Mechanistic Investigations of Test Article–Induced Pancreatic Toxicity at the Endocrine–Exocrine Interface in the Rat

Author:

Brenneman Karrie A.1,Ramaiah Shashi K.2,Rohde Cynthia M.3,Messing Dean M.1,O’Neil Shawn P.1,Gauthier Lauren M.1,Stewart Zachary S.1,Mantena Srinivasa R.1,Shevlin Kimberly M.1,Leonard Christopher G.1,Sokolowski Sharon A.4,Lin Hungyun2,Carraher Deborah C.1,Jesson Michael I.2,Tomlinson Lindsay2,Zhan Yutian1,Bobrowski Walter F.4,Bailey Steven A.1,Vogel W. Mark2,Morris Dale L.2,Whiteley Laurence O.2,Davis John W.1

Affiliation:

1. Pfizer, Worldwide Research & Development, Andover, Massachusetts, USA

2. Pfizer, Worldwide Research & Development, Cambridge, Massachusetts, USA

3. Pfizer, Worldwide Research & Development, Pearl River, New York, USA

4. Pfizer, Worldwide Research & Development, Groton, Connecticut, USA

Abstract

Pancreatic toxicity commonly affects the endocrine or exocrine pancreas. However, it can also occur at the endocrine–exocrine interface (EEI), where the capillary network of the islet merges with the capillaries of the surrounding acinar tissue, that is, the insulo-acinar portal system. The goal of this article is to describe a novel, test article–induced pancreatic toxicity that originated at the EEI and to summarize investigations into the mechanistic basis of the injury. This injury was initially characterized by light microscopy in 7/14 day-toxicity studies in Sprague-Dawley (Crl: CD®[SD]) rats with undisclosed test articles. Microvascular injury at the interface resulted in peri-islet serum exudation, fibrin deposition, hemorrhage, inflammation, and secondary degeneration/necrosis of surrounding exocrine tissue. More chronic injury presented as islet fibrosis and lobular atrophy. Direct cytotoxicity affecting the capillary endothelium at the EEI was confirmed ultrastructurally on day 4. Endothelial microparticle and blood flow studies further confirmed endothelial involvement. Similar lesions occurred less frequently in 2 other rat strains and not in the mouse, dog, or cynomolgus macaque. In summary, in vivo and investigative study data confirmed primary endothelial cytotoxicity in the pathogenesis of this lesion and suggested that the lesion may be rat/rat strain–specific and of uncertain relevance for human safety risk assessment.

Publisher

SAGE Publications

Subject

Cell Biology,Toxicology,Molecular Biology,Pathology and Forensic Medicine

Reference28 articles.

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1. Interactions between the Exocrine and the Endocrine Pancreas;Journal of Clinical Medicine;2024-02-19

2. Current Assays in Endocrine Safety Pharmacology;Drug Discovery and Evaluation: Safety and Pharmacokinetic Assays;2024

3. Exocrine Pancreas;Haschek and Rousseaux' s Handbook of Toxicologic Pathology;2024

4. Endocrine System;Haschek and Rousseaux' s Handbook of Toxicologic Pathology;2024

5. Off-target pharmacological activity at various kinases: Potential functional and pathological side effects;Journal of Pharmacological and Toxicological Methods;2023-09

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