Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD

BACKGROUND: Only a handful of signaling pathways are major actors of development and responsible for both the conservation and the diversification of animal morphologies. To explain this twofold nature, gene duplication and enhancer evolution were predominantly put forth as tinkering mechanisms wher...

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Autores principales: Sadier, Alexa, Lambert, Elise, Chevret, Pascale, Décimo, Didier, Sémon, Marie, Tohmé, Marie, Ruggiero, Florence, Ohlmann, Théophile, Pantalacci, Sophie, Laudet, Vincent
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4489351/
https://www.ncbi.nlm.nih.gov/pubmed/26134525
http://dx.doi.org/10.1186/s12862-015-0395-0
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author Sadier, Alexa
Lambert, Elise
Chevret, Pascale
Décimo, Didier
Sémon, Marie
Tohmé, Marie
Ruggiero, Florence
Ohlmann, Théophile
Pantalacci, Sophie
Laudet, Vincent
author_facet Sadier, Alexa
Lambert, Elise
Chevret, Pascale
Décimo, Didier
Sémon, Marie
Tohmé, Marie
Ruggiero, Florence
Ohlmann, Théophile
Pantalacci, Sophie
Laudet, Vincent
author_sort Sadier, Alexa
collection PubMed
description BACKGROUND: Only a handful of signaling pathways are major actors of development and responsible for both the conservation and the diversification of animal morphologies. To explain this twofold nature, gene duplication and enhancer evolution were predominantly put forth as tinkering mechanisms whereas the evolution of alternative isoforms has been, so far, overlooked. We investigate here the role of gain and loss of isoforms using Edaradd, a gene of the Ecodysplasin pathway, implicated in morphological evolution. A previous study had suggested a scenario of isoform gain and loss with an alternative isoform (A) newly gained in mammals but secondarily lost in mouse lineage. RESULTS: For a comprehensive view of A and B Edaradd isoforms history during mammal evolution, we obtained sequences for both isoforms in representative mammals and performed in vitro translations to support functional predictions. We showed that the ancestral B isoform is well conserved, whereas the mammal-specific A isoform was lost at least 7 times independently in terminal lineages throughout mammal phylogeny. Then, to gain insights into the functional relevance of this evolutionary pattern, we compared the biological function of these isoforms: i) In cellulo promoter assays showed that they are transcribed from two alternative promoters, only B exhibiting feedback regulation. ii) RT-PCR in various tissues and ENCODE data suggested that B isoform is systematically expressed whereas A isoform showed a more tissue-specific expression. iii) Both isoforms activated the NF-κB pathway in an in cellulo reporter assay, albeit at different levels and with different dynamics since A isoform exhibited feedback regulation at the protein level. Finally, only B isoform could rescue a zebrafish edaradd knockdown. CONCLUSIONS: These results suggest that the newly evolved A isoform enables modulating EDA signaling in specific conditions and with different dynamics. We speculate that during mammal diversification, A isoform regulation may have evolved rapidly, accompanying and possibly supporting the diversity of ectodermal appendages, while B isoform may have ensured essential roles. This study makes the case to pay greater attention to mosaic loss of evolutionarily speaking “young” isoforms as an important mechanism underlying phenotypic diversity and not simply as a manifestation of neutral evolution. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12862-015-0395-0) contains supplementary material, which is available to authorized users.
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spelling pubmed-44893512015-07-03 Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD Sadier, Alexa Lambert, Elise Chevret, Pascale Décimo, Didier Sémon, Marie Tohmé, Marie Ruggiero, Florence Ohlmann, Théophile Pantalacci, Sophie Laudet, Vincent BMC Evol Biol Research Article BACKGROUND: Only a handful of signaling pathways are major actors of development and responsible for both the conservation and the diversification of animal morphologies. To explain this twofold nature, gene duplication and enhancer evolution were predominantly put forth as tinkering mechanisms whereas the evolution of alternative isoforms has been, so far, overlooked. We investigate here the role of gain and loss of isoforms using Edaradd, a gene of the Ecodysplasin pathway, implicated in morphological evolution. A previous study had suggested a scenario of isoform gain and loss with an alternative isoform (A) newly gained in mammals but secondarily lost in mouse lineage. RESULTS: For a comprehensive view of A and B Edaradd isoforms history during mammal evolution, we obtained sequences for both isoforms in representative mammals and performed in vitro translations to support functional predictions. We showed that the ancestral B isoform is well conserved, whereas the mammal-specific A isoform was lost at least 7 times independently in terminal lineages throughout mammal phylogeny. Then, to gain insights into the functional relevance of this evolutionary pattern, we compared the biological function of these isoforms: i) In cellulo promoter assays showed that they are transcribed from two alternative promoters, only B exhibiting feedback regulation. ii) RT-PCR in various tissues and ENCODE data suggested that B isoform is systematically expressed whereas A isoform showed a more tissue-specific expression. iii) Both isoforms activated the NF-κB pathway in an in cellulo reporter assay, albeit at different levels and with different dynamics since A isoform exhibited feedback regulation at the protein level. Finally, only B isoform could rescue a zebrafish edaradd knockdown. CONCLUSIONS: These results suggest that the newly evolved A isoform enables modulating EDA signaling in specific conditions and with different dynamics. We speculate that during mammal diversification, A isoform regulation may have evolved rapidly, accompanying and possibly supporting the diversity of ectodermal appendages, while B isoform may have ensured essential roles. This study makes the case to pay greater attention to mosaic loss of evolutionarily speaking “young” isoforms as an important mechanism underlying phenotypic diversity and not simply as a manifestation of neutral evolution. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12862-015-0395-0) contains supplementary material, which is available to authorized users. BioMed Central 2015-07-02 /pmc/articles/PMC4489351/ /pubmed/26134525 http://dx.doi.org/10.1186/s12862-015-0395-0 Text en © Sadier et al. 2015 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 work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research Article
Sadier, Alexa
Lambert, Elise
Chevret, Pascale
Décimo, Didier
Sémon, Marie
Tohmé, Marie
Ruggiero, Florence
Ohlmann, Théophile
Pantalacci, Sophie
Laudet, Vincent
Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD
title Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD
title_full Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD
title_fullStr Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD
title_full_unstemmed Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD
title_short Tinkering signaling pathways by gain and loss of protein isoforms: the case of the EDA pathway regulator EDARADD
title_sort tinkering signaling pathways by gain and loss of protein isoforms: the case of the eda pathway regulator edaradd
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4489351/
https://www.ncbi.nlm.nih.gov/pubmed/26134525
http://dx.doi.org/10.1186/s12862-015-0395-0
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