Efficacy and safety of a novel oral isoxazoline, sarolaner (Simparica™), for the treatment of sarcoptic mange in dogs

Csilla Becskei; Filip De Bock; Joanna Illambas; Judith A Cherni; Josephus J Fourie; Melanie Lane; Sean P Mahabir; Robert H Six

doi:10.1016/j.vetpar.2016.02.017

Efficacy and safety of a novel oral isoxazoline, sarolaner (Simparica™), for the treatment of sarcoptic mange in dogs

Vet Parasitol. 2016 May 30:222:56-61. doi: 10.1016/j.vetpar.2016.02.017. Epub 2016 Feb 20.

Authors

Csilla Becskei¹, Filip De Bock², Joanna Illambas², Judith A Cherni³, Josephus J Fourie⁴, Melanie Lane³, Sean P Mahabir³, Robert H Six³

Affiliations

¹ Zoetis, Veterinary Medicine Research and Development, Mercuriusstraat 20, Zaventem 1930, Belgium. Electronic address: csilla.becskei@zoetis.com.
² Zoetis, Veterinary Medicine Research and Development, Mercuriusstraat 20, Zaventem 1930, Belgium.
³ Zoetis, Veterinary Medicine Research and Development, 333 Portage St., Kalamazoo, MI 49007, USA.
⁴ ClinVet International (Pty) Ltd., Uitsigweg, Bainsvlei 9338, Bloemfontein, Republic of South Africa.

PMID: 26928658
DOI: 10.1016/j.vetpar.2016.02.017

Abstract

The efficacy of the novel isoxazoline, sarolaner (Simparica™) was investigated in dogs with clinical signs consistent with sarcoptic mange and harbouring natural infestations of Sarcoptes scabiei. One placebo-controlled laboratory study and one multi-centred field study with a commercial comparator containing imidacloprid/moxidectin (Advocate(®) spot-on) were conducted. Oral or topical treatments were administered on Days 0 and 30. Up to 10 skin scrapings were taken for the assessment of S. scabiei infestations from each dog before treatment and on Days 14, 30, 44 and 60 in the laboratory study, and on Days 30 and 60 in the field study. In the laboratory study, efficacy was calculated based on the percent reduction of mean live mite counts compared to the placebo group. In the field study parasitological cure rate (% dogs free of mites) was determined and non-inferiority of sarolaner to the control product was assessed. In the laboratory study 44 mixed breed dogs were enrolled in four batches. Due to decreasing mite counts in the placebo treated dogs, immunosuppression with dexamethasone (0.4mg/kg three times per week for two weeks) was initiated in all dogs on study at that time (n=6) and those subsequently enrolled (n=14). In the field study, dogs were enrolled in a 2:1 ratio (sarolaner:comparator); 79 dogs were assessed for efficacy and safety, and an additional 45 dogs were assessed for safety only. There were no treatment related adverse events in either study. In the laboratory study, no mites were found on any sarolaner-treated dogs 14 days after the first treatment except for one dog that had a single mite on Day 44. In the field study, the parasitological cure rate was 88.7% and 100% in the sarolaner group and 84.6% and 96.0% in the imidacloprid/moxidectin group, on Days 30 and 60, respectively. Statistical analysis showed that sarolaner was non-inferior to imidacloprid/moxidectin at both time points. The clinical signs of sarcoptic mange, including hair loss, papules, pruritus, erythema, and scaling/crusting improved throughout the study. Sarolaner was safe, achieved 100% reduction in the numbers of S. scabiei detected and resulted in marked improvement of the clinical signs of sarcoptic mange in dogs following two monthly oral administrations.

Keywords: Dog; Efficacy; Isoxazoline; Palatability; Safety; Sarcoptes scabiei; Sarcoptic mange; Sarolaner; Simparica™.

MeSH terms

Administration, Oral
Administration, Topical
Animals
Dog Diseases / drug therapy
Dogs
Female
Insecticides / administration & dosage
Insecticides / standards
Isoxazoles / administration & dosage*
Isoxazoles / standards
Male
Parasite Load
Scabies / drug therapy
Scabies / veterinary*
Treatment Outcome

Substances

Insecticides
Isoxazoles