In dialysis patients without ischemic heart disease, cTnI was the most specific marker (elevated in 4%), whereas cTnT was frequently elevated (up to 71%) due to skeletal muscle expression.
Cross-Sectional (n=29)
Does skeletal muscle expression of cTnT explain elevated serum cTnT in dialysis patients without ischemic heart disease?
In dialysis patients without ischemic heart disease, cTnI is a more specific biomarker for myocardial injury than cTnT, as cTnT is frequently elevated due to its expression in skeletal muscle.
Serum cardiac troponin T (cTnT) concentrations are frequently increased in chronic dialysis patients as measured by the first-generation ELISA immunoassay, as is creatine kinase (CK) MB mass in the absence of acute ischemic heart disease. We designed this study to compare four serum markers of myocardial injury CK-MB mass, first-generation ELISA cTnT, second-generation Enzymun cTnT, and cardiac troponin I (cTnI) in dialysis patients without acute ischemic heart disease. We also evaluated skeletal muscle from dialysis patients as a potential source of serum cTnT. No patients in the clinical evaluation group (n = 24) studied by history and by physical examination, electrocardiography, and two-dimensional echocardiography had evidence of ischemic heart disease. Biochemical markers were measured in serial predialysis blood samples with specific monoclonal antibody-based immunoassays. For several patients at least one sample measured above the upper reference limit: CK-MB, 7 of 24 (30%); ELISA cTnT, 17 of 24 (71%); Enzymun cTnT, 3 of 18 (17%); and cTnI, 1 of 24 (4%). In a separate group of dialysis patients (n = 5), expression of cTnT, but not cTnI, was demonstrated by Western blot analysis in 4 of 5 skeletal muscle biopsies. Chronic dialysis patients without acute ischemic heart disease frequently had increased serum CK-MB and cTnT. The specificity of the second-generation cTnT (Enzymun) assay was improved over that of the first-generation (ELISA) assay; cTnI was the most specific of the currently available biochemical markers. cTnT, but not cTnI, was expressed in the skeletal muscle of dialysis patients.
McLaurin et al. (Sun,) conducted a cross-sectional in Chronic dialysis without acute ischemic heart disease (n=29). Chronic dialysis was evaluated on Serum marker concentration above the upper reference limit. In dialysis patients without ischemic heart disease, cTnI was the most specific marker (elevated in 4%), whereas cTnT was frequently elevated (up to 71%) due to skeletal muscle expression.
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