A novel multifunctional role for Hsp70 in binding post-translational modifications on client proteins

Author:

Nitika ORCID,Zheng Bo,Ruan Linhao,Kline Jake T.,Sikora Jacek,Torres Mara Texeira,Wang Yuhao,Takakuwa Jade E.,Huguet Romain,Klemm Cinzia,Segarra Verónica A.ORCID,Winters Matthew J.,Pryciak Peter M.,Thorpe Peter H.,Tatebayashi Kazuo,Li Rong,Fornelli Luca,Truman Andrew W.ORCID

Abstract

SummaryHsp70 interactions are critical for cellular viability and the response to stress. Previous attempts to characterize Hsp70 interactions have been limited by their transient nature and inability of current technologies to distinguish direct vs bridged interactions. We report the novel use of cross-linking mass spectrometry (XL-MS) to comprehensively characterize the budding yeast Hsp70 protein interactome. Using this approach, we have gained fundamental new insights into Hsp70 function, including definitive evidence of Hsp70 self-association as well as multi-point interaction with its client proteins. In addition to identifying a novel set of direct Hsp70 interactors which can be used to probe chaperone function in cells, we have also identified a suite of PTM-associated Hsp70 interactions. The majority of these PTMs have not been previously reported and appear to be critical in the regulation of client protein function. These data indicate that one of the mechanisms by which PTMs contribute to protein function is by facilitating interaction with chaperones. Taken together, we propose that XL-MS analysis of chaperone complexes may be used as a unique way to identify biologically-important PTMs on client proteins.In vivo confirmation of Hsp70 dimerizationComprehensive direct interactome of Hsp70Multi-domain interactions between Hsp70 and client proteinsIdentification of novel biologically-important client protein PTMs

Publisher

Cold Spring Harbor Laboratory

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