| Literature DB >> 29186691 |
Charles St-Pierre1, Erwan Morgand2, Mohamed Benhammadi1, Alexandre Rouette1, Marie-Pierre Hardy3, Louis Gaboury4, Claude Perreault5.
Abstract
The sole nonredundant role of the thymic medulla is to induce central tolerance, a vital process that depends on promiscuous gene expression (pGE), a unique feature of medullary thymic epithelial cells (mTECs). Although pGE enhances transcription of >3,000 genes in mTECs, its impact on the regulation of protein homeostasis remains unexplored. Here, we report that, because of pGE, mature mTECs synthesize substantially more proteins than other cell types and are exquisitely sensitive to loss of immunoproteasomes (IPs). Indeed, IP deficiency causes proteotoxic stress in mTECs and leads to exhaustion of postnatal mTEC progenitors. Moreover, IP-deficient mice show accelerated thymic involution, which is characterized by a selective loss of mTECs and multiorgan autoimmune manifestations. We conclude that pGE, the quintessential feature of mTECs, is a major burden for the maintenance of proteostasis, which is alleviated by the constitutive expression of IPs in mTECs.Entities:
Keywords: autoimmunity; immunoproteasomes; promiscuous gene expression; proteotoxic stress; self-tolerance; thymic epithelial cells; thymic involution
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Year: 2017 PMID: 29186691 DOI: 10.1016/j.celrep.2017.10.121
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423