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Cardiac troponin T in developing, regenerating and denervated rat skeletal muscle
Author(s) -
Leopoldo Saggin,
Luisa Gorza,
Simonetta Ausoni,
Stefano Schiaffino
Publication year - 1990
Publication title -
development
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.754
H-Index - 325
eISSN - 1477-9129
pISSN - 0950-1991
DOI - 10.1242/dev.110.2.547
Subject(s) - biology , immunocytochemistry , skeletal muscle , myosin , gene isoform , troponin t , denervation , cardiac muscle , embryogenesis , troponin , heart development , embryonic heart , medicine , myocyte , fetus , endocrinology , embryonic stem cell , microbiology and biotechnology , embryo , biochemistry , gene , pregnancy , genetics , myocardial infarction
Fetal rat skeletal muscles express a troponin T (TnT) isoform similar to the TnT isoform expressed in the embryonic heart with respect to electrophoretic mobility and immunoreactivity with cardiac TnT-specific monoclonal antibodies. Immunoblotting analyses reveal that both the embryonic and the adult isoforms of cardiac TnT are transiently expressed during the neonatal stages. In addition, other TnT species, different from both cardiac TnTs and from the TnT isoforms expressed in adult muscles, are present in skeletal muscles during the first two postnatal weeks. By immunocytochemistry, cardiac TnT is detectable at the somitic stage and throughout embryonic and fetal development, and disappears during the first weeks after birth, persisting exclusively in the bag fibers of the muscle spindles. Cardiac TnT is re-expressed in regenerating muscle fibers following a cold injury and in mature muscle fibers after denervation. Developmental regulation of this TnT variant is not coordinated with that of the embryonic myosin heavy chain with respect to timing of disappearance and cellular distribution. No obligatory correlation between the two proteins is likewise found in regenerating and denervated muscles.

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