Differential Contributions of ATF6 and XBP1 to the Activation of Endoplasmic Reticulum Stress-responsive Cis-acting Elements ERSE, UPRE and ERSE-II

Overview

Journal J Biochem

Publisher Oxford University Press

Specialty Biochemistry

Date 2004 Dec 16

PMID 15598891

Citations 217

Authors

Keisuke Yamamoto

Hiderou Yoshida

Koichi Kokame

Randal J Kaufman

Kazutoshi Mori

Affiliations

Soon will be listed here.

Abstract

ATF6 and XBP1 are transcription factors activated specifically in response to endoplasmic reticulum (ER) stress. Three cis-acting elements capable of binding to ATF6, XBP1 or both have been identified to date, namely ER stress-response element (ERSE), unfolded protein response element (UPRE) and ERSE-II. ERSE controls the expression of ER-localized molecular chaperones such as BiP that can refold unfolded proteins in the ER; transcription from ERSE is fully activated by ATF6 even in the absence of XBP1. In contrast, transcription from UPRE depends solely on XBP1 and it has been suggested that UPRE may control the expression of components of the ER-associated degradation system that can degrade unfolded proteins in the ER. The Herp gene, one of the most highly inducible genes under ER stress, encodes an ER membrane protein containing a ubiquitin-like domain with unknown functions, and carries ERSE-II in addition to ERSE in its promoter. In this report, we show that ERSE-II allows the NF-Y-dependent binding of ATF6 as in the case of ERSE and NF-Y-independent binding of XBP1 as in the case of UPRE, and that transcription from ERSE-II is mitigated in the absence of XBP1. Accordingly, the induction of Herp mRNA was diminished in the absence of XBP1 whereas that of BiP mRNA was not affected. These results may help in understanding the role of Herp in the quality control system in the ER.

Citing Articles

E3 ligase substrate adaptor SPOP fine-tunes the UPR of pancreatic β cells.

Oguh A, Haemmerle M, Sen S, Rozo A, Shrestha S, Cartailler J Genes Dev. 2025; 39(3-4):261-279.

PMID: 39797759 PMC: 11789638. DOI: 10.1101/gad.352010.124.

Transmission of unfolded protein response-a regulator of disease progression, severity, and spread in virus infections.

Prasad V mBio. 2025; 16(2):e0352224.

PMID: 39772778 PMC: 11796368. DOI: 10.1128/mbio.03522-24.

Exploring Endocannabinoid System: Unveiling New Roles in Modulating ER Stress.

Capolupo I, Miranda M, Musella S, Di Sarno V, Manfra M, Ostacolo C Antioxidants (Basel). 2024; 13(11).

PMID: 39594426 PMC: 11591047. DOI: 10.3390/antiox13111284.

BiP/GRP78 is a pro-viral factor for diverse dsDNA viruses that promotes the survival and proliferation of cells upon KSHV infection.

Najarro G, Brackett K, Woosley H, Dorman L, Turon-Lagot V, Khadka S PLoS Pathog. 2024; 20(10):e1012660.

PMID: 39471213 PMC: 11548844. DOI: 10.1371/journal.ppat.1012660.

A genome-wide CRISPR/Cas9 screen identifies calreticulin as a selective repressor of ATF6α.

Tung J, Huang L, George G, Harding H, Ron D, Ordonez A Elife. 2024; 13.

PMID: 39073063 PMC: 11286266. DOI: 10.7554/eLife.96979.