Biomechanical signals upregulate myogenic gene induction in the presence or absence of inflammation

doi:10.1152/ajpcell.00594.2006

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Am J Physiol Cell Physiol 293: C267-C276, 2007. First published March 28, 2007; doi:10.1152/ajpcell.00594.2006
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MUSCLE CELL BIOLOGY AND CELL MOTILITY

Biomechanical signals upregulate myogenic gene induction in the presence or absence of inflammation

Ravi Chandran, Thomas J. Knobloch, Mirela Anghelina, and Sudha Agarwal

Section of Oral Biology, The Ohio State University College of Dentistry, Columbus, Ohio

Submitted 29 November 2006 ; accepted in final form 24 March 2007

Inflammation of the muscle invariably leads to muscle cell damageand impaired regeneration. Biomechanical signals play a vitalrole in the regulation of myogenesis in healthy and inflamedmuscle. We hypothesized that biomechanical signals counteractthe actions of proinflammatory mediators and upregulate thebasic helix-loop-helix and MADS box transcription enhancer factor2 (MEF2) families of transcription factors, leading to increasedmyogenesis in inflamed muscle cells. For this purpose, C2C12cells plated on collagenized silastic membranes were subjectedto equibiaxial cyclic tensile strain (CTS) in the presence orabsence of TNF- ${alpha}$ , and the myogenic gene induction was examinedover a period of 72 h. Exposure of cells to CTS resulted ina significant upregulation of mRNA expressions and synthesisof myogenic regulatory factors, MYOD1, myogenin (MYOG), MEF2A,and cyclin-dependent kinase inhibitor 1A (CDKN1A; p21) as wellas muscle structural proteins like myosin heavy chain (MYHC)isoforms (MYH1, MYH2, and MYH4) and ${alpha}$ -tropomyosin (TPM1), eventuallyleading to an increase in myotube formation. Contrarily, TNF- ${alpha}$ suppressed the expression of all of the above differentiation-inducingfactors in C2C12 cells. Further results revealed that simultaneousexposure of C2C12 cells to CTS and TNF- ${alpha}$ abrogated the TNF- ${alpha}$ -mediateddownregulation of myogenic differentiation. In fact, the mRNAexpression and protein synthesis of all myogenic factors (Myod1,Myog, Mef2a, Cdkn1a, Myh1, Myh2, Myh4, and Tpm1) were increasedin stretched C2C12 cells despite the sustained presence of TNF- ${alpha}$ .These results demonstrate that mechanotransduction regulatesmultiple signaling molecules involved in C2C12 cell differentiation.On one hand, these signals are potent transducers of myotubephenotype in myoblasts; on the other, these signals counteractcatabolic actions of proinflammatory cytokines like TNF- ${alpha}$ andallow the expression of myogenic genes to upregulate musclecell differentiation.

myogenesis; myoblasts; inflammation; biomechanical signals

Address for reprint requests and other correspondence: S. Agarwal, 4171 Postle Hall, The Ohio State Univ. College of Dentistry, 305 W. 12th Ave., Columbus, OH 43210 (e-mail: Agarwal.61{at}osu.edu)