Ultrasensitive Cross-species Measurement of Cardiac Troponin-I Using the Erenna Immunoassay System

Schultze, A. Eric; Konrad, Robert J.; Credille, Kelly M.; Lu, Quynh Anh; Todd, John

doi:10.1177/0192623308322016

Cited by 39 publications

(54 citation statements)

References 19 publications

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“…Second, the ULoQ should be adequate to quantify large relative increases of cTnI concentration above baseline in studies of cardiotoxic compounds in rats. For example, cTnI concentrations in rats have been reported to be well over 1000 pg/mL following administration of isoproterenol at doses 0.5 mg/kg (Mitra et al 2008;Schultze et al 2008;York et al 2007), which is significantly greater than a fivefold change from our observed reference range. Thus, to provide maximum coverage of all possible and expected cTnI concentrations, such longitudinal studies require a sensitive immunoassay (LLoQ of at least 3 pg/mL) coupled with a wide dynamic range of over four logs.…”

Section: Discussionmentioning

confidence: 44%

“…All sera and calibrators were tested in duplicate and the results are presented as the mean of the two measurements. The human National Institute for Standards and Technology standard was used as the standard reference for calibration, which has been shown previously to provide accurate determinations of cTnI concentration in rat serum with this assay (Schultze et al 2008). …”

Section: Sample Analysismentioning

confidence: 99%

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Longitudinal Studies of Cardiac Troponin-I Concentrations in Serum from Male Sprague Dawley Rats: Baseline Reference Ranges and Effects of Handling and Placebo Dosing on Biological Variability

et al. 2009

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ABSTRSCTSerum cardiac troponin-I has been validated as a biomarker for cardiotoxicity in numerous animal models; however, baseline reference ranges for cTnI concentration in a healthy population of laboratory rats, as well as an investigation of biological cTnI variability in rats with respect to time, handling, and placebo dosing methods, have not been reported. In this study, we used an ultrasensitive cTnI immunoassay to quantify hourly concentrations of cTnI in live rats handled under standard laboratory conditions using 15 mL of serum per determination. The baseline reference range (mean 4.94 pg/mL, range 1-15 pg/mL, 99% confidence interval [CI]) of cTnI concentration in rats was consistent with previously reported reference ranges for cTnI in humans (1-12 pg/mL) and with preliminary studies in dogs (1-4 pg/mL) and monkeys (4-5 pg/mL) using the same cTnI assay method. In addition, cTnI concentrations in individual rat serum samples show minimal biological variability over a twenty-four-hour interval when compared to a meaningful reference change value of 193% to 206%. Furthermore, measurements of cTnI concentration were consistent within the reference limits in individual rats over long periods and under three different standard laboratory handling conditions. Thus, using this new method, rats can be followed longitudinally at hourly intervals, and a doubling of cTnI concentration would be significant above biological variability. This is a new paradigm for preclinical testing, which allows transient changes in cTnI concentration to be accurately quantified. This understanding of baseline and biological variability in rats will be fundamental for designing and analyzing future studies that assess potential cardiotoxicity in drug development.

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Section: Discussionmentioning

confidence: 44%

Section: Sample Analysismentioning

confidence: 99%

Longitudinal Studies of Cardiac Troponin-I Concentrations in Serum from Male Sprague Dawley Rats: Baseline Reference Ranges and Effects of Handling and Placebo Dosing on Biological Variability

et al. 2009

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“…While our assessment of the research assay was limited and the samples were over 2 years old, the precision of the assay was notably not as high as has been reported for rat serum with another high-sensitivity cTnI assay (Schultze et al 2008). Overall, it has been shown that cTnT is stable frozen for a least a year with a minimal decrease (7%) after 2 years of storage (Basit et al 2007).…”

Section: Discussionmentioning

confidence: 78%

Comparison of Cardiac Troponin I and T, Including the Evaluation of an Ultrasensitive Assay, as Indicators of Doxorubicin-induced Cardiotoxicity

et al. 2013

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Cardiac troponin (cTn) has been utilized to assess acute myocardial injury, but the cTn response in active/ongoing chronic injury is not well documented. The purpose of this study was to characterize the cardiac troponin I (cTnI), cardiac troponin T (cTnT), high-sensitivity cTnI, hematology, and clinical chemistry responses in rats treated with doxorubicin. Rats treated with 1, 2, or 3 mg/kg/week (wk) of doxorubicin for 2, 4, or 6 wks were sacrificed after 0, 2, or 4 wks of recovery and compared to untreated controls and animals treated with doxorubicin/dexrazoxane (50 mg/kg/wk) or etoposide (1 and 3 mg/kg/wk). The incidence and mean magnitude of cTn response increased with increasing dose and/or duration of doxorubicin treatment. Conversely, dexrazoxane/doxorubicin was partially protective for cardiotoxicity, and minimal cardiotoxicity occurred with etoposide treatment. Both cTnI and cTnT effectively identified doxorubicin-induced injury as indicated by vacuolation of cardiomyocytes of the atria/ventricles. The association between the cTn responses and histological changes was greater at the higher total exposures, but the magnitude of cTn response did not match closely with histologic grade. The high-sensitivity cTnI assay was also effective in identifying cardiac injury. Alterations occurred in the hematology and clinical chemistry parameters and reflected both dose and duration of doxorubicin treatment.

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“…cTnI concentrations in healthy human individuals, rats, dogs and monkeys are in the picomolar range, well below the analytical sensitivity of commercially available assays. 22,23 It is highly probable that healthy horses have similar plasma cTnI concentrations and assay sensitivity limitations are the likely reason for failure to detect cTnI in many horses. In addition to undetectable cTnI concentrations pre-anesthesia, most horses of this study did not develop detectable cTnI following anesthesia.…”

Section: Discussionmentioning

confidence: 99%

Effect of general anesthesia on plasma cardiac troponin I concentrations in healthy horses

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et al. 2011

Journal of Veterinary Cardiology

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Ultrasensitive Cross-species Measurement of Cardiac Troponin-I Using the Erenna Immunoassay System

Cited by 39 publications

References 19 publications

Longitudinal Studies of Cardiac Troponin-I Concentrations in Serum from Male Sprague Dawley Rats: Baseline Reference Ranges and Effects of Handling and Placebo Dosing on Biological Variability

Longitudinal Studies of Cardiac Troponin-I Concentrations in Serum from Male Sprague Dawley Rats: Baseline Reference Ranges and Effects of Handling and Placebo Dosing on Biological Variability

Comparison of Cardiac Troponin I and T, Including the Evaluation of an Ultrasensitive Assay, as Indicators of Doxorubicin-induced Cardiotoxicity

Effect of general anesthesia on plasma cardiac troponin I concentrations in healthy horses

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