Negative regulation of initial steps in skeletal myogenesis by mTOR and other kinases

Raphael A. Wilson; Jing Liu; Lin Xu; James Annis; Sara Helmig; Gregory Moore; Casey Timmerman; Carla Grandori; Yanbin Zheng; Stephen X. Skapek

doi:10.1038/srep20376

Negative regulation of initial steps in skeletal myogenesis by mTOR and other kinases

Raphael A. Wilson, Jing Liu, Lin Xu, James Annis, Sara Helmig, Gregory Moore, Casey Timmerman, Carla Grandori, Yanbin Zheng, Stephen X. Skapek

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Abstract

The transition from a committed progenitor cell to one that is actively differentiating represents a process that is fundamentally important in skeletal myogenesis. Although the expression and functional activation of myogenic regulatory transcription factors (MRFs) are well known to govern lineage commitment and differentiation, exactly how the first steps in differentiation are suppressed in a proliferating myoblast is much less clear. We used cultured mammalian myoblasts and an RNA interference library targeting 571 kinases to identify those that may repress muscle differentiation in proliferating myoblasts in the presence or absence of a sensitizing agent directed toward CDK4/6, a kinase previously established to impede muscle gene expression. We identified 55 kinases whose knockdown promoted myoblast differentiation, either independently or in conjunction with the sensitizer. A number of the hit kinases could be connected to known MRFs, directly or through one interaction node. Focusing on one hit, Mtor, we validated its role to impede differentiation in proliferating myoblasts and carried out mechanistic studies to show that it acts, in part, by a rapamycin-sensitive complex that involves Raptor. Our findings inform our understanding of kinases that can block the transition from lineage commitment to a differentiating state in myoblasts and offer a useful resource for others studying myogenic differentiation.

Original language	English (US)
Article number	20376
Journal	Scientific reports
Volume	6
DOIs	https://doi.org/10.1038/srep20376
State	Published - Feb 5 2016

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@article{0d65f9a7b37e429c8b4706dffff6faf0,

title = "Negative regulation of initial steps in skeletal myogenesis by mTOR and other kinases",

abstract = "The transition from a committed progenitor cell to one that is actively differentiating represents a process that is fundamentally important in skeletal myogenesis. Although the expression and functional activation of myogenic regulatory transcription factors (MRFs) are well known to govern lineage commitment and differentiation, exactly how the first steps in differentiation are suppressed in a proliferating myoblast is much less clear. We used cultured mammalian myoblasts and an RNA interference library targeting 571 kinases to identify those that may repress muscle differentiation in proliferating myoblasts in the presence or absence of a sensitizing agent directed toward CDK4/6, a kinase previously established to impede muscle gene expression. We identified 55 kinases whose knockdown promoted myoblast differentiation, either independently or in conjunction with the sensitizer. A number of the hit kinases could be connected to known MRFs, directly or through one interaction node. Focusing on one hit, Mtor, we validated its role to impede differentiation in proliferating myoblasts and carried out mechanistic studies to show that it acts, in part, by a rapamycin-sensitive complex that involves Raptor. Our findings inform our understanding of kinases that can block the transition from lineage commitment to a differentiating state in myoblasts and offer a useful resource for others studying myogenic differentiation.",

author = "Wilson, {Raphael A.} and Jing Liu and Lin Xu and James Annis and Sara Helmig and Gregory Moore and Casey Timmerman and Carla Grandori and Yanbin Zheng and Skapek, {Stephen X.}",

note = "Funding Information: The authors gratefully acknowledge Drs. N. Liu and E. Olson (UT Southwestern) for providing primary mouse myoblasts and advice on their cultivation; helpful discussions with J. Amatruda (UT Southwestern), G. Greene (U Chicago), and past and current members of the Skapek laboratory including D. Dighe, N. Iqbal, C. Sung, R. Widau; support from the UT Southwestern Medical Center Simmons Cancer Center Animal Resources Center (Supported by the NIH National Cancer Institute under award number 5P30CA142543); and grant support to SXS from the Cancer Prevention and Research Institute of Texas (RP120685-P2), St. Baldrick{\textquoteright}s Foundation, Ted Mullin Fund for Sarcoma Research, Children{\textquoteright}s Cancer Fund Dallas, and Wipe Out Kids{\textquoteright} Cancer; and to YZ from the Hyundai Hope on Wheels Foundation.",

year = "2016",

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doi = "10.1038/srep20376",

language = "English (US)",

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T1 - Negative regulation of initial steps in skeletal myogenesis by mTOR and other kinases

AU - Wilson, Raphael A.

