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J Appl Physiol 94: 2524-2533, 2003; doi:10.1152/japplphysiol.01078.2002
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Vol. 94, Issue 6, 2524-2533, June 2003

HIGHLIGHTED TOPICS
Genetic Models in Applied Physiology
Selected Contribution: Merosin deficiency leads to alterations in passive and active skeletal muscle mechanics

Suneal R. Jannapureddy, Nisha D. Patel, Willy Hwang, and Aladin M. Boriek

Department of Medicine, Baylor College of Medicine, Houston, Texas 77030

The role of extracellular elements on the mechanical properties of skeletal muscles is unknown. Merosin is an essential extracellular matrix protein that forms a mechanical junction between the sarcolemma and collagen. Therefore, it is possible that merosin plays a role in force transmission between muscle fibers and collagen. We hypothesized that deficiency in merosin may alter passive muscle stiffness, viscoelastic properties, and contractile muscle force in skeletal muscles. We used the dy/dy mouse, a merosin-deficient mouse model, to examine changes in passive and active muscle mechanics. After mice were anesthetized and the diaphragm or the biceps femoris hindlimb muscle was excised, passive length-tension relationships, stress-relaxation curves, or isometric contractile properties were determined with an in vitro biaxial mechanical testing apparatus. Compared with controls, extensibility was smaller in the muscle fiber direction and the transverse fiber direction of the mutant mice. The relaxed elastic modulus was smaller in merosin-deficient diaphragms compared with controls. Interestingly, maximal muscle tetanic stress was depressed in muscles from the mutant mice during uniaxial loading but not during biaxial loading. However, presence of transverse passive stretch increases maximal contractile stress in both the mutant and normal mice. Our data suggest that merosin contributes to muscle passive stiffness, viscoelasticity, and contractility and that the mechanism by which force is transmitted between adjacent myofibers via merosin possibly in shear.

muscular dystrophy; respiratory muscles; force transmission; extracellular matrix


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