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Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord

A main challenge of modern biology is to understand how specific constellations of genes are activated to differentiate cells and give rise to distinct tissues. This study focuses on elucidating how gene expression is initiated in the notochord, an axial structure that provides support and patternin...

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Autores principales: José-Edwards, Diana S., Oda-Ishii, Izumi, Kugler, Jamie E., Passamaneck, Yale J., Katikala, Lavanya, Nibu, Yutaka, Di Gregorio, Anna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4684326/
https://www.ncbi.nlm.nih.gov/pubmed/26684323
http://dx.doi.org/10.1371/journal.pgen.1005730
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author José-Edwards, Diana S.
Oda-Ishii, Izumi
Kugler, Jamie E.
Passamaneck, Yale J.
Katikala, Lavanya
Nibu, Yutaka
Di Gregorio, Anna
author_facet José-Edwards, Diana S.
Oda-Ishii, Izumi
Kugler, Jamie E.
Passamaneck, Yale J.
Katikala, Lavanya
Nibu, Yutaka
Di Gregorio, Anna
author_sort José-Edwards, Diana S.
collection PubMed
description A main challenge of modern biology is to understand how specific constellations of genes are activated to differentiate cells and give rise to distinct tissues. This study focuses on elucidating how gene expression is initiated in the notochord, an axial structure that provides support and patterning signals to embryos of humans and all other chordates. Although numerous notochord genes have been identified, the regulatory DNAs that orchestrate development and propel evolution of this structure by eliciting notochord gene expression remain mostly uncharted, and the information on their configuration and recurrence is still quite fragmentary. Here we used the simple chordate Ciona for a systematic analysis of notochord cis-regulatory modules (CRMs), and investigated their composition, architectural constraints, predictive ability and evolutionary conservation. We found that most Ciona notochord CRMs relied upon variable combinations of binding sites for the transcription factors Brachyury and/or Foxa2, which can act either synergistically or independently from one another. Notably, one of these CRMs contains a Brachyury binding site juxtaposed to an (AC) microsatellite, an unusual arrangement also found in Brachyury-bound regulatory regions in mouse. In contrast, different subsets of CRMs relied upon binding sites for transcription factors of widely diverse families. Surprisingly, we found that neither intra-genomic nor interspecific conservation of binding sites were reliably predictive hallmarks of notochord CRMs. We propose that rather than obeying a rigid sequence-based cis-regulatory code, most notochord CRMs are rather unique. Yet, this study uncovered essential elements recurrently used by divergent chordates as basic building blocks for notochord CRMs.
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spelling pubmed-46843262015-12-31 Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord José-Edwards, Diana S. Oda-Ishii, Izumi Kugler, Jamie E. Passamaneck, Yale J. Katikala, Lavanya Nibu, Yutaka Di Gregorio, Anna PLoS Genet Research Article A main challenge of modern biology is to understand how specific constellations of genes are activated to differentiate cells and give rise to distinct tissues. This study focuses on elucidating how gene expression is initiated in the notochord, an axial structure that provides support and patterning signals to embryos of humans and all other chordates. Although numerous notochord genes have been identified, the regulatory DNAs that orchestrate development and propel evolution of this structure by eliciting notochord gene expression remain mostly uncharted, and the information on their configuration and recurrence is still quite fragmentary. Here we used the simple chordate Ciona for a systematic analysis of notochord cis-regulatory modules (CRMs), and investigated their composition, architectural constraints, predictive ability and evolutionary conservation. We found that most Ciona notochord CRMs relied upon variable combinations of binding sites for the transcription factors Brachyury and/or Foxa2, which can act either synergistically or independently from one another. Notably, one of these CRMs contains a Brachyury binding site juxtaposed to an (AC) microsatellite, an unusual arrangement also found in Brachyury-bound regulatory regions in mouse. In contrast, different subsets of CRMs relied upon binding sites for transcription factors of widely diverse families. Surprisingly, we found that neither intra-genomic nor interspecific conservation of binding sites were reliably predictive hallmarks of notochord CRMs. We propose that rather than obeying a rigid sequence-based cis-regulatory code, most notochord CRMs are rather unique. Yet, this study uncovered essential elements recurrently used by divergent chordates as basic building blocks for notochord CRMs. Public Library of Science 2015-12-18 /pmc/articles/PMC4684326/ /pubmed/26684323 http://dx.doi.org/10.1371/journal.pgen.1005730 Text en © 2015 José-Edwards 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
José-Edwards, Diana S.
Oda-Ishii, Izumi
Kugler, Jamie E.
Passamaneck, Yale J.
Katikala, Lavanya
Nibu, Yutaka
Di Gregorio, Anna
Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord
title Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord
title_full Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord
title_fullStr Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord
title_full_unstemmed Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord
title_short Brachyury, Foxa2 and the cis-Regulatory Origins of the Notochord
title_sort brachyury, foxa2 and the cis-regulatory origins of the notochord
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4684326/
https://www.ncbi.nlm.nih.gov/pubmed/26684323
http://dx.doi.org/10.1371/journal.pgen.1005730
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