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Ultrastructure of the skeletal muscle in the X chromosome-linked dystrophic (mdx) mouse
Authors:M. J. Cullen  E. Jaros
Affiliation:(1) Muscular Dystrophy Group Research Laboratories, Newcastle General Hospital, Westgate Road, NE4 6BE Newcastle-upon-Tyne, UK
Abstract:Summary Ultrastructurally there are some clear differences in the pathology of muscle in X chromosomelinked muscular dystrophy of the mouse (mdx) and Duchenne muscular dystrophy (DMD). In particular the mouse muscle does not become infiltrated by large aggregations of connective tissue. It has been proposed that the differences are due to secondary biochemical changes consequent on the absence of dystrophin in both conditions. If this is the case, attention should be directed to the earliest ultrastructural changes held in common by both disorders. The most conspicuous of these, preceding myofibril breakdown, is dilation of the sarcoplasmic reticulum. Any physiological link between this and the absence of dystrophin remains to be determined. We suggest that in themdx mouse, the widespread myofibre necrosis occurring at 3–4 weeks is triggered by increased mechanical demands causing the lack of dystrophin to become critical at this time. Subsequent regeneration of the myofibres appears to be almost completely successful. The ultimate failure of regeneration in DMD, in contrast, may be due to an additional factors acting in DMD exacerbating the lack of dystrophin. This additional factor may be associated with the plasma membrane lesions (not seen inmdx). Alternatively there may be factors present in the mouse that compensate for the lack of dystrophin. It is pointed out that to understand better the different processes occurring inmdx and DMD we need to learn more about the factors which control the balance between the growth of muscle and the growth of connective tissue in both normal and pathological human and mouse muscle.Supported by the Muscular Dystrophy Group of Great Britain and the Medical Research Council
Keywords:mdx Mouse  Muscle pathology  Regeneration  Duchenne muscular dystrophy
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