Inflammation and Immunogenicity Limit the Utility of the Rabbit As a Nonclinical Species for Ocular Biologic Therapeutics

Overview

Journal Regul Toxicol Pharmacol

Publisher Elsevier

Specialties Pharmacology
Toxicology

Date 2017 Mar 22

PMID 28322894

Citations 11

Authors

Christina L Zuch de Zafra

Vito G Sasseville

Steven Matsumoto

Christian Freichel

Mark Milton

Timothy K MacLachlan

Cindy Farman

Iona Raymond

Swati Gupta

Ronald Newton

Elke-Astrid Atzpodien

Evan A Thackaberry

Affiliations

Soon will be listed here.

Abstract

The nonclinical safety evaluation of therapeutic drug candidates is commonly conducted in two species (rodent and non-rodent) in keeping with international health authority guidance. Biologic drugs typically have restricted species cross-reactivity, necessitating the evaluation of safety in non-human primates and thus limiting the utility of lower order species. Safety studies of cross-reactive ocular biologic drug candidates have been conducted in rabbits as a second toxicology species, despite the fact that rabbits are not a rodent species. Such studies are often confounded by the development of anti-drug antibodies and severe ocular inflammation, the latter requiring studies to be terminated prematurely for animal welfare reasons. Notably, these confounding factors preclude the interpretation of safety. Nonclinical toxicology programs should be designed with consideration of ethical animal use and 3Rs principles (Replacement, Reduction and Refinement). The experience of several pharmaceutical sponsors, demonstrating that toxicology studies of ocular (intravitreal and topical ocular) biologic drug candidates in the rabbit are of limited interpretive value, calls into question the utility of such studies in this species and indicates that such studies should not be conducted.

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