Evaluation of the translation of multiple cardiovascular regulatory mechanisms in the anesthetized dog

被引:0
作者
Antic, Olivera [1 ,2 ]
Koshman, Yevgeniya E. [1 ]
Bird, Brandan M. [1 ]
Jasiek, Geena [1 ]
Wilsey, Amanda S. [1 ]
Mittelstadt, Scott W. [1 ]
Foley, C. Michael
机构
[1] Abbvie Inc, 1 North Waukegan Rd, N Chicago, IL 60064 USA
[2] Abbvie Inc, Safety Pharmacol, Bld AP9A,01L9A,1 N Waukegan Rd, N Chicago, IL 60064 USA
关键词
Anesthetized dog; Cardiovascular regulatory mechanism; Nonclinical; Safety pharmacology; LEFT-VENTRICULAR FUNCTION; DRUG-INDUCED CHANGES; HEART-RATE; IVABRADINE; ATROPINE; PHARMACOKINETICS; AMLODIPINE; PRAZOSIN; HYDROCHLOROTHIAZIDE; CONTRACTILITY;
D O I
10.1016/j.vascn.2024.107497
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The strategic and targeted use of an anesthetized canine cardiovascular model early in drug discovery enables a comprehensive cardiovascular and electrophysiological assessment of potential safety liabilities and guides compound selection prior to initiation of chronic toxicological studies. An ideal model would enable exposureresponse relationships to guide safety margin calculations, have a low threshold to initiate, and have quick delivery of decision quality data. We have aimed to profile compounds with diverse mechanism of actions (MoAs) of " non-QT " cardiovascular drug effects and evaluate the ability of nonclinical in vivo cardiovascular models to detect clinically reported effects. The hemodynamic effects of 11 drugs (atropine, itraconazole, atenolol, ivabradine, milrinone, enalaprilat, fasudil, amlodipine, prazosin, amiloride, and hydrochlorothiazide) were profiled in an anesthetized dog cardiovascular model. Derived parameters included: heart rate, an index of left ventricular contractility, mean arterial pressure, systemic vascular resistance, and cardiac output. Species specific plasma protein data was generated (human, dog) and utilized to calculate free drug concentrations. Using the anesthetized dog cardiovascular model, 10 of the 11 drugs displayed the predicted changes in CV parameters based on their primary MoAs and corresponding clinically described effects. Interestingly but not unexpected, 1 of 11 failed to display their predicted CV pattern which is likely due to a delay in pharmacodynamic effect that is beyond the duration of the experimental model (hydrochlorothiazide). The analysis from the current study supports the strategic use of the anesthetized dog model early in the drug discovery process for a comprehensive cardiovascular evaluation with good translation to human.
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页数:14
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