimmune diseases, but they can lead to infections like tuberculosis (TB) and hepatitis B, so doctors recommend screening patients for these infections.
  • A study looked at over 140,000 patients using TNFα inhibitors to see how many developed TB and hepatitis B, finding that cases were much higher in places like Asia and Africa compared to Europe and North America.
  • The researchers concluded that most infections happen in areas where TB and hepatitis B are common, suggesting that doctors should focus on checking patients based on the risk in their area instead of testing everyone.

Article Abstract

TNFα inhibitors are regularly used to treat autoimmune diseases. Tuberculosis (TB) and viral hepatitis B are considered potential infectious complications, and screening and surveillance are therefore recommended. Current guidelines do not take into account regional differences in endemicity of these infections. A systematic literature review of TB and viral hepatitis in patients receiving TNFα-inhibitors was performed, searching in PubMed, Embase, MEDLINE and Web of Science databases. Studies were selected against predefined eligibility criteria and assessed using the Newcastle-Ottawa scale. The number of TB and viral hepatitis cases/1,000 TNFα-inhibitor patients were evaluated, and regional variation compared. 105 observational studies involving over 140,000 patients were included. Overall, 1% of patients developed TB or viral hepatitis B. TB cases/1,000 TNFα-inhibitor patients were 4-fold higher in Asia, Africa, and South America than in Europe, North America, and Australasia where only 0%-0.4% of patients developed TB. Hepatitis B cases/1,000 patients were over 15-fold higher in countries with high prevalence (China, Taiwan, South Korea, Thailand) compared with low prevalence ( < 0.00001) where only 0.4% of patients developed hepatitis B. Only three of 143 patients developed viral hepatitis C, and there was insufficient data to allow regional sub-analysis. TB and viral hepatitis B infections in patients treated with TNFα inhibitors are largely confined to countries with high prevalence of these infections. As only 1/2,500 patients in low prevalence countries treated with TNFα inhibitors develop TB or viral hepatitis B, we suggest an individualized, risk-based approach, rather than universal screening for all patients.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9894886PMC
http://dx.doi.org/10.3389/fphar.2023.1046306DOI Listing

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