Exposure to sequestered self-antigens in vivo is not sufficient for the induction of autoimmune diabetes.

Nobuyuki Ono,Salim Dhanji,Thomas Calzascia,Pamela S Ohashi,Kiichi Murakami,Håkan Hall,Alisha R Elford,Patty Yen,David M Spencer,Olivia Chan,Pierre Bobé

doi:10.1371/journal.pone.0173176

Abstract

Although the role of T cells in autoimmunity has been explored for many years, the mechanisms leading to the initial priming of an autoimmune T cell response remain enigmatic. The ‘hit and run’ model suggests that self-antigens released upon cell death can provide the initial signal for a self-sustaining autoimmune response. Using a novel transgenic mouse model where we could induce the release of self-antigens via caspase-dependent apoptosis. We tracked the fate of CD8+ T cells specific for the self-antigen. Our studies demonstrated that antigens released from apoptotic cells were cross-presented by CD11c+ cells in the draining lymph node. This cross-presentation led to proliferation of self-antigen specific T cells, followed by a transient ability to produce IFN-γ, but did not lead to the development of autoimmune diabetes. Using this model we examined the consequences on T cell immunity when apoptosis was combined with dendritic cell maturation signals, an autoimmune susceptible genetic background, and the deletion of Tregs. The results of our study demonstrate that autoimmune diabetes cannot be initiated by the presentation of antigens released from apoptotic cells in vivo even in the presence of factors known to promote autoimmunity.

Highlights

Over the years, the field of autoimmunity has gained insights into mechanisms of tolerance, regulatory pathways and genes that have an impact on the development of autoimmunity
Our results suggest that antigens derived from apoptotic cells are capable of activating autoreactive CD8 T cells but is insufficient to promote autoimmune diabetes
The results of this study provide evidence that the release of self-antigen from apoptotic cells can be presented to T cells, but this encounter leads to T cell tolerance and is not sufficient to induce self-sustaining autoimmune diabetes

Summary

Introduction

The field of autoimmunity has gained insights into mechanisms of tolerance, regulatory pathways and genes that have an impact on the development of autoimmunity. The underlying events that lead to the initiation of an autoimmune T cell response remain unclear. One mechanism that has been proposed is known as the ‘hit and run hypothesis’[1, 2], which suggests that infection, trauma, or injury to a particular tissue leads to cell death and the release of normally sequestered self-antigens. This process is believed to be a key PLOS ONE | DOI:10.1371/journal.pone.0173176. Sequestered self-antigens are not immunogenic in vivo http://www.chairs-chaires.gc.ca). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript

Methods

Results

Conclusion