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The Regulatory T Cell Lineage Factor Foxp3 Regulates Gene Expression through Several Distinct Mechanisms Mostly Independent of Direct DNA Binding
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نویسنده
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xie x. ,stubbington m.j.t. ,nissen j.k. ,andersen k.g. ,hebenstreit d. ,teichmann s.a. ,betz a.g.
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منبع
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plos genetics - 2015 - دوره : 11 - شماره : 6
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چکیده
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The lineage factor foxp3 is essential for the development and maintenance of regulatory t cells,but little is known about the mechanisms involved. here,we demonstrate that an n-terminal proline-rich interaction region is crucial for foxp3’s function. subdomains within this key region link foxp3 to several independent mechanisms of transcriptional regulation. our study suggests that foxp3,even in the absence of its dna-binding forkhead domain,acts as a bridge between dna-binding interaction partners and proteins with effector function permitting it to regulate a large number of genes. we show that,in one such mechanism,foxp3 recruits class i histone deacetylases to the promoters of target genes,counteracting activation-induced histone acetylation and thereby suppressing their expression. © 2015 xie et al.
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آدرس
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mrc laboratory of molecular biology,cambridge, United Kingdom, european molecular biology laboratory-european bioinformatics institute (embl-ebi),hinxton, United Kingdom, mrc laboratory of molecular biology,cambridge, United Kingdom, mrc laboratory of molecular biology,cambridge,united kingdom,center for systems biology,department of organismic and evolutionary biology,harvard university,and broad institute of mit and harvard,cambridge,ma, United States, mrc laboratory of molecular biology,cambridge,united kingdom,university of warwick,coventry, United Kingdom, european molecular biology laboratory-european bioinformatics institute (embl-ebi),hinxton, United Kingdom, mrc laboratory of molecular biology,cambridge, United Kingdom
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Authors
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