Author:
Gautam Nagsen,McMillan JoEllyn M.,Kumar Devendra,Bade Aditya N.,Pan Qiaoyu,Kulkarni Tanmay A.,Li Wenkuan,Smith Nathan A,Dyavar Shetty Bhagya L.,Sillman Brady,Szlachetka Adam,Edagwa Benson J.,Gendelman Howard E.,Alnouti Yazen
Abstract
AbstractA single, once every eight-week cabotegravir (CAB) long-acting parenteral is more effective than daily oral emtricitabine and tenofovir disoproxil fumarate in preventing human immunodeficiency virus type one (HIV-1) transmission. Extending CAB dosing to a yearly injectable can advance efforts leading to the elimination of viral transmission. The current submission adds rigor, reproducibility and mechanistic insights for the extended apparent half-life of a yearlong antiretroviral injectable. Pharmacokinetic (PK) profiles of a nanoformulated fatty acid ester CAB prodrug (named NM2CAB) were affirmed at two academic and one contract research laboratory. PK profiles showed plasma CAB levels at or above the protein-adjusted 90% inhibitory concentration for up to one year after a single dose. Measures of drug biodistribution demonstrated sustained native drug at the muscle injection site and in lymphoid tissues (spleen and lymph nodes). The results paralleled NM2CAB uptake and retention in human macrophages. NM2CAB nanocrystals were stable in blood, tissue and liver homogenates. The long apparent drug half-life followed pH-dependent slow prodrug release in weeks from the nanocrystal. In contrast, solubilized prodrug was hydrolyzed in hours in plasma and tissues recorded from multiple mammalian species at basic pH. No measurable toxicities were recorded. These results, taken together, affirm the pharmacological mechanistic properties of a year-long nanoformulated CAB prodrug supporting the established protocol design for formulation safety, rigor and reproducibility.
Publisher
Cold Spring Harbor Laboratory
Cited by
1 articles.
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1. Nanotechnology Based Drug Delivery for HIV-AIDS Treatment;AIDS Updates - Recent Advances and New Perspectives;2021-10-13