| Literature DB >> 29351844 |
Denisse Sepulveda1, Diego Rojas-Rivera1, Diego A Rodríguez2, Jody Groenendyk3, Andres Köhler4, Cynthia Lebeaupin5, Shinya Ito6, Hery Urra1, Amado Carreras-Sureda1, Younis Hazari1, Mireille Vasseur-Cognet7, Maruf M U Ali8, Eric Chevet9, Gisela Campos10, Patricio Godoy10, Tomas Vaisar11, Béatrice Bailly-Maitre5, Kazuhiro Nagata6, Marek Michalak3, Jimena Sierralta4, Claudio Hetz12.
Abstract
Maintenance of endoplasmic reticulum (ER) proteostasis is controlled by a dynamic signaling network known as the unfolded protein response (UPR). IRE1α is a major UPR transducer, determining cell fate under ER stress. We used an interactome screening to unveil several regulators of the UPR, highlighting the ER chaperone Hsp47 as the major hit. Cellular and biochemical analysis indicated that Hsp47 instigates IRE1α signaling through a physical interaction. Hsp47 directly binds to the ER luminal domain of IRE1α with high affinity, displacing the negative regulator BiP from the complex to facilitate IRE1α oligomerization. The regulation of IRE1α signaling by Hsp47 is evolutionarily conserved as validated using fly and mouse models of ER stress. Hsp47 deficiency sensitized cells and animals to experimental ER stress, revealing the significance of Hsp47 to global proteostasis maintenance. We conclude that Hsp47 adjusts IRE1α signaling by fine-tuning the threshold to engage an adaptive UPR.Entities:
Keywords: ER stress; Hsp47; IRE1α; RRID; UPR; UPRosome; XBP1; cell death; proteostasis; stress sensing
Mesh:
Substances:
Year: 2018 PMID: 29351844 DOI: 10.1016/j.molcel.2017.12.028
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970