Newer cardiac troponin I assays have similar performance to troponin T in patients with end-stage renal disease

Hickman, Peter E.; Koerbin, Gus; Southcott, Emma; Tate, Jill; Dimeski, Goce; Carter, Andrew; McGill, David; Talaulikar, Girish; Potter, Julia M.

doi:10.1258/000456307780480855

Cited by 31 publications

(35 citation statements)

References 14 publications

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“…Interestingly, allcause mortality during a median 24-month follow-up was associated with abnormal, i.e., detectable cTnT, but not with abnormal cTnI in this study [90]. However, more sensitive cTnI assays displayed similar data to the cTnT results [91].…”

Section: Prognostic Applications Of Medium Sensitivity Ctn Assaysmentioning

confidence: 43%

High sensitivity cardiac troponin assays in the clinical laboratories

Jarolím

2015

Clinical Chemistry and Laboratory Medicine (CCLM)

115

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Abstract:Immunoassays measuring cardiac troponins I or T have become firmly established as critical tools for diagnosing acute myocardial infarction. While most contemporary assays provide adequate diagnostic performance, the increased sensitivity and precision of the new, high sensitivity assays that have already been introduced into clinical practice, provide the potential to further shorten intervals between blood draws or the time needed to detect the first significant troponin elevation. In addition to the relatively modest benefits at the diagnostic end, the high sensitivity assays and the investigational ultrasensitive cardiac troponin assays offer improvements for predicting major adverse cardiovascular events, development of heart failure or transition to end-stage kidney disease. These novel high sensitivity assays can measure troponin concentrations in 50%-100% of healthy individuals and therefore allow for the distribution of troponin values within a healthy cohort to be measured, patient's baseline troponin levels to be monitored, and clinicians to be alerted of deteriorating cardiorenal conditions. We envisage that the high sensitivity assays will become important tools for predicting each patient's risk of future adverse events and for guiding and monitoring corresponding adjustments of preventative therapeutic interventions.

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Section: Prognostic Applications Of Medium Sensitivity Ctn Assaysmentioning

confidence: 43%

High sensitivity cardiac troponin assays in the clinical laboratories

Jarolím

2015

Clinical Chemistry and Laboratory Medicine (CCLM)

115

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“…The exact frequency of these elevations varies somewhat between studies, depending on the patient inclusion criteria, the applied cut-off values and the troponin assay used. In general, cTnT has been found elevated more often than cTnI (roughly 53% for cTnT and 17% for cTnI as reviewed in (Kanderian & Francis, 2006)) although recent publications, using more sensitive assays suggest that the frequency of cTnT and cTnI elevations are similar (Hickman et al, 2007;Kumar, Michelis, Devita, Panagopoulos, & Rosenstock, 2010). It is important to note that the number of detected cTn elevations depends on the cut-offs that are used to define elevated values.…”

Section: Cardiac Troponin Elevations In Esrdmentioning

confidence: 99%

Cardiac Biomarkers in End-Stage Renal Disease

Jacobs¹,

Mingels²,

Dieijen-Visser³

2012

Chronic Kidney Disease and Renal Transplantation

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“…Degradation products of TnT were also found both in animal models of ischemia/reperfusion injury [38,39] and in serum of patients with AMI [40,41]. In 2000, TnI and TnT have been approved as the biomarkers for AMI diagnosis [42], and several kits have been commercially developed and used in clinical studies [43][44][45]. In addition to TnI and TnT, other myofilament proteins, including TnC [46], LC2 [46], aactinin [32] and MyBP-C [47], were also reported as useful markers in animal models of ischemia/reperfusion injury.…”

Section: Degradationmentioning

confidence: 99%

“…Alternatively, the degradation site can be mapped using antibody epitope analysis [62], in which an array of mAb recognizing different regions within protein sequences is used [43][44][45].…”

Section: Degradationmentioning

confidence: 99%

Myofilament proteins: From cardiac disorders to proteomic changes

Yuan

Solaro

2008

Proteomics Clinical Apps

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Myofilament proteins of the cardiac sarcomere house the molecular machinery responsible for generating tension and pressure. Release of intracellular Ca 21 triggers myofilament tension generation and shortening, but the response to Ca 21 is modulated by changes in key regulatory proteins. We review how these proteomic changes are essential to adaptive physiological regulation of cardiac output and become maladaptive in cardiac disorders. We also review the essentials of proteomic techniques used to study myofilament protein changes, including degradation, isoform expression, phosphorylation and oxidation. Selected proteomic studies illustrate the applications of these approaches.

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Newer cardiac troponin I assays have similar performance to troponin T in patients with end-stage renal disease

Cited by 31 publications

References 14 publications

High sensitivity cardiac troponin assays in the clinical laboratories

High sensitivity cardiac troponin assays in the clinical laboratories

Cardiac Biomarkers in End-Stage Renal Disease

Myofilament proteins: From cardiac disorders to proteomic changes

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