| Literature DB >> 33846299 |
Netta Shemesh1,2, Juman Jubran1, Shiran Dror2, Eyal Simonovsky1, Omer Basha1, Chanan Argov1, Idan Hekselman1, Mehtap Abu-Qarn2, Ekaterina Vinogradov1, Omry Mauer1, Tatiana Tiago3, Serena Carra3, Anat Ben-Zvi4, Esti Yeger-Lotem5.
Abstract
The sensitivity of the protein-folding environment to chaperone disruption can be highly tissue-specific. Yet, the organization of the chaperone system across physiological human tissues has received little attention. Through computational analyses of large-scale tissue transcriptomes, we unveil that the chaperone system is composed of core elements that are uniformly expressed across tissues, and variable elements that are differentially expressed to fit with tissue-specific requirements. We demonstrate via a proteomic analysis that the muscle-specific signature is functional and conserved. Core chaperones are significantly more abundant across tissues and more important for cell survival than variable chaperones. Together with variable chaperones, they form tissue-specific functional networks. Analysis of human organ development and aging brain transcriptomes reveals that these functional networks are established in development and decline with age. In this work, we expand the known functional organization of de novo versus stress-inducible eukaryotic chaperones into a layered core-variable architecture in multi-cellular organisms.Entities:
Year: 2021 PMID: 33846299 DOI: 10.1038/s41467-021-22369-9
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919