Reproductive and margin of safety of a fixed-dose combination injectable endectocide (0.2 mg/kg doramectin; 6.0 mg/kg levamisole hydrochloride) in cattle

Matthew J Krautmann; Matthew Edmonds; Jenifer Edmonds; Nicholas K Van Engen; Kevin Esch; Rodney K Frank; Erin Quist; Jezaniah Kira Tena; Kayla M Saad; Noelle Cotey; Andrew A DeRosa

doi:10.1016/j.vetpar.2023.110071

Reproductive and margin of safety of a fixed-dose combination injectable endectocide (0.2 mg/kg doramectin; 6.0 mg/kg levamisole hydrochloride) in cattle

Vet Parasitol. 2023 Nov:323S:110071. doi: 10.1016/j.vetpar.2023.110071. Epub 2023 Nov 10.

Affiliations

¹ Zoetis, Veterinary Medicine Research and Development, 333 Portage St, Kalamazoo, MI 49007 USA.
² Johnson Research LLC, 24007 Hwy 20-26, Parma, ID 83660, USA.
³ Zoetis, Veterinary Medicine Research and Development, 333 Portage St, Kalamazoo, MI 49007 USA. Electronic address: kevin.esch@zoetis.com.
⁴ Experimental Pathology Laboratories Inc, 615 Davis Drive Ste 500, Durham, NC 27713, USA.

PMID: 37951737
DOI: 10.1016/j.vetpar.2023.110071

Abstract

We present a fixed-dose combination injectable (FDCI) solution for cattle formulated for a single subcutaneous administration at a dose rate of 1 ml/25 kg of body weight to deliver a dose of 0.2 mg/kg of doramectin and 6.0 mg/kg of levamisole hydrochloride (5.1 mg/kg base equivalent). This drug product is marketed in the United States under the tradename Valcor® and in Australia and New Zealand under the tradename Dectomax V®. Both levamisole and doramectin have histories of safe and effective use in ruminants, with safety margins of 3X and 25X, respectively. Three studies were conducted to demonstrate the safety of the new FDCI: margin of safety (Study 1), and reproductive safety in sexually nulliparous beef heifers (Studies 2 and 3). In Study 1, 3-month-old sexually intact male and female calves were given either saline (control) or 1X, 2X, or 3X FDCI on Days 0, 14, and 28. General health, clinical, and neurological observations were made throughout the study, and clinical and pathology evaluations were made at study end. Studies 2 and 3 demonstrated the reproductive safety of the FDCI on sexually nulliparous beef heifers using estrus synchronization and timed artificial insemination. Treatments of either saline (control) or 3X FDCI were administered to coincide with either folliculogenesis, implantation, organogenesis, early gestation, or late gestation. Reproductive safety was demonstrated by evaluating rates of conception, calving, abortion, and stillbirth, dystocia scores, and calf health. In all studies, the FDCI at 1X, 2X, or 3X dosages was well tolerated. In the margin of safety study, 3X calves showed increased incidence of salivation for up to 8 h post-dosing compared to other groups. Injection sites were palpable post-dosing in all three FDCI groups but resolved by Day 28 in all but one animal each in 2X and 3X. In the reproductive safety studies, the FDCI had no effect on conception, pregnancy, fetal development, or postnatal viability. Injection site swelling was increased in frequency and duration compared to controls. The studies demonstrate the safety of the new FDCI in cattle from 3 months of age and in reproducing heifers during all reproductive stages from folliculogenesis through gestation and up to a month post-partum.

Keywords: Anthelmintic; Dectomax V®; Doramectin; Folliculogenesis; Implantation; Levamisole; Macrocyclic lactone; Margin of safety; Organogenesis; Pregnancy; Reproductive safety; Toxicology; Valcor®.

MeSH terms

Animals
Body Weight
Cattle
Female
Insemination, Artificial / veterinary
Ivermectin
Levamisole* / pharmacology
Male
Pregnancy
Reproduction*

Substances

doramectin
Levamisole
Ivermectin