Crinophagic Granules in Pancreatic β Cells Contribute to Mouse Autoimmune Diabetes by Diversifying Pathogenic Epitope Repertoire

Overview

Journal Nat Commun

Specialty Biology

Date 2024 Sep 27

PMID 39333495

Authors

Hao Hu

Anthony N Vomund

Orion J Peterson

Neetu Srivastava

Tiandao Li

Lisa Kain

Wandy L Beatty

Bo Zhang

Chyi-Song Hsieh

Luc Teyton

Cheryl F Lichti

Emil R Unanue

Xiaoxiao Wan

Affiliations

Soon will be listed here.

Abstract

Autoimmune attack toward pancreatic β cells causes permanent loss of glucose homeostasis in type 1 diabetes (T1D). Insulin secretory granules store and secrete insulin but are also thought to be tissue messengers for T1D. Here, we show that the crinophagic granules (crinosome), a minor set of vesicles formed by fusing lysosomes with the conventional insulin dense-core granules (DCG), are pathogenic in T1D development in mouse models. Pharmacological inhibition of crinosome formation in β cells delays T1D progression without affecting the dominant DCGs. Mechanistically, crinophagy inhibition diminishes the epitope repertoire in pancreatic islets, including cryptic, modified and disease-relevant epitopes derived from insulin. These unconventional insulin epitopes are largely undetectable in the MHC-II epitope repertoire of the thymus, where only canonical insulin epitopes are presented. CD4 T cells targeting unconventional insulin epitopes display autoreactive phenotypes, unlike tolerized T cells recognizing epitopes presented in the thymus. Thus, the crinophagic pathway emerges as a tissue-intrinsic mechanism that transforms insulin from a signature thymic self-protein to a critical autoantigen by creating a peripheral-thymic mismatch in the epitope repertoire.

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