Väth K, et al. (2021)

Reference: Väth K, et al. (2021) Cysteine cross-linking in native membranes establishes the transmembrane architecture of Ire1. J Cell Biol 220(8)

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Abstract

The ER is a key organelle of membrane biogenesis and crucial for the folding of both membrane and secretory proteins. Sensors of the unfolded protein response (UPR) monitor the unfolded protein load in the ER and convey effector functions for maintaining ER homeostasis. Aberrant compositions of the ER membrane, referred to as lipid bilayer stress, are equally potent activators of the UPR. How the distinct signals from lipid bilayer stress and unfolded proteins are processed by the conserved UPR transducer Ire1 remains unknown. Here, we have generated a functional, cysteine-less variant of Ire1 and performed systematic cysteine cross-linking experiments in native membranes to establish its transmembrane architecture in signaling-active clusters. We show that the transmembrane helices of two neighboring Ire1 molecules adopt an X-shaped configuration independent of the primary cause for ER stress. This suggests that different forms of stress converge in a common, signaling-active transmembrane architecture of Ire1.

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Reference Type: Journal Article | Research Support, Non-U.S. Gov't | Video-Audio Media
Authors: Väth K, Mattes C, Reinhard J, Covino R, Stumpf H, Hummer G, Ernst R
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