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The modulation of macrophage subsets in celiac disease pathogenesis

Sara Molaaghaee‐Rouzbahani, Nastaran Asri, Somayeh Jahani‐Sherafat, Davar Amani, Andrea Masotti, Kaveh Baghaei, Abbas Yadegar, Hamed Mirjalali, Mohammad Rostami‐Nejad

2022Immunity Inflammation and Disease14 citationsDOIOpen Access PDF

Abstract

BACKGROUND: So far, limited studies have focused on the role of Macrophages (MQs) in the development or progression of celiac disease (CD). Researchers believe that increasing knowledge about the function of MQs in inflammatory disorders plays a critical role in finding a new treatment for these kinds of diseases. MAIN BODY: CD is a permanent autoimmune intestinal disorder triggered by gluten exposure in predisposed individuals. This disorder happens due to the loss of intestinal epithelial barrier integrity characterized by dysregulated innate and adaptive immune responses. MQs are known as key players of the innate immune system that link innate and adaptive immunity. MQs of human intestinal lamina propria participate in maintaining tissue homeostasis, and also intestinal inflammation development. Previous studies suggested that gliadin triggers a proinflammatory phenotype (M1 MQ) in human primary MQs. Moreover, M2-related immunosuppressive mediators are also present in CD. In fact, CD patients present an impaired transition from pro-inflammatory to anti-inflammatory responses due to inappropriate responses to gliadin peptides. CONCLUSION: The M1/M2 MQs polarization balancing regulators can be considered novel therapeutic targets for celiac disease.

Topics & Concepts

ImmunologyInflammationImmune systemProinflammatory cytokineInnate immune systemMacrophage polarizationAcquired immune systemPathogenesisDiseaseLamina propriaMedicineImmunityInnate lymphoid cellPhenotypeBiologyInternal medicinePathologyGeneGeneticsEpitheliumCeliac Disease Research and ManagementLiver Diseases and ImmunityMicroscopic Colitis
The modulation of macrophage subsets in celiac disease pathogenesis | Litcius