Plasma Cytokeratin 18 and fecal Alpha‐1 Antitrypsin concentrations in dogs with osteosarcoma receiving carboplatin chemotherapy

Kathryn Taikowski; Adam J. Rudinsky; Darian S. Louke; Emma Warry; Joelle M. Fenger

doi:10.1002/vms3.392

Veterinary Medicine and Science (Mar 2021)

Plasma Cytokeratin 18 and fecal Alpha‐1 Antitrypsin concentrations in dogs with osteosarcoma receiving carboplatin chemotherapy

Kathryn Taikowski,
Adam J. Rudinsky,
Darian S. Louke,
Emma Warry,
Joelle M. Fenger

Affiliations

Kathryn Taikowski: Department of Veterinary Clinical Sciences College of Veterinary Medicine The Ohio State University Columbus OH USA
Adam J. Rudinsky: Department of Veterinary Clinical Sciences College of Veterinary Medicine The Ohio State University Columbus OH USA
Darian S. Louke: Department of Veterinary Clinical Sciences College of Veterinary Medicine The Ohio State University Columbus OH USA
Emma Warry: Department of Small Animal Clinical Sciences College of Veterinary Medicine Texas A&M University College Station TX USA
Joelle M. Fenger: Department of Veterinary Clinical Sciences College of Veterinary Medicine The Ohio State University Columbus OH USA

DOI: https://doi.org/10.1002/vms3.392
Journal volume & issue: Vol. 7, no. 2
pp. 385 – 392

Abstract

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Abstract Gastrointestinal (GI) toxicosis is a common side effect of cytotoxic chemotherapy treatment in humans and dogs. Measurement of cytokeratin 18 (CK18), an intracellular structural protein released during epithelial apoptosis, and Alpha1‐Antitrypsin (A1AT) in faeces provides a mechanism for evaluating damage to the intestinal mucosa secondary to cytotoxic chemotherapy. Our goal was to evaluate the clinical utility of plasma CK18 and faecal A1‐AT levels as non‐invasive biomarkers of cytotoxic chemotherapy induced GI toxicity. We conducted a prospective cohort study in dogs (N = 10) with osteosarcoma undergoing amputation followed by carboplatin chemotherapy. We hypothesized that plasma CK18 and faecal A1‐AT levels would increase following carboplatin administration due to drug‐induced GI epithelial damage/apoptosis, and that plasma CK18 and faecal A1‐AT levels would correlate with severity of GI toxicity. Mean baseline plasma CK18 concentration was variable amongst patients; however, CK18 concentration prior to carboplatin chemotherapy treatment was not significantly different from CK18 levels after treatment. There was significant intra and inter‐patient variability in mean faecal A1‐AT levels at baseline. Mean A1‐AT concentration did not change significantly from day 0 to day 21. Gastrointestinal toxicity was minimal; therefore, we were unable to determine the association of plasma CK18 and faecal A1‐AT concentrations with development of GI toxicosis. In this study population, plasma CK18 and faecal A1‐AT concentration were not clinically useful biomarkers for the detection of GI toxicosis secondary to carboplatin administration. Further prospective evaluation of CK18 and A1‐AT as biomarkers of drug‐induced GI toxicity is warranted in a larger cohort of dogs receiving cytotoxic chemotherapy. AVMA clinical trial registration number: AAHSD004827.

Published in Veterinary Medicine and Science

ISSN: 2053-1095 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Agriculture: Animal culture: Veterinary medicine
Website: https://onlinelibrary.wiley.com/journal/20531095

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