Sanjay Menon
Zoetis
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Featured researches published by Sanjay Menon.
Veterinary Parasitology | 2016
Tom L. McTier; Nathan Anthony Logan Chubb; Michael P. Curtis; Laura Hedges; Gregory A. Inskeep; Christopher S. Knauer; Sanjay Menon; Brian Mills; Aleah Pullins; Erich Zinser; Debra J. Woods; Patrick F.M. Meeus
The novel isoxazoline ectoparasiticide, sarolaner, was identified during a lead optimization program for an orally-active compound with efficacy against fleas and ticks on dogs. The aim of the discovery program was to identify a novel isoxazoline specifically for use in companion animals, beginning with de novo synthesis in the Zoetis research laboratories. The sarolaner molecule has unique structural features important for its potency and pharmacokinetic (PK) properties, including spiroazetidine and sulfone moieties. The flea and tick activity resides in the chirally pure S-enantiomer, which was purified to alleviate potential off-target effects from the inactive enantiomer. The mechanism of action was established in electrophysiology assays using CHO-K1 cell lines stably expressing cat flea (Ctenocephalides felis) RDL (resistance-to-dieldrin) genes for assessment of GABA-gated chloride channel (GABACls) pharmacology. As expected, sarolaner inhibited GABA-elicited currents at both susceptible (CfRDL-A285) and resistant (CfRDL-S285) flea GABACls with similar potency. Initial whole organism screening was conducted in vitro using a blood feeding assay against C. felis. Compounds which demonstrated robust activity in the flea feed assay were subsequently tested in an in vitro ingestion assay against the soft tick, Ornithodoros turicata. Efficacious compounds which were confirmed safe in rodents at doses up to 30mg/kg were progressed to safety, PK and efficacy studies in dogs. In vitro sarolaner demonstrated an LC80 of 0.3μg/mL against C. felis and an LC100 of 0.003μg/mL against O. turicata. In a head-to-head comparative in vitro assay with both afoxolaner and fluralaner, sarolaner demonstrated superior flea and tick potency. In exploratory safety studies in dogs, sarolaner demonstrated safety in dogs≥8 weeks of age upon repeated monthly dosing at up to 20mg/kg. Sarolaner was rapidly and well absorbed following oral dosing. Time to maximum plasma concentration occurred within the first day post-dose. Bioavailability for sarolaner was calculated at >85% and the compound was highly protein bound (>99.9%). The half-life for sarolaner was calculated at 11-12 days. Sarolaner plasma concentrations indicated dose proportionality over the range 1.25-5mg/kg, and these same doses provided robust efficacy (>99%) for ≥35days against both fleas (C. felis) and multiple species of ticks (Rhipicephalus sanguineus, Ixodes ricinus and Dermacentor reticulatus) after oral administration to dogs. As a result of these exploratory investigations, sarolaner was progressed for development as an oral monthly dose for treatment and control of fleas and ticks on dogs.
Bioorganic & Medicinal Chemistry Letters | 2016
Michael P. Curtis; Valerie A. Vaillancourt; Richard M. Goodwin; Nathan Anthony Logan Chubb; William Howson; Tom L. McTier; Aleah Pullins; Erich Zinser; Patrick F.M. Meeus; Debra J. Woods; Laura Hedges; Tim Stuk; Jeffrey E. Price; Jason Koch; Sanjay Menon
Over the last decade, the isoxazoline motif has become the intense focus of crop protection and animal health companies in their search for novel pesticides and ectoparasiticides. Herein we report the discovery of sarolaner, a proprietary, optimized-for-animal health use isoxazoline, for once-a-month oral treatment of flea and tick infestation on dogs.
Bioorganic & Medicinal Chemistry Letters | 2014
Michael P. Curtis; Nathan Anthony Logan Chubb; Edmund L. Ellsworth; Richard M. Goodwin; Sue Holzmer; Jason Koch; Tom L. McTier; Sanjay Menon; Kent Mills; Aleah Pullins; Tim Stuk; Erich Zinser
Haematobia irritans (horn fly) infestation in cattle is responsible for over a billion dollars a year in global economic loss due to decreased milk production and lower feed conversion. There is significant need for new insecticidal agents since current treatments such as organophosphates and pyrethroids suffer from field resistance. Isoxazoline oxime ethers represent a new class of γ-aminobutyric acid (GABA) receptor channel blockers which show good activity (LD(90) = 1.0 μg/mL) against horn flies in an in vitro feed assay and have demonstrated efficacy (>90% reduction at 1.0mg/kg) as a topical treatment in a field study.
Angewandte Chemie | 2006
Alexander Dömling; Barbara Beck; Uwe Eichelberger; Sukumar Sakamuri; Sanjay Menon; Quin-Zene Chen; Yingchun Lu; Ludger A. Wessjohann
Archive | 2003
Alexander Dömling; Bernd Henkel; Barbara Beck; Katrin Illgen; Sukumar Sakamuri; Sanjay Menon
Bioorganic & Medicinal Chemistry Letters | 2006
Walfrido Antuch; Sanjay Menon; Quin-Zene Chen; Yingchun Lu; Sukumar Sakamuri; Barbara Beck; Vesna Schauer-Vukašinović; Seema Agarwal; Sibylle Hess; Alexander Dömling
Archive | 2011
Valerie A. Vaillancourt; Nathan Anthony Logan Chubb; Michael P. Curtis; William Howson; Graham M. Kyne; Sanjay Menon; Susan M. K. Sheehan; Donald James Skalitzky; John Adam Wendt
Molecular Cancer Therapeutics | 2007
Natalia Skobeleva; Sanjay Menon; Lutz Weber; Erica A. Golemis; Vladimir Khazak
Bioorganic & Medicinal Chemistry Letters | 2004
Yingchun Lu; Sukumar Sakamuri; Quin-Zene Chen; Yen-Fang Keng; Vladimir Khazak; Katrin Illgen; Silke Schabbert; Lutz Weber; Sanjay Menon
Archive | 2011
Nathan Anthony Logan Chubb; Todd Michael Maddux; Sanjay Menon