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Endotypes in T1D: B lymphocytes and early onset

Mia J. Smith, John C. Cambier, Peter A. Gottlieb

2020Current Opinion in Endocrinology Diabetes and Obesity27 citationsDOIOpen Access PDF

Abstract

PURPOSE OF REVIEW: Although type 1 diabetes (T1D) is characterized by destruction of the pancreatic beta cells by self-reactive T cells, it has become increasingly evident that B cells also play a major role in disease development, likely functioning as antigen-presenting cells. Here we review the biology of islet antigen-reactive B cells and their participation in autoimmune diabetes. RECENT FINDINGS: Relative to late onset, individuals who develop T1D at an early age display increased accumulation of insulin-reactive B cells in islets. This B-cell signature is also associated with rapid progression of disease and responsiveness to B-cell depletion therapy. Also suggestive of B-cell participation in disease is loss of anergy in high-affinity insulin-reactive B cells. Importantly, loss of anergy is seen in patient's healthy first-degree relatives carrying certain T1D risk alleles, suggesting a role early in disease development. SUMMARY: Recent studies indicate that islet-reactive B cells may play a pathogenic role very early in T1D development in young patients, and suggest utility of therapies that target these cells.

Topics & Concepts

ImmunologyDiseaseAutoimmunityIsletB cellAntigenMedicineBiologyDiabetes mellitusImmune systemInternal medicineEndocrinologyAntibodyDiabetes and associated disordersPancreatic function and diabetesT-cell and B-cell Immunology
Endotypes in T1D: B lymphocytes and early onset | Litcius