HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation

HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation

Brown adipose tissue (BAT) plays critical thermogenic, metabolic and endocrine roles in mammals, and aberrant BAT function is associated with metabolic disorders including obesity and diabetes. The major BAT depots are clustered at the neck and forelimb levels, and arise largely within the dermomyot...

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Main Authors: Miriam A. Holzman, Abigail Ryckman, Tova M. Finkelstein, Kim Landry-Truchon, Kyra A. Schindler, Jenna M. Bergmann, Lucie Jeannotte, Jennifer H. Mansfield
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-02-01
Series:Frontiers in Cell and Developmental Biology
Subjects:
Hoxa5
brown adipose tissue
adipose development
skeletal muscle development
differentiation
Online Access:https://www.frontiersin.org/articles/10.3389/fcell.2021.632303/full
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spelling doaj-374503c7f6d14bd99d4f77f7f36a5d2c2021-02-25T06:22:54ZengFrontiers Media S.A.Frontiers in Cell and Developmental Biology2296-634X2021-02-01910.3389/fcell.2021.632303632303HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte DifferentiationMiriam A. Holzman0Abigail Ryckman1Tova M. Finkelstein2Kim Landry-Truchon3Kyra A. Schindler4Jenna M. Bergmann5Lucie Jeannotte6Jennifer H. Mansfield7Department of Biology, Barnard College, Columbia University, New York, NY, United StatesDepartment of Biology, Barnard College, Columbia University, New York, NY, United StatesDepartment of Biology, Barnard College, Columbia University, New York, NY, United StatesCentre de Recherche sur le Cancer de l’Université Laval, CRCHU de Québec-Université Laval (Oncology), Québec City, QC, CanadaDepartment of Biology, Barnard College, Columbia University, New York, NY, United StatesDepartment of Biology, Barnard College, Columbia University, New York, NY, United StatesCentre de Recherche sur le Cancer de l’Université Laval, CRCHU de Québec-Université Laval (Oncology), Québec City, QC, CanadaDepartment of Biology, Barnard College, Columbia University, New York, NY, United StatesBrown adipose tissue (BAT) plays critical thermogenic, metabolic and endocrine roles in mammals, and aberrant BAT function is associated with metabolic disorders including obesity and diabetes. The major BAT depots are clustered at the neck and forelimb levels, and arise largely within the dermomyotome of somites, from a common progenitor with skeletal muscle. However, many aspects of BAT embryonic development are not well understood. Hoxa5 patterns other tissues at the cervical and brachial levels, including skeletal, neural and respiratory structures. Here, we show that Hoxa5 also positively regulates BAT development, while negatively regulating formation of epaxial skeletal muscle. HOXA5 protein is expressed in embryonic preadipocytes and adipocytes as early as embryonic day 12.5. Hoxa5 null mutant embryos and rare, surviving adults show subtly reduced iBAT and sBAT formation, as well as aberrant marker expression, lower adipocyte density and altered lipid droplet morphology. Conversely, the epaxial muscles that arise from a common dermomyotome progenitor are expanded in Hoxa5 mutants. Conditional deletion of Hoxa5 with Myf5/Cre can reproduce both BAT and epaxial muscle phenotypes, indicating that HOXA5 is necessary within Myf5-positive cells for proper BAT and epaxial muscle development. However, recombinase-based lineage tracing shows that Hoxa5 does not act cell-autonomously to repress skeletal muscle fate. Interestingly, Hoxa5-dependent regulation of adipose-associated transcripts is conserved in lung and diaphragm, suggesting a shared molecular role for Hoxa5 in multiple tissues. Together, these findings establish a role for Hoxa5 in embryonic BAT development.https://www.frontiersin.org/articles/10.3389/fcell.2021.632303/fullHoxa5brown adipose tissueadipose developmentskeletal muscle developmentdifferentiation
collection DOAJ
language English
format Article
sources DOAJ
author Miriam A. Holzman
Abigail Ryckman
Tova M. Finkelstein
Kim Landry-Truchon
Kyra A. Schindler
Jenna M. Bergmann
Lucie Jeannotte
Jennifer H. Mansfield
spellingShingle Miriam A. Holzman
Abigail Ryckman
Tova M. Finkelstein
Kim Landry-Truchon
Kyra A. Schindler
Jenna M. Bergmann
Lucie Jeannotte
Jennifer H. Mansfield
HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation
Frontiers in Cell and Developmental Biology
Hoxa5
brown adipose tissue
adipose development
skeletal muscle development
differentiation
author_facet Miriam A. Holzman
Abigail Ryckman
Tova M. Finkelstein
Kim Landry-Truchon
Kyra A. Schindler
Jenna M. Bergmann
Lucie Jeannotte
Jennifer H. Mansfield
author_sort Miriam A. Holzman
title HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation
title_short HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation
title_full HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation
title_fullStr HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation
title_full_unstemmed HOXA5 Participates in Brown Adipose Tissue and Epaxial Skeletal Muscle Patterning and in Brown Adipocyte Differentiation
title_sort hoxa5 participates in brown adipose tissue and epaxial skeletal muscle patterning and in brown adipocyte differentiation
publisher Frontiers Media S.A.
series Frontiers in Cell and Developmental Biology
issn 2296-634X
publishDate 2021-02-01
description Brown adipose tissue (BAT) plays critical thermogenic, metabolic and endocrine roles in mammals, and aberrant BAT function is associated with metabolic disorders including obesity and diabetes. The major BAT depots are clustered at the neck and forelimb levels, and arise largely within the dermomyotome of somites, from a common progenitor with skeletal muscle. However, many aspects of BAT embryonic development are not well understood. Hoxa5 patterns other tissues at the cervical and brachial levels, including skeletal, neural and respiratory structures. Here, we show that Hoxa5 also positively regulates BAT development, while negatively regulating formation of epaxial skeletal muscle. HOXA5 protein is expressed in embryonic preadipocytes and adipocytes as early as embryonic day 12.5. Hoxa5 null mutant embryos and rare, surviving adults show subtly reduced iBAT and sBAT formation, as well as aberrant marker expression, lower adipocyte density and altered lipid droplet morphology. Conversely, the epaxial muscles that arise from a common dermomyotome progenitor are expanded in Hoxa5 mutants. Conditional deletion of Hoxa5 with Myf5/Cre can reproduce both BAT and epaxial muscle phenotypes, indicating that HOXA5 is necessary within Myf5-positive cells for proper BAT and epaxial muscle development. However, recombinase-based lineage tracing shows that Hoxa5 does not act cell-autonomously to repress skeletal muscle fate. Interestingly, Hoxa5-dependent regulation of adipose-associated transcripts is conserved in lung and diaphragm, suggesting a shared molecular role for Hoxa5 in multiple tissues. Together, these findings establish a role for Hoxa5 in embryonic BAT development.
topic Hoxa5
brown adipose tissue
adipose development
skeletal muscle development
differentiation
url https://www.frontiersin.org/articles/10.3389/fcell.2021.632303/full
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