Severe myopathy in mice lacking the MEF2/SRF-dependent gene leiomodin-3
Bercin K. Cenik, … , Eric N. Olson, Ning Liu
Bercin K. Cenik, … , Eric N. Olson, Ning Liu
Published March 16, 2015
Citation Information: J Clin Invest. 2015;125(4):1569-1578. https://doi.org/10.1172/JCI80115.
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Research Article Muscle biology

Severe myopathy in mice lacking the MEF2/SRF-dependent gene leiomodin-3

Abstract

Maintenance of skeletal muscle structure and function requires a precise stoichiometry of sarcomeric proteins for proper assembly of the contractile apparatus. Absence of components of the sarcomeric thin filaments causes nemaline myopathy, a lethal congenital muscle disorder associated with aberrant myofiber structure and contractility. Previously, we reported that deficiency of the kelch-like family member 40 (KLHL40) in mice results in nemaline myopathy and destabilization of leiomodin-3 (LMOD3). LMOD3 belongs to a family of tropomodulin-related proteins that promote actin nucleation. Here, we show that deficiency of LMOD3 in mice causes nemaline myopathy. In skeletal muscle, transcription of Lmod3 was controlled by the transcription factors SRF and MEF2. Myocardin-related transcription factors (MRTFs), which function as SRF coactivators, serve as sensors of actin polymerization and are sequestered in the cytoplasm by actin monomers. Conversely, conditions that favor actin polymerization de-repress MRTFs and activate SRF-dependent genes. We demonstrated that the actin nucleator LMOD3, together with its stabilizing partner KLHL40, enhances MRTF-SRF activity. In turn, SRF cooperated with MEF2 to sustain the expression of LMOD3 and other components of the contractile apparatus, thereby establishing a regulatory circuit to maintain skeletal muscle function. These findings provide insight into the molecular basis of the sarcomere assembly and muscle dysfunction associated with nemaline myopathy.

Authors

Bercin K. Cenik, Ankit Garg, John R. McAnally, John M. Shelton, James A. Richardson, Rhonda Bassel-Duby, Eric N. Olson, Ning Liu

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Figure 7

A model for the role of LMOD3 and KLHL40 in actin cycling and MRTF/SRF- and MEF2-dependent transcription.

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A model for the role of LMOD3 and KLHL40 in actin cycling and MRTF/SRF- ...
In normal muscle cells, MRTF/SRF and MEF2 regulate LMOD3 expression, and MEF2 regulates KLHL40 expression. KLHL40 functions in the cytoplasm to stabilize LMOD3 protein. Together, they promote actin polymerization by converting G-actin to F-actin, allowing normal sarcomeric function. In muscles lacking LMOD3, accumulation of G-actin monomers not only disrupt sarcomeric integrity, but also repress MRTF-A expression, which in turn suppresses SRF-dependent target genes encoding cytoskeletal proteins and components of the contractile apparatus, leading to nemaline myopathy.