Distinct role of ERp57 and ERdj5 as a disulfide isomerase and reductase during ER protein folding

Author:

Robinson Philip John12ORCID,Pringle Marie Anne12ORCID,Fleming Bethany12ORCID,Bulleid Neil John12ORCID

Affiliation:

1. School of Molecular Biosciences, College of Medical Veterinary and Life Sciences , Davidson Building , , Glasgow G12 8QQ , UK

2. University of Glasgow , Davidson Building , , Glasgow G12 8QQ , UK

Abstract

ABSTRACT Proteins entering the secretory pathway need to attain native disulfide pairings to fold correctly. For proteins with complex disulfides, this process requires the reduction and isomerisation of non-native disulfides. Two key members of the protein disulfide isomerase (PDI) family, ERp57 and ERdj5 (also known as PDIA3 and DNAJC10, respectively), are thought to be required for correct disulfide formation but it is unknown whether they act as a reductase, an isomerase or both. In addition, it is unclear how reducing equivalents are channelled through PDI family members to substrate proteins. Here, we show that neither enzyme is required for disulfide formation, but ERp57 is required for isomerisation of non-native disulfides within glycoproteins. In addition, alternative PDIs compensate for the absence of ERp57 to isomerise glycoprotein disulfides, but only in the presence of a robust reductive pathway. ERdj5 is required for this alternative pathway to function efficiently indicating its role as a reductase. Our results define the essential cellular functions of two PDIs, highlighting a distinction between formation, reduction and isomerisation of disulfide bonds.

Funder

Wellcome Trust

University of Glasgow

Publisher

The Company of Biologists

Subject

Cell Biology

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