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Semi-solid prodrug nanoparticles for long-acting delivery of water-soluble antiretroviral drugs within combination HIV therapies

机译:半固体前药纳米颗粒可在HIV联合疗法中长效递送水溶性抗逆转录病毒药物

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摘要

The increasing global prevalence of human immunodeficiency virus (HIV) is estimated at 36.7 million people currently infected. Lifelong antiretroviral (ARV) drug combination dosing allows management as a chronic condition by suppressing circulating viral load to allow for a near-normal life; however, the daily burden of oral administration may lead to non-adherence and drug resistance development. Long-acting (LA) depot injections of nanomilled poorly water-soluble ARVs have shown highly promising clinical results with drug exposure largely maintained over months after a single injection. ARV oral combinations rely on water-soluble backbone drugs which are not compatible with nanomilling. Here, we evaluate a unique prodruganoparticle formation strategy to facilitate semi-solid prodrug nanoparticles (SSPNs) of the highly water-soluble nucleoside reverse transcriptase inhibitor (NRTI) emtricitabine (FTC), and injectable aqueous nanodispersions; in vitro to in vivo extrapolation (IVIVE) modelling predicts sustained prodrug release, with activation in relevant biological environments, representing a first step towards complete injectable LA regimens containing NRTIs.
机译:据估计,目前全球感染人类免疫缺陷病毒的人数为3670万人。终生抗逆转录病毒(ARV)药物联合给药可通过抑制循环病毒载量来维持接近正常的寿命,从而将其作为慢性病进行管理;然而,口服的日常负担可能导致不粘连和耐药性的发展。纳米级水溶性差的抗逆转录病毒药物的长效(LA)储库注射已显示出非常有前途的临床结果,单次注射后数月内基本上保持了药物暴露。 ARV口服组合物依赖与纳米研磨不相容的水溶性骨架药物。在这里,我们评估了独特的前药/纳米颗粒形成策略,以促进高度水溶性核苷逆转录酶抑制剂(NRTI)恩曲他滨(FTC)的半固体前药纳米颗粒(SSPN)和可注射的水性纳米分散体;体外到体内外推(IVIVE)建模预测了前药的持续释放,并在相关的生物环境中被激活,这是迈向包含NRTIs的完整可注射LA方案的第一步。

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