AU - Liu, Jing

AU - Xu, Lin

AU - Annis, James

AU - Helmig, Sara

AU - Moore, Gregory

AU - Timmerman, Casey

AU - Grandori, Carla

AU - Zheng, Yanbin

AU - Skapek, Stephen X.

N1 - Funding Information: The authors gratefully acknowledge Drs. N. Liu and E. Olson (UT Southwestern) for providing primary mouse myoblasts and advice on their cultivation; helpful discussions with J. Amatruda (UT Southwestern), G. Greene (U Chicago), and past and current members of the Skapek laboratory including D. Dighe, N. Iqbal, C. Sung, R. Widau; support from the UT Southwestern Medical Center Simmons Cancer Center Animal Resources Center (Supported by the NIH National Cancer Institute under award number 5P30CA142543); and grant support to SXS from the Cancer Prevention and Research Institute of Texas (RP120685-P2), St. Baldrick’s Foundation, Ted Mullin Fund for Sarcoma Research, Children’s Cancer Fund Dallas, and Wipe Out Kids’ Cancer; and to YZ from the Hyundai Hope on Wheels Foundation.

PY - 2016/2/5

Y1 - 2016/2/5

N2 - The transition from a committed progenitor cell to one that is actively differentiating represents a process that is fundamentally important in skeletal myogenesis. Although the expression and functional activation of myogenic regulatory transcription factors (MRFs) are well known to govern lineage commitment and differentiation, exactly how the first steps in differentiation are suppressed in a proliferating myoblast is much less clear. We used cultured mammalian myoblasts and an RNA interference library targeting 571 kinases to identify those that may repress muscle differentiation in proliferating myoblasts in the presence or absence of a sensitizing agent directed toward CDK4/6, a kinase previously established to impede muscle gene expression. We identified 55 kinases whose knockdown promoted myoblast differentiation, either independently or in conjunction with the sensitizer. A number of the hit kinases could be connected to known MRFs, directly or through one interaction node. Focusing on one hit, Mtor, we validated its role to impede differentiation in proliferating myoblasts and carried out mechanistic studies to show that it acts, in part, by a rapamycin-sensitive complex that involves Raptor. Our findings inform our understanding of kinases that can block the transition from lineage commitment to a differentiating state in myoblasts and offer a useful resource for others studying myogenic differentiation.

AB - The transition from a committed progenitor cell to one that is actively differentiating represents a process that is fundamentally important in skeletal myogenesis. Although the expression and functional activation of myogenic regulatory transcription factors (MRFs) are well known to govern lineage commitment and differentiation, exactly how the first steps in differentiation are suppressed in a proliferating myoblast is much less clear. We used cultured mammalian myoblasts and an RNA interference library targeting 571 kinases to identify those that may repress muscle differentiation in proliferating myoblasts in the presence or absence of a sensitizing agent directed toward CDK4/6, a kinase previously established to impede muscle gene expression. We identified 55 kinases whose knockdown promoted myoblast differentiation, either independently or in conjunction with the sensitizer. A number of the hit kinases could be connected to known MRFs, directly or through one interaction node. Focusing on one hit, Mtor, we validated its role to impede differentiation in proliferating myoblasts and carried out mechanistic studies to show that it acts, in part, by a rapamycin-sensitive complex that involves Raptor. Our findings inform our understanding of kinases that can block the transition from lineage commitment to a differentiating state in myoblasts and offer a useful resource for others studying myogenic differentiation.

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JF - Scientific reports

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ER -

Negative regulation of initial steps in skeletal myogenesis by mTOR and other kinases

Abstract

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