Proteomics

Dataset Information

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Tissue adaptation is the dominant driver of the proteomic landscape of intestinal intraepithelial lymphocytes


ABSTRACT: Intestinal intraepithelial T lymphocytes (T-IEL) patrol the single layer of epithelial cells lining the gut, and consist of both induced T-IEL, derived from systemic antigen-experienced lymphocytes, and natural IEL, that are developmentally targeted to the intestine. To gain functional insights into these enigmatic cells, we used high-resolution quantitative mass spectrometry to investigate the proteomic landscape of the main T-IEL populations in the gut. Comparing the proteomes of induced T-IEL, tissue-resident memory TCRαβ+ CD8αβ+ cells and natural TCRγδ+ CD8αα+ and TCRαβ+ CD8αα+ T-IEL, with naive CD8+ T cells from lymph nodes reveals striking similarities between T-IEL subsets and the dominant effect of the gut environment on T-IEL phenotypes. Analysis of copy numbers/cell of >7000 proteins provides new understanding of the differences in composition of T cell antigen receptor signal transduction pathways in T-IEL versus conventional T cells and reveals skewing of the metabolic machinery towards an exhausted T cell phenotype adapted to the intestinal environment. This study provides a resource for exploring and understanding how multiple inputs are integrated into T-IEL function.

INSTRUMENT(S): Orbitrap Fusion

ORGANISM(S): Mus Musculus (mouse)

TISSUE(S): Gut, Lymph Node

SUBMITTER: Alejandro Brenes  

LAB HEAD: Angus I. Lamond

PROVIDER: PXD023140 | Pride | 2021-03-15

REPOSITORIES: Pride

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Publications

Tissue environment, not ontogeny, defines murine intestinal intraepithelial T lymphocytes.

Brenes Alejandro J AJ   Vandereyken Maud M   James Olivia J OJ   Watt Harriet H   Hukelmann Jens J   Spinelli Laura L   Dikovskaya Dina D   Lamond Angus I AI   Swamy Mahima M  

eLife 20210902


Tissue-resident intestinal intraepithelial T lymphocytes (T-IEL) patrol the gut and have important roles in regulating intestinal homeostasis. T-IEL include both induced T-IEL, derived from systemic antigen-experienced lymphocytes, and natural T-IEL, which are developmentally targeted to the intestine. While the processes driving T-IEL development have been elucidated, the precise roles of the different subsets and the processes driving activation and regulation of these cells remain unclear. To  ...[more]

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