The effects of pretransportation or arrival meloxicam administration to calves entering the feedlot on morbidity, biomarkers, performance, and carcass characteristics

Nicholas K Van Engen; Terry J Engelken; Caleb G Lockard; Jeffery Lakritz; Natalia Cernicchiaro; Blake K Wilson; Clint R Krehbiel; Johann F Coetzee

doi:10.1093/tas/txz070

The effects of pretransportation or arrival meloxicam administration to calves entering the feedlot on morbidity, biomarkers, performance, and carcass characteristics

Transl Anim Sci. 2019 May 13;3(2):620-632. doi: 10.1093/tas/txz070. eCollection 2019 Mar.

Authors

Nicholas K Van Engen¹, Terry J Engelken¹, Caleb G Lockard², Jeffery Lakritz³, Natalia Cernicchiaro⁴, Blake K Wilson², Clint R Krehbiel², Johann F Coetzee⁴

Affiliations

¹ Department of Veterinary Diagnostics and Production Medicine, College of Veterinary Medicine, Iowa State University, Ames, IA.
² Department of Animal Science, Oklahoma State University, Stillwater, OK.
³ Department of Veterinary Clinical Sciences, College of Veterinary Medicine, The Ohio State University, Colombus, OH.
⁴ Department of Anatomy and Physiology and Diagnostic Medicine/Pathobiology, College of Veterinary Medicine, Kansas State University, Manhattan, KS.

Abstract

The objective of this trial was to investigate the effects of using meloxicam as a pretransport or on arrival therapeutic on disease outcomes of bovine respiratory disease (BRD), biomarker outcomes associated with BRD, performance characteristics over the first 42 d on feed, and carcass traits at harvest in cross bred beef cattle. Multisourced, crossbred steer calves (n = 168) consisting of mainly British and British-Continental breeds were purchased from an auction market in central Missouri. Calves were processed prior to transportation and again upon feedlot arrival. Animals were randomized to 3 separate treatments: pretransport meloxicam (PMEL), arrival meloxicam (AMEL), and a control group receiving inactive excipient (CONT). Dosing at 1 mg/kg on weighted averaged administered per os. Animals were weighed and blood was collected pre- and post-transport. Haptoglobin (Hp)-matrix metaloproteinase (MMP)-9 complex, cortisol, and substance P were quantified. Weights were taken again at 42 d and at harvest. Clinical signs of BRD were monitored using indicators of depression, appetite, respiration, and temperature that qualified the animals for treatment. Harvest parameters were collected using a standardized United States Department of Agriculture grading system for quality grade and yield grade. Meloxicam did not have a significant effect on BRD morbidity over the course of the study and there was no significant effect on performance characteristics at 42 d (P > 0.10). Of the calves that did succumb to BRD, no significant differences were found in severity of disease (P > 0.10). Concentrations of substance P and Hp- MMP-9, were increased on arrival (P ≤ 0.05) however no significant treatment effect or interaction were found between AMEL, PMEL, CONT, or across different levels of biomarkers (P > 0.10). Meloxicam use prior to or on arrival does not mitigate disease or improve performance during the feeding period.

Keywords: biomarkers; bovine respiratory disease; cattle; meloxicam; performance.