A reservoir of brown adipocyte progenitors in human skeletal muscle.

M. Crisan; L. Casteilla; L. Lehr; M. Carmona; A. Paoloni Giacobino; S. Yap; B. Sun; B. Leger; A. Logar; L. Penicaud; P. Schrauwen; D. Smith; R.A. Paul; B. Peault; J.P. Giacobino

doi:10.1634/stemcells.2008-0325

A reservoir of brown adipocyte progenitors in human skeletal muscle.

M. Crisan, L. Casteilla, L. Lehr, M. Carmona, A. Paoloni Giacobino, S. Yap, B. Sun, B. Leger, A. Logar, L. Penicaud, P. Schrauwen, D. Smith, R.A. Paul, B. Peault, J.P. Giacobino^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Brown adipose tissue uncoupling protein-1 (UCP1) plays a major role in the control of energy balance in rodents. It has long been thought, however, that there is no physiologically relevant UCP1 expression in adult humans. In this study we show, using an original approach consisting in sorting cells from various tissues and differentiating them in an adipogenic medium, that a stationary population of skeletal muscle cells expressing the CD34 surface protein can differentiate in vitro into genuine brown adipocytes with a high level of UCP1 expression and uncoupled respiration. These cells can be expanded in culture and their UCP1 mRNA expression is strongly increased by cell permeating cAMP derivatives and a peroxisome-proliferator-activated receptor-gamma (PPARgamma) agonist. Furthermore, UCP1 mRNA was detected in the skeletal muscle of adult humans and its expression was increased in vivo by PPARgamma agonist treatment. All the studies concerning UCP1 expression in adult humans have until now been focused on the white adipose tissue. Here we show for the first time the existence in human skeletal muscle and the prospective isolation of progenitor cells with a high potential for UCP1 expression The discovery of this reservoir generates a new hope of treating obesity by acting on energy dissipation.

Original language	English
Pages (from-to)	2425-2433
Journal	Stem Cells
Volume	26
Issue number	9
DOIs	https://doi.org/10.1634/stemcells.2008-0325
Publication status	Published - 1 Jan 2008

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10.1634/stemcells.2008-0325

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@article{2a69fe05d43a48c99b9b19fde5178f03,

title = "A reservoir of brown adipocyte progenitors in human skeletal muscle.",

abstract = "Brown adipose tissue uncoupling protein-1 (UCP1) plays a major role in the control of energy balance in rodents. It has long been thought, however, that there is no physiologically relevant UCP1 expression in adult humans. In this study we show, using an original approach consisting in sorting cells from various tissues and differentiating them in an adipogenic medium, that a stationary population of skeletal muscle cells expressing the CD34 surface protein can differentiate in vitro into genuine brown adipocytes with a high level of UCP1 expression and uncoupled respiration. These cells can be expanded in culture and their UCP1 mRNA expression is strongly increased by cell permeating cAMP derivatives and a peroxisome-proliferator-activated receptor-gamma (PPARgamma) agonist. Furthermore, UCP1 mRNA was detected in the skeletal muscle of adult humans and its expression was increased in vivo by PPARgamma agonist treatment. All the studies concerning UCP1 expression in adult humans have until now been focused on the white adipose tissue. Here we show for the first time the existence in human skeletal muscle and the prospective isolation of progenitor cells with a high potential for UCP1 expression The discovery of this reservoir generates a new hope of treating obesity by acting on energy dissipation.",

author = "M. Crisan and L. Casteilla and L. Lehr and M. Carmona and {Paoloni Giacobino}, A. and S. Yap and B. Sun and B. Leger and A. Logar and L. Penicaud and P. Schrauwen and D. Smith and R.A. Paul and B. Peault and J.P. Giacobino",

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T1 - A reservoir of brown adipocyte progenitors in human skeletal muscle.

AU - Crisan, M.

AU - Casteilla, L.

AU - Lehr, L.

AU - Carmona, M.

AU - Paoloni Giacobino, A.

AU - Yap, S.

AU - Sun, B.

AU - Leger, B.

AU - Logar, A.

AU - Penicaud, L.

AU - Schrauwen, P.

AU - Smith, D.

AU - Paul, R.A.

AU - Peault, B.

AU - Giacobino, J.P.

PY - 2008/1/1

Y1 - 2008/1/1

N2 - Brown adipose tissue uncoupling protein-1 (UCP1) plays a major role in the control of energy balance in rodents. It has long been thought, however, that there is no physiologically relevant UCP1 expression in adult humans. In this study we show, using an original approach consisting in sorting cells from various tissues and differentiating them in an adipogenic medium, that a stationary population of skeletal muscle cells expressing the CD34 surface protein can differentiate in vitro into genuine brown adipocytes with a high level of UCP1 expression and uncoupled respiration. These cells can be expanded in culture and their UCP1 mRNA expression is strongly increased by cell permeating cAMP derivatives and a peroxisome-proliferator-activated receptor-gamma (PPARgamma) agonist. Furthermore, UCP1 mRNA was detected in the skeletal muscle of adult humans and its expression was increased in vivo by PPARgamma agonist treatment. All the studies concerning UCP1 expression in adult humans have until now been focused on the white adipose tissue. Here we show for the first time the existence in human skeletal muscle and the prospective isolation of progenitor cells with a high potential for UCP1 expression The discovery of this reservoir generates a new hope of treating obesity by acting on energy dissipation.

AB - Brown adipose tissue uncoupling protein-1 (UCP1) plays a major role in the control of energy balance in rodents. It has long been thought, however, that there is no physiologically relevant UCP1 expression in adult humans. In this study we show, using an original approach consisting in sorting cells from various tissues and differentiating them in an adipogenic medium, that a stationary population of skeletal muscle cells expressing the CD34 surface protein can differentiate in vitro into genuine brown adipocytes with a high level of UCP1 expression and uncoupled respiration. These cells can be expanded in culture and their UCP1 mRNA expression is strongly increased by cell permeating cAMP derivatives and a peroxisome-proliferator-activated receptor-gamma (PPARgamma) agonist. Furthermore, UCP1 mRNA was detected in the skeletal muscle of adult humans and its expression was increased in vivo by PPARgamma agonist treatment. All the studies concerning UCP1 expression in adult humans have until now been focused on the white adipose tissue. Here we show for the first time the existence in human skeletal muscle and the prospective isolation of progenitor cells with a high potential for UCP1 expression The discovery of this reservoir generates a new hope of treating obesity by acting on energy dissipation.

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DO - 10.1634/stemcells.2008-0325

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