Cardiac troponin I is a sensitive, specific biomarker of cardiac injury in laboratory animals

Author:

O'Brien P J1,Smith D E C1,Knechtel T J2,Marchak M A2,Pruimboom-Brees I3,Brees D J3,Spratt D P4,Archer F J4,Butler P5,Potter A N1,Provost J P6,Richard J6,Snyder P A3,Reagan W J3

Affiliation:

1. Safety Sciences Europe, Sandwich, Kent CT1 3NJ, UK

2. Safety Sciences, Pfizer Inc, Kalamazoo, Michigan, USA

3. Safety Sciences, Pfizer Inc, Groton, Connecticut, USA

4. Cambridge Veterinary School, Cambridge, Cambridgeshire, UK

5. Candidate Research Group, Discovery Biology, Pfizer Ltd, Sandwich, Kent CT1 3NJ, UK

6. Safety Sciences Europe, Pfizer Ltd, Amboise, France

Abstract

This study directly demonstrates that cardiac troponin I (cTnI) is a sensitive, specific, and persistent biomarker in laboratory animals. Histopathological and pathophysiological cardiac changes in dogs, rats and mice correlated with increased serum cTnI with various cardiac inotropic agents, and cardiotoxic drugs and with cardiac arrhythmias, tachycardia, cardiac effusion with dyspnoea, and ageing. A comparison of six immunoassays for cTnI and cardiac troponin T (cTnT) to detect and monitor cardiac injury in a rodent model indicated that enzyme-linked immunosorbent (Life Diagnostics Inc and TriChem Resources Inc, West Chester, Philadelphia, USA) and Immulite (Diagnostic Products Corporation, Llanberis, UK) assays had low sensitivity and less than 1% of the dynamic range of Centaur (Bayer Healthcare Diagnostics, Newbury, UK) cTnI and Elecsys (Roche Diagnostics, Basel, Switzerland) and M8 (Bioveris Europe, Whitney, UK) cTnT assays. In dogs, however, the Immulite assay was effective and correlated with the Centaur. Serum concentrations were highly correlated but 10-fold lower for cTnT compared with cTnI with cardiac injury. Centaur assay also detected cTnI in myocardium from marmosets, swine, cattle, and guineapigs, indicating it to be candidate cardiac biomarker for these species as well. Purified rat cTnI was 50% more reactive than purified human cTnI in the Centaur assay. In the rat, an age- and gender-dependent variation in serum cTnI was found. Male rats aged six and eight months had a 10-fold greater serum cTnI than age-matched females and three-month-old rats. These increases correlated with minimal histopathological change. Isoproterenol-induced serum cTnI increased up to 760-fold the minimal detectable concentration of 0.07 μg/L, within 4–6 h and decreased with a half-life of 6 h, with an expected return to baseline of 60 h. Severity of histopathological change correlated with serum cTnI during the ongoing injury.

Publisher

SAGE Publications

Subject

General Veterinary,Animal Science and Zoology

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