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The Cellular Pharmacokinetics of HIV Protease Inhibitors: Current Knowledge and Future Perspectives

机译:HIV蛋白酶抑制剂的细胞药代动力学:当前知识和未来观点。

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摘要

HIV protease inhibitors (Pis) are the cornerstone of Highly Active Antiretroviral Therapy (HAART). Their antiretroviral potent is attributable to their pharmacokinetic properties. Yet, as the pharmacologic target of HIV Pis is localized within HIV-infected cells, cellular pharmacokinetic properties must also be determined to predict not only efficacy, but also toxicity. In this review, we review recent studies about cellular pharmacokinetics of current marketed HIV Pis, as well as the physicochemical properties of HIV Pis and their drug transporters and enzymes. Additionally, a summary of potential strategies for optimizing cellular pharmacokinetics of HIV Pis and initial ideas to study cellular pharmacokinetics is also discussed. Cellular pharmacokinetics of HIV Pis is an important budding field of research that will significantly influence efficacy and toxicity profiles of these essential drugs, and we hope our review will aid in fundamental knowledge for future research.
机译:HIV蛋白酶抑制剂(Pis)是高效抗逆转录病毒疗法(HAART)的基石。它们的抗逆转录病毒效力归因于它们的药代动力学特性。然而,由于HIV Pis的药理学靶标位于HIV感染的细胞内,因此还必须确定细胞药代动力学特性,以不仅预测功效,而且预测毒性。在这篇综述中,我们回顾了有关当前上市的HIV Pis的细胞药代动力学的最新研究,以及HIV Pis及其药物转运蛋白和酶的理化性质。此外,还讨论了优化HIV Pis的细胞药代动力学的潜在策略和研究细胞药代动力学的初步思路。 HIV Pis的细胞药代动力学是一个重要的新兴研究领域,它将显着影响这些基本药物的功效和毒性谱,我们希望我们的综述将有助于基础知识,以便将来进行研究。

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