Biologic Agents in Crohn's Patients Reduce CD4 + T Cells Activation and Are Inversely Related to Treg Cells.
Eliane Aparecida Rosseto-WelterLeticia D'argenio-GarciaFilipa Blasco Tavares Pereira LopesAna Eduarda Zulim CarvalhoFernando FlaquerVanessa Severo-LemosClaudia Concer Viero NoraFlavio SteinwurzLucas Pires Garcia OliveriaThiago AloiaLuiz Vicente RizzoCristóvão Luis Pitangueira MangueiraKarina Inacio CarvalhoPublished in: Canadian journal of gastroenterology & hepatology (2022)
Crohn's disease (CD) is a chronic inflammatory disease with a complex interface of broad factors. There are two main treatments for Chron's disease: biological therapy and nonbiological therapy. Biological agent therapy (e.g., anti-TNF) is the most frequently prescribed treatment; however, it is not universally accessible. In fact, in Brazil, many patients are only given the option of receiving nonbiological therapy. This approach prolongs the subsequent clinical relapse; however, this procedure could be implicated in the immune response and enhance disease severity. Our purpose was to assess the effects of different treatments on CD4 + T cells in a cohort of patients with Crohn's disease compared with healthy individuals. To examine the immune status in a Brazilian cohort, we analyzed CD4 + T cells, activation status, cytokine production, and Treg cells in blood of Crohn's patients. Patients that underwent biological therapy can recover the percentage of CD4 + CD73 + T cells, decrease the CD4 + T cell activation/effector functions, and maintain the peripheral percentage of regulatory T cells. These results show that anti-TNF agents can improve CD4 + T cell subsets, thereby inducing Crohn's patients to relapse and remission rates.