Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis

Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis

The paradigm of developmental regulation by Polycomb group (PcG) proteins posits that they maintain silencing outside the spatial expression domains of their target genes, particularly of Hox genes, starting from mid embryogenesis. The Enhancer of zeste [E(z)] PcG protein is the catalytic subunit of...

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Main Authors: Emilie Le Goff, Camille Martinand-Mari, Marianne Martin, Jérôme Feuillard, Yvan Boublik, Nelly Godefroy, Paul Mangeat, Stephen Baghdiguian, Giacomo Cavalli
Format: Article
Language:English
Published: The Company of Biologists 2015-09-01
Series:Biology Open
Subjects:
Ciona intestinalis
Enhancer of zeste
Polycomb
PRC2
Embryogenesis
Online Access:http://bio.biologists.org/content/4/9/1109
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spelling doaj-cd243a1186a24c618477e4854e0f8c912021-06-02T18:43:51ZengThe Company of BiologistsBiology Open2046-63902015-09-01491109112110.1242/bio.010835010835Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesisEmilie Le Goff0Camille Martinand-Mari1Marianne Martin2Jérôme Feuillard3Yvan Boublik4Nelly Godefroy5Paul Mangeat6Stephen Baghdiguian7Giacomo Cavalli8 Université Montpellier, Place Eugène Bataillon, Montpellier 34095, Cedex 5, France Université Montpellier, Place Eugène Bataillon, Montpellier 34095, Cedex 5, France Université Montpellier, Place Eugène Bataillon, Montpellier 34095, Cedex 5, France Centre de Recherche de Biochimie Macromoléculaire (CRBM), UMR5237, CNRS, Montpellier 34293, Cedex 05, France Centre de Recherche de Biochimie Macromoléculaire (CRBM), UMR5237, CNRS, Montpellier 34293, Cedex 05, France Université Montpellier, Place Eugène Bataillon, Montpellier 34095, Cedex 5, France Université Montpellier, Place Eugène Bataillon, Montpellier 34095, Cedex 5, France Université Montpellier, Place Eugène Bataillon, Montpellier 34095, Cedex 5, France Institute of Human Genetics (IGH), UPR 1142, CNRS, Montpellier 34396, France The paradigm of developmental regulation by Polycomb group (PcG) proteins posits that they maintain silencing outside the spatial expression domains of their target genes, particularly of Hox genes, starting from mid embryogenesis. The Enhancer of zeste [E(z)] PcG protein is the catalytic subunit of the PRC2 complex, which silences its targets via deposition of the H3K27me3 mark. Here, we studied the ascidian Ciona intestinalis counterpart of E(z). Ci-E(z) is detected by immunohistochemistry as soon as the 2- and 4-cell stages as a cytoplasmic form and becomes exclusively nuclear thereafter, whereas the H3K27me3 mark is detected starting from the gastrula stage and later. Morpholino invalidation of Ci-E(z) leads to the total disappearance of both Ci-E(z) protein and its H3K27me3 mark. Ci-E(z) morphants display a severe phenotype. Strikingly, the earliest defects occur at the 4-cell stage with the dysregulation of cell positioning and mitotic impairment. At later stages, Ci-E(z)-deficient embryos are affected by terminal differentiation defects of neural, epidermal and muscle tissues, by the failure to form a notochord and by the absence of caudal nerve. These major phenotypic defects are specifically rescued by injection of a morpholino-resistant Ci-E(z) mRNA, which restores expression of Ci-E(z) protein and re-deposition of the H3K27me3 mark. As observed by qPCR analyses, Ci-E(z) invalidation leads to the early derepression of tissue-specific developmental genes, whereas late-acting developmental genes are generally down-regulated. Altogether, our results suggest that Ci-E(z) plays a major role during embryonic development in Ciona intestinalis by silencing early-acting developmental genes in a Hox-independent manner.http://bio.biologists.org/content/4/9/1109Ciona intestinalisEnhancer of zestePolycombPRC2Embryogenesis
collection DOAJ
language English
format Article
sources DOAJ
author Emilie Le Goff
Camille Martinand-Mari
Marianne Martin
Jérôme Feuillard
Yvan Boublik
Nelly Godefroy
Paul Mangeat
Stephen Baghdiguian
Giacomo Cavalli
spellingShingle Emilie Le Goff
Camille Martinand-Mari
Marianne Martin
Jérôme Feuillard
Yvan Boublik
Nelly Godefroy
Paul Mangeat
Stephen Baghdiguian
Giacomo Cavalli
Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis
Biology Open
Ciona intestinalis
Enhancer of zeste
Polycomb
PRC2
Embryogenesis
author_facet Emilie Le Goff
Camille Martinand-Mari
Marianne Martin
Jérôme Feuillard
Yvan Boublik
Nelly Godefroy
Paul Mangeat
Stephen Baghdiguian
Giacomo Cavalli
author_sort Emilie Le Goff
title Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis
title_short Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis
title_full Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis
title_fullStr Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis
title_full_unstemmed Enhancer of zeste acts as a major developmental regulator of Ciona intestinalis embryogenesis
title_sort enhancer of zeste acts as a major developmental regulator of ciona intestinalis embryogenesis
publisher The Company of Biologists
series Biology Open
issn 2046-6390
publishDate 2015-09-01
description The paradigm of developmental regulation by Polycomb group (PcG) proteins posits that they maintain silencing outside the spatial expression domains of their target genes, particularly of Hox genes, starting from mid embryogenesis. The Enhancer of zeste [E(z)] PcG protein is the catalytic subunit of the PRC2 complex, which silences its targets via deposition of the H3K27me3 mark. Here, we studied the ascidian Ciona intestinalis counterpart of E(z). Ci-E(z) is detected by immunohistochemistry as soon as the 2- and 4-cell stages as a cytoplasmic form and becomes exclusively nuclear thereafter, whereas the H3K27me3 mark is detected starting from the gastrula stage and later. Morpholino invalidation of Ci-E(z) leads to the total disappearance of both Ci-E(z) protein and its H3K27me3 mark. Ci-E(z) morphants display a severe phenotype. Strikingly, the earliest defects occur at the 4-cell stage with the dysregulation of cell positioning and mitotic impairment. At later stages, Ci-E(z)-deficient embryos are affected by terminal differentiation defects of neural, epidermal and muscle tissues, by the failure to form a notochord and by the absence of caudal nerve. These major phenotypic defects are specifically rescued by injection of a morpholino-resistant Ci-E(z) mRNA, which restores expression of Ci-E(z) protein and re-deposition of the H3K27me3 mark. As observed by qPCR analyses, Ci-E(z) invalidation leads to the early derepression of tissue-specific developmental genes, whereas late-acting developmental genes are generally down-regulated. Altogether, our results suggest that Ci-E(z) plays a major role during embryonic development in Ciona intestinalis by silencing early-acting developmental genes in a Hox-independent manner.
topic Ciona intestinalis
Enhancer of zeste
Polycomb
PRC2
Embryogenesis
url http://bio.biologists.org/content/4/9/1109
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AT mariannemartin enhancerofzesteactsasamajordevelopmentalregulatorofcionaintestinalisembryogenesis
AT jeromefeuillard enhancerofzesteactsasamajordevelopmentalregulatorofcionaintestinalisembryogenesis
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