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Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development

Mechanisms generating diverse cell types from multipotent progenitors are crucial for normal development. Neural crest cells (NCCs) are multipotent stem cells that give rise to numerous cell-types, including pigment cells. Medaka has four types of NCC-derived pigment cells (xanthophores, leucophores...

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Autores principales: Nagao, Yusuke, Suzuki, Takao, Shimizu, Atsushi, Kimura, Tetsuaki, Seki, Ryoko, Adachi, Tomoko, Inoue, Chikako, Omae, Yoshihiro, Kamei, Yasuhiro, Hara, Ikuyo, Taniguchi, Yoshihito, Naruse, Kiyoshi, Wakamatsu, Yuko, Kelsh, Robert N., Hibi, Masahiko, Hashimoto, Hisashi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3974636/
https://www.ncbi.nlm.nih.gov/pubmed/24699463
http://dx.doi.org/10.1371/journal.pgen.1004246
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author Nagao, Yusuke
Suzuki, Takao
Shimizu, Atsushi
Kimura, Tetsuaki
Seki, Ryoko
Adachi, Tomoko
Inoue, Chikako
Omae, Yoshihiro
Kamei, Yasuhiro
Hara, Ikuyo
Taniguchi, Yoshihito
Naruse, Kiyoshi
Wakamatsu, Yuko
Kelsh, Robert N.
Hibi, Masahiko
Hashimoto, Hisashi
author_facet Nagao, Yusuke
Suzuki, Takao
Shimizu, Atsushi
Kimura, Tetsuaki
Seki, Ryoko
Adachi, Tomoko
Inoue, Chikako
Omae, Yoshihiro
Kamei, Yasuhiro
Hara, Ikuyo
Taniguchi, Yoshihito
Naruse, Kiyoshi
Wakamatsu, Yuko
Kelsh, Robert N.
Hibi, Masahiko
Hashimoto, Hisashi
author_sort Nagao, Yusuke
collection PubMed
description Mechanisms generating diverse cell types from multipotent progenitors are crucial for normal development. Neural crest cells (NCCs) are multipotent stem cells that give rise to numerous cell-types, including pigment cells. Medaka has four types of NCC-derived pigment cells (xanthophores, leucophores, melanophores and iridophores), making medaka pigment cell development an excellent model for studying the mechanisms controlling specification of distinct cell types from a multipotent progenitor. Medaka many leucophores-3 (ml-3) mutant embryos exhibit a unique phenotype characterized by excessive formation of leucophores and absence of xanthophores. We show that ml-3 encodes sox5, which is expressed in premigratory NCCs and differentiating xanthophores. Cell transplantation studies reveal a cell-autonomous role of sox5 in the xanthophore lineage. pax7a is expressed in NCCs and required for both xanthophore and leucophore lineages; we demonstrate that Sox5 functions downstream of Pax7a. We propose a model in which multipotent NCCs first give rise to pax7a-positive partially fate-restricted intermediate progenitors for xanthophores and leucophores; some of these progenitors then express sox5, and as a result of Sox5 action develop into xanthophores. Our results provide the first demonstration that Sox5 can function as a molecular switch driving specification of a specific cell-fate (xanthophore) from a partially-restricted, but still multipotent, progenitor (the shared xanthophore-leucophore progenitor).
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spelling pubmed-39746362014-04-08 Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development Nagao, Yusuke Suzuki, Takao Shimizu, Atsushi Kimura, Tetsuaki Seki, Ryoko Adachi, Tomoko Inoue, Chikako Omae, Yoshihiro Kamei, Yasuhiro Hara, Ikuyo Taniguchi, Yoshihito Naruse, Kiyoshi Wakamatsu, Yuko Kelsh, Robert N. Hibi, Masahiko Hashimoto, Hisashi PLoS Genet Research Article Mechanisms generating diverse cell types from multipotent progenitors are crucial for normal development. Neural crest cells (NCCs) are multipotent stem cells that give rise to numerous cell-types, including pigment cells. Medaka has four types of NCC-derived pigment cells (xanthophores, leucophores, melanophores and iridophores), making medaka pigment cell development an excellent model for studying the mechanisms controlling specification of distinct cell types from a multipotent progenitor. Medaka many leucophores-3 (ml-3) mutant embryos exhibit a unique phenotype characterized by excessive formation of leucophores and absence of xanthophores. We show that ml-3 encodes sox5, which is expressed in premigratory NCCs and differentiating xanthophores. Cell transplantation studies reveal a cell-autonomous role of sox5 in the xanthophore lineage. pax7a is expressed in NCCs and required for both xanthophore and leucophore lineages; we demonstrate that Sox5 functions downstream of Pax7a. We propose a model in which multipotent NCCs first give rise to pax7a-positive partially fate-restricted intermediate progenitors for xanthophores and leucophores; some of these progenitors then express sox5, and as a result of Sox5 action develop into xanthophores. Our results provide the first demonstration that Sox5 can function as a molecular switch driving specification of a specific cell-fate (xanthophore) from a partially-restricted, but still multipotent, progenitor (the shared xanthophore-leucophore progenitor). Public Library of Science 2014-04-03 /pmc/articles/PMC3974636/ /pubmed/24699463 http://dx.doi.org/10.1371/journal.pgen.1004246 Text en © 2014 Nagao 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
Nagao, Yusuke
Suzuki, Takao
Shimizu, Atsushi
Kimura, Tetsuaki
Seki, Ryoko
Adachi, Tomoko
Inoue, Chikako
Omae, Yoshihiro
Kamei, Yasuhiro
Hara, Ikuyo
Taniguchi, Yoshihito
Naruse, Kiyoshi
Wakamatsu, Yuko
Kelsh, Robert N.
Hibi, Masahiko
Hashimoto, Hisashi
Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development
title Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development
title_full Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development
title_fullStr Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development
title_full_unstemmed Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development
title_short Sox5 Functions as a Fate Switch in Medaka Pigment Cell Development
title_sort sox5 functions as a fate switch in medaka pigment cell development
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3974636/
https://www.ncbi.nlm.nih.gov/pubmed/24699463
http://dx.doi.org/10.1371/journal.pgen.1004246
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