mRNA expression signatures of human skeletal muscle atrophy identify a natural compound that increases muscle mass

Steven D. Kunkel; Manish Suneja; Scott M. Ebert; Kale S. Bongers; Daniel K. Fox; Sharon E. Malmberg; Fariborz Alipour; Richard K. Shields; Christopher M. Adams

doi:10.1016/j.cmet.2011.03.020

mRNA expression signatures of human skeletal muscle atrophy identify a natural compound that increases muscle mass

Steven D. Kunkel, Manish Suneja, Scott M. Ebert, Kale S. Bongers, Daniel K. Fox, Sharon E. Malmberg, Fariborz Alipour, Richard K. Shields, Christopher M. Adams

Endocrinology, Diabetes, Metabolism, and Nutrition

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

Abstract

Skeletal muscle atrophy is a common and debilitating condition that lacks a pharmacologic therapy. To develop a potential therapy, we identified 63 mRNAs that were regulated by fasting in both human and mouse muscle, and 29 mRNAs that were regulated by both fasting and spinal cord injury in human muscle. We used these two unbiased mRNA expression signatures of muscle atrophy to query the Connectivity Map, which singled out ursolic acid as a compound whose signature was opposite to those of atrophy-inducing stresses. A natural compound enriched in apples, ursolic acid reduced muscle atrophy and stimulated muscle hypertrophy in mice. It did so by enhancing skeletal muscle insulin/IGF-I signaling and inhibiting atrophy-associated skeletal muscle mRNA expression. Importantly, ursolic acid's effects on muscle were accompanied by reductions in adiposity, fasting blood glucose, and plasma cholesterol and triglycerides. These findings identify a potential therapy for muscle atrophy and perhaps other metabolic diseases.

Original language	English (US)
Pages (from-to)	627-638
Number of pages	12
Journal	Cell Metabolism
Volume	13
Issue number	6
DOIs	https://doi.org/10.1016/j.cmet.2011.03.020
State	Published - Jun 8 2011

ASJC Scopus subject areas

Physiology
Molecular Biology
Cell Biology

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10.1016/j.cmet.2011.03.020

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title = "mRNA expression signatures of human skeletal muscle atrophy identify a natural compound that increases muscle mass",

abstract = "Skeletal muscle atrophy is a common and debilitating condition that lacks a pharmacologic therapy. To develop a potential therapy, we identified 63 mRNAs that were regulated by fasting in both human and mouse muscle, and 29 mRNAs that were regulated by both fasting and spinal cord injury in human muscle. We used these two unbiased mRNA expression signatures of muscle atrophy to query the Connectivity Map, which singled out ursolic acid as a compound whose signature was opposite to those of atrophy-inducing stresses. A natural compound enriched in apples, ursolic acid reduced muscle atrophy and stimulated muscle hypertrophy in mice. It did so by enhancing skeletal muscle insulin/IGF-I signaling and inhibiting atrophy-associated skeletal muscle mRNA expression. Importantly, ursolic acid's effects on muscle were accompanied by reductions in adiposity, fasting blood glucose, and plasma cholesterol and triglycerides. These findings identify a potential therapy for muscle atrophy and perhaps other metabolic diseases.",

author = "Kunkel, {Steven D.} and Manish Suneja and Ebert, {Scott M.} and Bongers, {Kale S.} and Fox, {Daniel K.} and Malmberg, {Sharon E.} and Fariborz Alipour and Shields, {Richard K.} and Adams, {Christopher M.}",

note = "Funding Information: We thank Drs. Michael Welsh and Peter Snyder for invaluable advice and critical review of the manuscript, and Drs. Daryl Granner, John Stokes, and Allyn Mark for helpful discussions. This work was supported by a Clinical Scientist Development Award from the Doris Duke Charitable Foundation, a Career Development Award from the Department of Veterans Affairs, a Junior Faculty Award from the American Diabetes Association, grant number 1R01AR059115-01 from NIAMS/NIH, NIH T32 GM073610, Cardiovascular Interdisciplinary Research Fellowship HL007121, and grants from the University of Iowa Institute for Clinical and Translational Science, the University of Iowa Research Foundation, and the Fraternal Order of Eagles Diabetes Research Center. ",

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AU - Kunkel, Steven D.

AU - Suneja, Manish

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AU - Fox, Daniel K.

AU - Malmberg, Sharon E.

AU - Alipour, Fariborz

AU - Shields, Richard K.

AU - Adams, Christopher M.

N1 - Funding Information: We thank Drs. Michael Welsh and Peter Snyder for invaluable advice and critical review of the manuscript, and Drs. Daryl Granner, John Stokes, and Allyn Mark for helpful discussions. This work was supported by a Clinical Scientist Development Award from the Doris Duke Charitable Foundation, a Career Development Award from the Department of Veterans Affairs, a Junior Faculty Award from the American Diabetes Association, grant number 1R01AR059115-01 from NIAMS/NIH, NIH T32 GM073610, Cardiovascular Interdisciplinary Research Fellowship HL007121, and grants from the University of Iowa Institute for Clinical and Translational Science, the University of Iowa Research Foundation, and the Fraternal Order of Eagles Diabetes Research Center.

PY - 2011/6/8

Y1 - 2011/6/8

N2 - Skeletal muscle atrophy is a common and debilitating condition that lacks a pharmacologic therapy. To develop a potential therapy, we identified 63 mRNAs that were regulated by fasting in both human and mouse muscle, and 29 mRNAs that were regulated by both fasting and spinal cord injury in human muscle. We used these two unbiased mRNA expression signatures of muscle atrophy to query the Connectivity Map, which singled out ursolic acid as a compound whose signature was opposite to those of atrophy-inducing stresses. A natural compound enriched in apples, ursolic acid reduced muscle atrophy and stimulated muscle hypertrophy in mice. It did so by enhancing skeletal muscle insulin/IGF-I signaling and inhibiting atrophy-associated skeletal muscle mRNA expression. Importantly, ursolic acid's effects on muscle were accompanied by reductions in adiposity, fasting blood glucose, and plasma cholesterol and triglycerides. These findings identify a potential therapy for muscle atrophy and perhaps other metabolic diseases.

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mRNA expression signatures of human skeletal muscle atrophy identify a natural compound that increases muscle mass

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