Myosin heavy-chain fragments and cardiac troponins in the serum in rhabdomyolysis. Diagnostic specificity of new biochemical markers

Myosin heavy-chain fragments and cardiac troponins in the serum in rhabdomyolysis. Diagnostic specificity of new biochemical markers

Myosin is the major structural protein in muscle. Antibodies to beta-type heavy meromyosin react with cardiac and slow-twitch skeletal muscle. Cardiac TnT and TnI were developed as tissue-specific indicators. To study myosin heavy-chain fragments as a delayed marker of previous rhabdomyolysis. To ex...

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Bibliographic Details
Published in:Archives of neurology (Chicago) Vol. 52; no. 12; p. 1210
Main Authors: Löfberg, M, Tähtelä, R, Härkönen, M, Somer, H
Format: Journal Article
Language:English
Published: United States 01-12-1995
Subjects:
Adult
Aged
Biomarkers - blood
Creatine Kinase - blood
Female
Humans
Male
Middle Aged
Myocardium - metabolism
Myocardium - pathology
Myosin Heavy Chains - blood
Peptide Fragments - blood
Predictive Value of Tests
Rhabdomyolysis - blood
Rhabdomyolysis - diagnosis
Rhabdomyolysis - pathology
Sensitivity and Specificity
Troponin - blood
Troponin I
Troponin T
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Summary:Myosin is the major structural protein in muscle. Antibodies to beta-type heavy meromyosin react with cardiac and slow-twitch skeletal muscle. Cardiac TnT and TnI were developed as tissue-specific indicators. To study myosin heavy-chain fragments as a delayed marker of previous rhabdomyolysis. To examine the cardiac specificity of cardiac troponin T (TnT) and cardiac troponin I (TnI) in patients with severe skeletal muscle damage. Serum myosin heavy-chain fragments, TnT, and TnI were studied up to 12 days after diagnosis in relationship to the serum creatine kinase level in 20 patients with rhabdomyolysis. The mean peak serum creatine kinase activity was 91,300 U/L. Myosin heavy-chain fragments were measured by an immunoradiometric assay, TnT by a one-step immunoenzymometric assay, and TnI by an immunoenzymometric assay. Values for serum myosin heavy-chain fragments were greater than the upper limit of normal in all patients. The peak value (70 times the upper normal limit, on average) was usually achieved 4 to 7 days after the diagnosis of rhabdomyolysis, and it was increased up to 12 days. The peak level of TnT was increased in 95% of the patients, and it correlated strongly with the peak activity of serum creatine kinase. The highest TnI value was above the detection limit of myocardial infarction in 30% of the patients. Half of these patients were the only patients with ischemic changes observed on an electrocardiogram performed on admission to the hospital. The measurement of myosin heavy-chain fragments was useful in the diagnosis of previous rhabdomyolysis up to 12 days. The role of TnT was negligible as an indicator of cardiac muscle damage in patients with severe rhabdomyolysis. Cardiac TnI is a more tissue-specific marker for myocardial damage even with concurrent rhabdomyolysis.
ISSN:0003-9942
DOI:10.1001/archneur.1995.00540360090020