Evaluation of cardiovascular changes in dogs administered three positive controls using jacketed external telemetry-blood pressure (JET-BP)

John J Kremer; Andrew J Bills; Nathanael J Hanke; Hepei Chen; William A Meier; Mark A Osinski; C Michael Foley

doi:10.1016/j.vascn.2015.05.008

Evaluation of cardiovascular changes in dogs administered three positive controls using jacketed external telemetry-blood pressure (JET-BP)

J Pharmacol Toxicol Methods. 2015 Sep-Oct:75:27-37. doi: 10.1016/j.vascn.2015.05.008. Epub 2015 May 20.

Authors

John J Kremer¹, Andrew J Bills², Nathanael J Hanke², Hepei Chen², William A Meier², Mark A Osinski², C Michael Foley²

Affiliations

¹ Covance Laboratories Inc., 3301 Kinsman Boulevard, Madison, WI 53704-2523, USA. Electronic address: john.kremer@covance.com.
² Covance Laboratories Inc., 3301 Kinsman Boulevard, Madison, WI 53704-2523, USA.

PMID: 26001324
DOI: 10.1016/j.vascn.2015.05.008

Abstract

Introduction: Nonclinical safety studies are increasingly incorporating cardiac safety endpoints to discover potential cardiovascular liabilities. This trend for more thorough cardiovascular nonclinical safety evaluation is prudent given the high attrition rate of potential therapeutics due to unexpected cardiovascular liabilities discovered in late-stage clinical trials or post-market approval. In particular, the causal relationship of blood pressure changes that lead to risk of major adverse cardiac events suggests hemodynamic changes should be critically evaluated in preclinical studies of novel therapeutics.

Methods: Jacketed external telemetry with an implanted miniature blood pressure transmitter (JET-BP) was used to characterize the tolerability, functionality, and sensitivity of this study design in dogs. Thirty-six male or female beagles (n=6 dogs/sex/group) were administered vehicle control (reverse osmosis water) or etilefrine (1, 10mg/kg), sotalol (3, 30mg/kg), and hydralazine (1, 10mg/kg) on separate days. Telemetry data were evaluated for positive control article-related changes and retrospective power analysis was also completed. Animals were evaluated for instrumentation-related changes in clinical and anatomic pathology endpoints.

Results: All three positive controls elicited the expected pharmacologic responses that were statistically different at high and low doses. Retrospective power analysis confirmed this study design was able to statistically differentiate minor (approximately 5 to 15%) changes in electrocardiography and blood pressure values. This study also demonstrated the potential advantages of combining cardiovascular data across sex when the test article exposure and pharmacodynamics were consistent. Data collection using miniature telemetry blood pressure transmitters did not result in anatomic or clinical pathology findings that would prevent their use in general toxicology studies.

Discussion: This characterization study indicates that JET-BP in dogs offers a scientifically-robust method to evaluate novel therapeutics for potential cardiovascular liabilities.

Keywords: Blood pressure; Cardiovascular; Dogs; Electrocardiography; Methods; Nonclinical; Power analysis; QT interval; Safety pharmacology; Telemetry.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Blood Pressure / drug effects*
Cardiotoxicity / diagnosis*
Dogs
Dose-Response Relationship, Drug
Drug Evaluation, Preclinical / methods*
Electrocardiography / methods
Etilefrine / administration & dosage
Etilefrine / pharmacology
Female
Hydralazine / administration & dosage
Hydralazine / pharmacology
Male
Research Design
Sotalol / administration & dosage
Sotalol / pharmacology
Telemetry / methods*

Substances

Hydralazine
Sotalol
Etilefrine