Oral dosing of the nucleoside analog obeldesivir is efficacious against RSV infection in African green monkeys

口服核苷类似物奥贝地西韦对非洲绿猴的呼吸道合胞病毒感染有效。

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作者:Jared Pitts #,J Lizbeth Reyes Zamora #,Savrina Manhas,Thomas Aeschbacher,Josolyn Chan,Vincent Cutillas,Varsha Nair,Nicholas C Riola,Arya Vijjapurapu,Meghan S Vermillion,Stacey Eng,Christopher Richards,Dong Han,Jason K Perry,Subhra Chaudhuri,Szu-Wen Liu,Clarissa Martinez,Nadine Peinovich,Kai-Hui Sun,Arthur Cai,Ross Martin,Jasmine Moshiri,Charlotte Hedskog,Darius Babusis,Dustin S Siegel,Rao Kalla,Vasanthi Avadhanula,Pedro A Piedra,Kim Stobbelaar,Peter L Delputte,Caleb Marceau,Roberto Mateo,Evguenia Maiorova,Hongmei Mo,Raju Subramanian,Richard L Mackman,Tomas Cihlar,Simon P Fletcher,John P Bilello

Abstract

Respiratory syncytial virus (RSV) is a significant cause of morbidity and mortality in high-risk populations. Although prophylactic options are available, there are no effective oral therapeutics for RSV infection. Obeldesivir (ODV) is an orally bioavailable prodrug of the nucleoside analog GS-441524, which is converted intracellularly to its active nucleoside triphosphate and inhibits the RSV RNA polymerase. Here we report the potent antiviral activity of ODV against geographically and temporally diverse RSV A and B clinical isolates (EC50: 0.20-0.66 μM). Resistance selection studies with ODV and GS-441524 against RSV identify a single amino acid substitution, I777L, in the L polymerase with reduced susceptibility (3.3-3.8-fold) to ODV and GS-441524, indicating a high barrier for resistance development. In an African green monkey RSV infection model, once-daily oral ODV doses of 30 or 90 mg/kg initiated ~24 hours post-infection significantly reduces log10 viral RNA copies/mL × day area under the curve by 69-92% in the upper and lower respiratory tracts. Together, these preclinical data support the clinical evaluation of ODV for the treatment of RSV infection.

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