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Emerging role of integrase inhibitors in the management of treatment-experienced patients with HIV infection

机译:整合酶抑制剂在治疗经验丰富的HIV感染患者管理中的新兴作用

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摘要

Integrase is an essential HIV-1-specific enzyme that is an active target for antiretroviral drug development. Recently, a new class of drugs that specifically inhibits strand transfer, one of the three steps of HIV integration into the host DNA, has been developed. Two drugs in this class have reached late stages of development for use in HIV-1 infected individuals: raltegravir, which has just been approved for use in treatment-experienced patients, and elvitegravir, currently in phase III trials. Both are potent with an IC50 in the 30 nM range and active in vitro against wild type as well as in strains highly resistant to all other existing classes of drugs. Clinical trials in both treatment-naïve and -experienced patients have demonstrated raltegravir to be highly effective with an excellent tolerability profile and no specific clinical or metabolic side effects. Longer follow up is necessary to ensure this early safety profile is sustained. The rapid rate of viral decay observed with raltegravir challenges the current understanding of HIV-1 turnover and may open new strategies for long term treatment and management of infected patients.
机译:整合酶是必不可少的HIV-1特异性酶,是抗逆转录病毒药物开发的积极目标。最近,已经开发出一种新的可特异性抑制链转移的药物,这是HIV整合入宿主DNA的三个步骤之一。该类中的两种药物已经进入开发阶段,可用于感染HIV-1的个体:刚刚批准用于治疗经验丰富的患者的raltegravir和目前正在进行III期试验的elvitegravir。两者均具有30 nM的IC50效力,并且在体外对野生型以及对所有其他现有药物高度耐药的菌株均具有活性。在未接受过治疗和有经验的患者中进行的临床试验表明,raltegravir是高效的,具有出色的耐受性,并且没有特定的临床或代谢副作用。必须进行更长的随访,以确保维持早期的安全状况。 raltegravir观察到的病毒衰减迅速,这对当前对HIV-1转化的理解提出了挑战,并可能为感染患者的长期治疗和管理打开新的策略。

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