| Literature DB >> 29061044 |
Katherine R Adams, Sitara Chauhan, Divya B Patel, Virginia K Clements1, Yan Wang2, Steven M Jay, Nathan J Edwards3, Suzanne Ostrand-Rosenberg1, Catherine Fenselau.
Abstract
Ubiquitinated proteins carried by the extracellular vesicles (EV) released by myeloid-derived suppressor cells (MDSC) have been investigated using proteomic strategies to examine the effect of tumor-associated inflammation. EV were collected from MDSC directly following isolation from tumor-bearing mice with low and high inflammation. Among the 1092 proteins (high inflammation) and 925 proteins (low inflammation) identified, more than 50% were observed as ubiquitinated proteoforms. More than three ubiquitin-attachment sites were characterized per ubiquitinated protein, on average. Multiple ubiquitination sites were identified in the pro-inflammatory proteins S100 A8 and S100 A9, characteristic of MDSC and in histones and transcription regulators among other proteins. Spectral counting and pathway analysis suggest that ubiquitination occurs independently of inflammation. Some ubiquitinated proteins were shown to cause the migration of MDSC, which has been previously connected with immune suppression and tumor progression. Finally, MDSC EV are found collectively to carry all the enzymes required to catalyze ubiquitination, and the hypothesis is presented that a portion of the ubiquitinated proteins are produced in situ.Entities:
Keywords: LC−MS/MS; MDSC; extracellular vesicles; inflammation; spectral counting; top-down proteomics; tumor-induced immune suppression; ubiquitome
Mesh:
Substances:
Year: 2017 PMID: 29061044 PMCID: PMC6137330 DOI: 10.1021/acs.jproteome.7b00585
Source DB: PubMed Journal: J Proteome Res ISSN: 1535-3893 Impact factor: 4.466