| Literature DB >> 31061531 |
Joseph M Dybas1,2,3, Claire E O'Leary2, Hua Ding2, Lynn A Spruce2, Steven H Seeholzer2, Paula M Oliver4,5,6.
Abstract
Despite gathering evidence that ubiquitylation can direct non-degradative outcomes, most investigations of ubiquitylation in T cells have focused on degradation. Here, we integrated proteomic and transcriptomic datasets from primary mouse CD4+ T cells to establish a framework for predicting degradative or non-degradative outcomes of ubiquitylation. Di-glycine remnant profiling was used to reveal ubiquitylated proteins, which in combination with whole-cell proteomic and transcriptomic data allowed prediction of protein degradation. Analysis of ubiquitylated proteins identified by di-glycine remnant profiling indicated that activation of CD4+ T cells led to an increase in non-degradative ubiquitylation. This correlated with an increase in non-proteasome-targeted K29, K33 and K63 polyubiquitin chains. This study revealed over 1,200 proteins that were ubiquitylated in primary mouse CD4+ T cells and highlighted the relevance of non-proteasomally targeted ubiquitin chains in T cell signaling.Entities:
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Year: 2019 PMID: 31061531 PMCID: PMC7007700 DOI: 10.1038/s41590-019-0381-6
Source DB: PubMed Journal: Nat Immunol ISSN: 1529-2908 Impact factor: 25.606