Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>

<p>Abstract</p> <p>Background</p> <p><it>Polycomb-group genes </it>(<it>PcG</it>) encode proteins that maintain homeotic (<it>Hox</it>) gene repression throughout development. Conversely, <it>trithorax-group </it>(<it&g...

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Main Authors: Boldyreva Lidiya, Daulny Anne, Bussière Marianne, Mouchel-Vielh Emmanuèle, Decoville Martine, Salvaing Juliette, Zhimulev Igor, Locker Daniel, Peronnet Frédérique
Format: Article
Language:English
Published: BMC 2006-04-01
Series:BMC Biology
Online Access:http://www.biomedcentral.com/1741-7007/4/9
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spelling doaj-6455bd7b1d724da781cdfa26e35427992020-11-24T21:11:58ZengBMCBMC Biology1741-70072006-04-0141910.1186/1741-7007-4-9Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>Boldyreva LidiyaDaulny AnneBussière MarianneMouchel-Vielh EmmanuèleDecoville MartineSalvaing JulietteZhimulev IgorLocker DanielPeronnet Frédérique<p>Abstract</p> <p>Background</p> <p><it>Polycomb-group genes </it>(<it>PcG</it>) encode proteins that maintain homeotic (<it>Hox</it>) gene repression throughout development. Conversely, <it>trithorax-group </it>(<it>trxG</it>) genes encode positive factors required for maintenance of long term <it>Hox </it>gene activation. Both kinds of factors bind chromatin regions called maintenance elements (ME). Our previous work has shown that <it>corto</it>, which codes for a chromodomain protein, and <it>dsp1</it>, which codes for an HMGB protein, belong to a class of genes called the <it>Enhancers of trithorax and Polycomb </it>(<it>ETP</it>) that interact with both <it>PcG </it>and <it>trxG</it>. Moreover, <it>dsp1 </it>interacts with the <it>Hox </it>gene <it>Scr</it>, the DSP1 protein is present on a <it>Scr </it>ME in S2 cells but not in embryos. To understand better the role of <it>ETP</it>, we addressed genetic and molecular interactions between <it>corto </it>and <it>dsp1</it>.</p> <p>Results</p> <p>We show that Corto and DSP1 proteins co-localize at 91 sites on polytene chromosomes and co-immunoprecipitate in embryos. They interact directly through the DSP1 HMG-boxes and the amino-part of Corto, which contains a chromodomain. In order to search for a common target, we performed a genetic interaction analysis. We observed that <it>corto </it>mutants suppressed <it>dsp1<sup>1 </sup></it>sex comb phenotypes and enhanced <it>Antp<sup>Scx </sup></it>phenotypes, suggesting that <it>corto </it>and <it>dsp1 </it>are simultaneously involved in the regulation of <it>Scr</it>. Using chromatin immunoprecipitation of the <it>Scr </it>ME, we found that Corto was present on this ME both in <it>Drosophila </it>S2 cells and in embryos, whereas DSP1 was present only in S2 cells.</p> <p>Conclusion</p> <p>Our results reveal that the proteins Corto and DSP1 are differently recruited to a <it>Scr </it>ME depending on whether the ME is active, as seen in S2 cells, or inactive, as in most embryonic cells. The presence of a given combination of ETPs on an ME would control the recruitment of either PcG or TrxG complexes, propagating the silenced or active state.</p> http://www.biomedcentral.com/1741-7007/4/9
collection DOAJ
language English
format Article
sources DOAJ
author Boldyreva Lidiya
Daulny Anne
Bussière Marianne
Mouchel-Vielh Emmanuèle
Decoville Martine
Salvaing Juliette
Zhimulev Igor
Locker Daniel
Peronnet Frédérique
spellingShingle Boldyreva Lidiya
Daulny Anne
Bussière Marianne
Mouchel-Vielh Emmanuèle
Decoville Martine
Salvaing Juliette
Zhimulev Igor
Locker Daniel
Peronnet Frédérique
Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>
BMC Biology
author_facet Boldyreva Lidiya
Daulny Anne
Bussière Marianne
Mouchel-Vielh Emmanuèle
Decoville Martine
Salvaing Juliette
Zhimulev Igor
Locker Daniel
Peronnet Frédérique
author_sort Boldyreva Lidiya
title Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>
title_short Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>
title_full Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>
title_fullStr Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>
title_full_unstemmed Corto and DSP1 interact and bind to a maintenance element of the <it>Scr Hox </it>gene: understanding the role of <it>Enhancers of trithorax and Polycomb</it>
title_sort corto and dsp1 interact and bind to a maintenance element of the <it>scr hox </it>gene: understanding the role of <it>enhancers of trithorax and polycomb</it>
publisher BMC
series BMC Biology
issn 1741-7007
publishDate 2006-04-01
description <p>Abstract</p> <p>Background</p> <p><it>Polycomb-group genes </it>(<it>PcG</it>) encode proteins that maintain homeotic (<it>Hox</it>) gene repression throughout development. Conversely, <it>trithorax-group </it>(<it>trxG</it>) genes encode positive factors required for maintenance of long term <it>Hox </it>gene activation. Both kinds of factors bind chromatin regions called maintenance elements (ME). Our previous work has shown that <it>corto</it>, which codes for a chromodomain protein, and <it>dsp1</it>, which codes for an HMGB protein, belong to a class of genes called the <it>Enhancers of trithorax and Polycomb </it>(<it>ETP</it>) that interact with both <it>PcG </it>and <it>trxG</it>. Moreover, <it>dsp1 </it>interacts with the <it>Hox </it>gene <it>Scr</it>, the DSP1 protein is present on a <it>Scr </it>ME in S2 cells but not in embryos. To understand better the role of <it>ETP</it>, we addressed genetic and molecular interactions between <it>corto </it>and <it>dsp1</it>.</p> <p>Results</p> <p>We show that Corto and DSP1 proteins co-localize at 91 sites on polytene chromosomes and co-immunoprecipitate in embryos. They interact directly through the DSP1 HMG-boxes and the amino-part of Corto, which contains a chromodomain. In order to search for a common target, we performed a genetic interaction analysis. We observed that <it>corto </it>mutants suppressed <it>dsp1<sup>1 </sup></it>sex comb phenotypes and enhanced <it>Antp<sup>Scx </sup></it>phenotypes, suggesting that <it>corto </it>and <it>dsp1 </it>are simultaneously involved in the regulation of <it>Scr</it>. Using chromatin immunoprecipitation of the <it>Scr </it>ME, we found that Corto was present on this ME both in <it>Drosophila </it>S2 cells and in embryos, whereas DSP1 was present only in S2 cells.</p> <p>Conclusion</p> <p>Our results reveal that the proteins Corto and DSP1 are differently recruited to a <it>Scr </it>ME depending on whether the ME is active, as seen in S2 cells, or inactive, as in most embryonic cells. The presence of a given combination of ETPs on an ME would control the recruitment of either PcG or TrxG complexes, propagating the silenced or active state.</p>
url http://www.biomedcentral.com/1741-7007/4/9
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