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Selective synthesis and degradation of slow skeletal myosin heavy chains in developing muscle fibers
Dr. Gurtej K. Dhoot PhD,
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Dr. Gurtej K. Dhoot PhD
Department of Immunology, Medical School, University of Birmingham, Birmingham, England
Department of Immunology, Medical School, University of Birmingham, Vincent Drive, Edgbaston, Birmingham, England B15 2TJSearch for more papers by this authorDr. Gurtej K. Dhoot PhD,
Corresponding Author
Dr. Gurtej K. Dhoot PhD
Department of Immunology, Medical School, University of Birmingham, Birmingham, England
Department of Immunology, Medical School, University of Birmingham, Vincent Drive, Edgbaston, Birmingham, England B15 2TJSearch for more papers by this authorAbstract
During fetal development of fast skeletal muscles in the rat, three types of cells could be identified using a monoclonal antibody to slow skeletal muscle myosin heavy chain. Presumptive type I cells stained positive for slow forms of skeletal myosin heavy chain and a previously described protein5 of an apparent molecular weight of 100 KD, whereas presumptive type 2B cells did not stain for either of these peptides. Presumptive type 2A cells, on the other hand, did not stain for slow isoform of 100-K protein, but did stain positive for slow skeletal myosin heavy chain. There was a progressive suppression or degradation of slow skeletal myosin heavy chain in presumptive type 2A cells during subsequent fetal development, so that it was almost undetectable in most animals at birth. Soleus, a slow muscle, however, did not show clear differentiation into presumptive type I and type 2 cells until 4 days after birth.
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