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Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C

The development of niches for tissue-specific stem cells is an important aspect of stem cell biology. Determination of niche size and niche numbers during organogenesis involves precise control of gene expression. How this is achieved in the context of a complex chromatin landscape is largely unknow...

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Autores principales: Hitrik, Anna, Popliker, Malka, Gancz, Dana, Mukamel, Zohar, Lifshitz, Aviezer, Schwartzman, Omer, Tanay, Amos, Gilboa, Lilach
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5147775/
https://www.ncbi.nlm.nih.gov/pubmed/27846223
http://dx.doi.org/10.1371/journal.pgen.1006330
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author Hitrik, Anna
Popliker, Malka
Gancz, Dana
Mukamel, Zohar
Lifshitz, Aviezer
Schwartzman, Omer
Tanay, Amos
Gilboa, Lilach
author_facet Hitrik, Anna
Popliker, Malka
Gancz, Dana
Mukamel, Zohar
Lifshitz, Aviezer
Schwartzman, Omer
Tanay, Amos
Gilboa, Lilach
author_sort Hitrik, Anna
collection PubMed
description The development of niches for tissue-specific stem cells is an important aspect of stem cell biology. Determination of niche size and niche numbers during organogenesis involves precise control of gene expression. How this is achieved in the context of a complex chromatin landscape is largely unknown. Here we show that the nuclear protein Combgap (Cg) supports correct ovarian niche formation in Drosophila by controlling ecdysone-Receptor (EcR)- mediated transcription and long-range chromatin contacts in the broad locus (BR-C). Both cg and BR-C promote ovarian growth and the development of niches for germ line stem cells. BR-C levels were lower when Combgap was either reduced or over-expressed, indicating an intricate regulation of the BR-C locus by Combgap. Polytene chromosome stains showed that Cg co-localizes with EcR, the major regulator of BR-C, at the BR-C locus and that EcR binding to chromatin was sensitive to changes in Cg levels. Proximity ligation assay indicated that the two proteins could reside in the same complex. Finally, chromatin conformation analysis revealed that EcR-bound regions within BR-C, which span ~30 KBs, contacted each other. Significantly, these contacts were stabilized in an ecdysone- and Combgap-dependent manner. Together, these results highlight Combgap as a novel regulator of chromatin structure that promotes transcription of ecdysone target genes and ovarian niche formation.
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spelling pubmed-51477752016-12-21 Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C Hitrik, Anna Popliker, Malka Gancz, Dana Mukamel, Zohar Lifshitz, Aviezer Schwartzman, Omer Tanay, Amos Gilboa, Lilach PLoS Genet Research Article The development of niches for tissue-specific stem cells is an important aspect of stem cell biology. Determination of niche size and niche numbers during organogenesis involves precise control of gene expression. How this is achieved in the context of a complex chromatin landscape is largely unknown. Here we show that the nuclear protein Combgap (Cg) supports correct ovarian niche formation in Drosophila by controlling ecdysone-Receptor (EcR)- mediated transcription and long-range chromatin contacts in the broad locus (BR-C). Both cg and BR-C promote ovarian growth and the development of niches for germ line stem cells. BR-C levels were lower when Combgap was either reduced or over-expressed, indicating an intricate regulation of the BR-C locus by Combgap. Polytene chromosome stains showed that Cg co-localizes with EcR, the major regulator of BR-C, at the BR-C locus and that EcR binding to chromatin was sensitive to changes in Cg levels. Proximity ligation assay indicated that the two proteins could reside in the same complex. Finally, chromatin conformation analysis revealed that EcR-bound regions within BR-C, which span ~30 KBs, contacted each other. Significantly, these contacts were stabilized in an ecdysone- and Combgap-dependent manner. Together, these results highlight Combgap as a novel regulator of chromatin structure that promotes transcription of ecdysone target genes and ovarian niche formation. Public Library of Science 2016-11-15 /pmc/articles/PMC5147775/ /pubmed/27846223 http://dx.doi.org/10.1371/journal.pgen.1006330 Text en © 2016 Hitrik et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Hitrik, Anna
Popliker, Malka
Gancz, Dana
Mukamel, Zohar
Lifshitz, Aviezer
Schwartzman, Omer
Tanay, Amos
Gilboa, Lilach
Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C
title Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C
title_full Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C
title_fullStr Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C
title_full_unstemmed Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C
title_short Combgap Promotes Ovarian Niche Development and Chromatin Association of EcR-Binding Regions in BR-C
title_sort combgap promotes ovarian niche development and chromatin association of ecr-binding regions in br-c
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5147775/
https://www.ncbi.nlm.nih.gov/pubmed/27846223
http://dx.doi.org/10.1371/journal.pgen.1006330
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