Inadequate BiP availability defines endoplasmic reticulum stress

Vitale M.; Bakunts A.; Orsi A.; Lari F.; Tade L.; DANIELI, ANTONELLA; Rato C.; Valetti C.; Sitia R.; Raimondi A.; Christianson J. C.; Van Anken E.

Published 2019 | Version v1

Publication Metadata-only

Inadequate BiP availability defines endoplasmic reticulum stress

Contributors

Others:

How endoplasmic reticulum (ER) stress leads to cytotoxicity is ill-defined. Previously we showed that HeLa cells readjust homeostasis upon proteostatically driven ER stress, triggered by inducible bulk expression of secretory immunoglobulin M heavy chain (ms) thanks to the unfolded protein response (UPR; Bakunts et al., 2017). Here we show that conditions that prevent that an excess of the ER resident chaperone (and UPR target gene) BiP over ms is restored lead to ms-driven proteotoxicity, i.e. abrogation of HRD1-mediated ER-associated degradation (ERAD), or of the UPR, in particular the ATF6a branch. Such conditions are tolerated instead upon removal of the BiP-sequestering first constant domain (CH1) from ms. Thus, our data define proteostatic ER stress to be a specific consequence of inadequate BiP availability, which both the UPR and ERAD redeem.

Additional details

URL: http://hdl.handle.net/11567/955458
URN: urn:oai:iris.unige.it:11567/955458

Origin repository: UNIGE

	All versions	This version
Views	7	7
Downloads	0	0
Data volume	0 Bytes	0 Bytes

Inadequate BiP availability defines endoplasmic reticulum stress

Creators

Contributors

Others:

Description

Additional details

Identifiers

Origin repository