AI Article Synopsis

  • - In type 1 diabetes, CD8+ T cells that target insulin-producing β cells in the pancreas are involved in the destruction of these cells, but the role of similar T cells found in the blood is not well understood.
  • - A study tracked different circulating β cell-reactive CD8+ T cell subsets and β cell function for 2 years post-diagnosis, finding a positive correlation between certain T cells (CD57+ memory T cells) and insulin levels in kids under 12.
  • - The research suggests that changes in these specific T cells can reflect the body's ability to produce insulin, indicating their potential use for monitoring the immune response and as a target for future treatments in type 1 diabetes.

Article Abstract

In type 1 diabetes, cytotoxic CD8+ T cells with specificity for β cell autoantigens are found in the pancreatic islets, where they are implicated in the destruction of insulin-secreting β cells. In contrast, the disease relevance of β cell-reactive CD8+ T cells that are detectable in the circulation, and their relationship to β cell function, are not known. Here, we tracked multiple, circulating β cell-reactive CD8+ T cell subsets and measured β cell function longitudinally for 2 years, starting immediately after diagnosis of type 1 diabetes. We found that change in β cell-specific effector memory CD8+ T cells expressing CD57 was positively correlated with C-peptide change in subjects below 12 years of age. Autoreactive CD57+ effector memory CD8+ T cells bore the signature of enhanced effector function (higher expression of granzyme B, killer-specific protein of 37 kDa, and CD16, and reduced expression of CD28) compared with their CD57- counterparts, and network association modeling indicated that the dynamics of β cell-reactive CD57+ effector memory CD8+ T cell subsets were strongly linked. Thus, coordinated changes in circulating β cell-specific CD8+ T cells within the CD57+ effector memory subset calibrate to functional insulin reserve in type 1 diabetes, providing a tool for immune monitoring and a mechanism-based target for immunotherapy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6063477PMC
http://dx.doi.org/10.1172/JCI120555DOI Listing

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