Transcriptomics

Dataset Information

0

Human intraepithelial mast cell differentiation and effector function are directed by TGF-b signaling


ABSTRACT: Mast cells (MCs) expressing a distinctive protease phenotype (MCTs) selectively expand within the epithelium of human mucosal tissues during type 2 (T2) inflammation. While MCTs are phenotypically distinct from subepithelial MCs (MCTCs), signals driving human MCT differentiation and this subset’s contribution to inflammation remain unexplored. Here, we identify TGF-b as a key driver of the MCT transcriptome in nasal polyps. We find that short-term TGF-b signaling alters MC cell surface receptor expression and partially recapitulates the in vivo MCT transcriptome, while TGF-β signaling during MC differentiation upregulates a larger number of MCT-associated transcripts and inhibits the hallmark MCTC proteases chymase and cathepsin G at both the transcript and protein level, allowing selective in vitro differentiation of MCTs for functional study. We identify discrete differences in effector phenotype between in vitro-derived MCTs and MCTCs, with MCTs greatly enhancing pro-inflammatory lipid mediator generation while selectively modifying cytokine, chemokine, and growth factor production in response to both innate and adaptive stimuli, recapitulating functional features of their tissue-associated counterpart MC subsets. Thus, our findings support a role for TGF-β in promoting human MCT differentiation and identify a discrete contribution of this cell type to T2 inflammation.

ORGANISM(S): Homo sapiens

PROVIDER: GSE279240 | GEO | 2024/12/11

REPOSITORIES: GEO

Dataset's files

Source:
Action DRS
Other
Items per page:
1 - 1 of 1

Similar Datasets

2024-11-01 | GSE279289 | GEO
2022-06-22 | GSE206680 | GEO
2018-07-22 | GSE85424 | GEO
2024-07-03 | GSE235240 | GEO
2015-12-21 | GSE71247 | GEO
2022-08-31 | GSE181457 | GEO
2021-11-25 | PXD023851 | Pride
2019-03-13 | GSE111971 | GEO
2018-12-01 | GSE123161 | GEO
2024-06-18 | PXD044140 | Pride