Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity

Tle/Groucho proteins are transcriptional corepressors interacting with Tcf/Lef and Runx transcription factors, but their physiological roles in T cell development remain unknown. Conditional targeting of Tle1, Tle3 and Tle4 revealed gene dose–dependent requirements for Tle proteins in CD8(+) lineage...

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Autores principales: Xing, Shaojun, Shao, Peng, Li, Fengyin, Zhao, Xudong, Seo, Wooseok, Wheat, Justin C., Ramasamy, Selvi, Wang, Jianfeng, Li, Xiang, Peng, Weiqun, Yu, Shuyang, Liu, Chengyu, Taniuchi, Ichiro, Sweetser, David A., Xue, Hai-Hui
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Rockefeller University Press 2018
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6080905/
https://www.ncbi.nlm.nih.gov/pubmed/30045946
http://dx.doi.org/10.1084/jem.20171514
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author Xing, Shaojun
Shao, Peng
Li, Fengyin
Zhao, Xudong
Seo, Wooseok
Wheat, Justin C.
Ramasamy, Selvi
Wang, Jianfeng
Li, Xiang
Peng, Weiqun
Yu, Shuyang
Liu, Chengyu
Taniuchi, Ichiro
Sweetser, David A.
Xue, Hai-Hui
author_facet Xing, Shaojun
Shao, Peng
Li, Fengyin
Zhao, Xudong
Seo, Wooseok
Wheat, Justin C.
Ramasamy, Selvi
Wang, Jianfeng
Li, Xiang
Peng, Weiqun
Yu, Shuyang
Liu, Chengyu
Taniuchi, Ichiro
Sweetser, David A.
Xue, Hai-Hui
author_sort Xing, Shaojun
collection PubMed
description Tle/Groucho proteins are transcriptional corepressors interacting with Tcf/Lef and Runx transcription factors, but their physiological roles in T cell development remain unknown. Conditional targeting of Tle1, Tle3 and Tle4 revealed gene dose–dependent requirements for Tle proteins in CD8(+) lineage cells. Upon ablating all three Tle proteins, generation of CD8(+) T cells was greatly diminished, largely owing to redirection of MHC-I–selected thymocytes to CD4(+) lineage; the remaining CD8-positive T cells showed aberrant up-regulation of CD4(+) lineage-associated genes including Cd4, Thpok, St8sia6, and Foxp3. Mechanistically, Tle3 bound to Runx-occupied Thpok silencer, in post-selection double-positive thymocytes to prevent excessive ThPOK induction and in mature CD8(+) T cells to silence Thpok expression. Tle3 also bound to Tcf1-occupied sites in a few CD4(+) lineage-associated genes, including Cd4 silencer and St8sia6 introns, to repress their expression in mature CD8(+) T cells. These findings indicate that Tle corepressors are differentially partitioned to Runx and Tcf/Lef complexes to instruct CD8(+) lineage choice and cooperatively establish CD8(+) T cell identity, respectively.
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spelling pubmed-60809052019-02-06 Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity Xing, Shaojun Shao, Peng Li, Fengyin Zhao, Xudong Seo, Wooseok Wheat, Justin C. Ramasamy, Selvi Wang, Jianfeng Li, Xiang Peng, Weiqun Yu, Shuyang Liu, Chengyu Taniuchi, Ichiro Sweetser, David A. Xue, Hai-Hui J Exp Med Research Articles Tle/Groucho proteins are transcriptional corepressors interacting with Tcf/Lef and Runx transcription factors, but their physiological roles in T cell development remain unknown. Conditional targeting of Tle1, Tle3 and Tle4 revealed gene dose–dependent requirements for Tle proteins in CD8(+) lineage cells. Upon ablating all three Tle proteins, generation of CD8(+) T cells was greatly diminished, largely owing to redirection of MHC-I–selected thymocytes to CD4(+) lineage; the remaining CD8-positive T cells showed aberrant up-regulation of CD4(+) lineage-associated genes including Cd4, Thpok, St8sia6, and Foxp3. Mechanistically, Tle3 bound to Runx-occupied Thpok silencer, in post-selection double-positive thymocytes to prevent excessive ThPOK induction and in mature CD8(+) T cells to silence Thpok expression. Tle3 also bound to Tcf1-occupied sites in a few CD4(+) lineage-associated genes, including Cd4 silencer and St8sia6 introns, to repress their expression in mature CD8(+) T cells. These findings indicate that Tle corepressors are differentially partitioned to Runx and Tcf/Lef complexes to instruct CD8(+) lineage choice and cooperatively establish CD8(+) T cell identity, respectively. Rockefeller University Press 2018-08-06 /pmc/articles/PMC6080905/ /pubmed/30045946 http://dx.doi.org/10.1084/jem.20171514 Text en © 2018 Xing et al. http://www.rupress.org/terms/https://creativecommons.org/licenses/by-nc-sa/4.0/This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms/). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 International license, as described at https://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Research Articles
Xing, Shaojun
Shao, Peng
Li, Fengyin
Zhao, Xudong
Seo, Wooseok
Wheat, Justin C.
Ramasamy, Selvi
Wang, Jianfeng
Li, Xiang
Peng, Weiqun
Yu, Shuyang
Liu, Chengyu
Taniuchi, Ichiro
Sweetser, David A.
Xue, Hai-Hui
Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity
title Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity
title_full Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity
title_fullStr Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity
title_full_unstemmed Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity
title_short Tle corepressors are differentially partitioned to instruct CD8(+) T cell lineage choice and identity
title_sort tle corepressors are differentially partitioned to instruct cd8(+) t cell lineage choice and identity
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6080905/
https://www.ncbi.nlm.nih.gov/pubmed/30045946
http://dx.doi.org/10.1084/jem.20171514
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