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Pharmacological intervention of HIV-1 maturation

机译:HIV-1成熟的药理干预

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摘要

Despite significant advances in antiretroviral therapy, increasing drug resistance and toxicities observed among many of the current approved human immunodeficiency virus (HIV) drugs indicate a need for discovery and development of potent and safe antivirals with a novel mechanism of action. Maturation inhibitors (MIs) represent one such new class of HIV therapies. MIs inhibit a late step in the HIV-1 Gag processing cascade, causing defective core condensation and the release of non-infectious virus particles from infected cells, thus blocking the spread of the infection to new cells. Clinical proof-of-concept for the MIs was established with betulinic acid derived bevirimat, the prototype HIV-1 MI. Despite the discontinuation of its further clinical development in 2010 due to a lack of uniform patient response caused by naturally occurring drug resistance Gag polymorphisms, several second-generation MIs with improved activity against viruses exhibiting Gag polymorphism mediated resistance have been recently discovered and are under clinical evaluation in HIV/AID patients. In this review, current understanding of HIV-1 MIs is described and recent progress made toward elucidating the mechanism of action, target identification and development of second-generation MIs is reviewed.
机译:尽管抗逆转录病毒疗法取得了重大进展,但是在许多当前批准的人类免疫缺陷病毒(HIV)药物中观察到的耐药性和毒性增加表明,需要发现和开发具有新颖作用机制的有效且安全的抗病毒药物。成熟抑制剂(MIs)代表了这类新型的HIV治疗方法。 MIs抑制了HIV-1 Gag加工级联的后期步骤,导致缺陷的核心凝结和感染细胞中非感染性病毒颗粒的释放,从而阻止了感染向新细胞的传播。 MIs的临床概念证明是由桦木酸衍生的bevirimat(HIV-1 MI的原型)建立的。尽管由于自然发生的耐药性Gag多态性导致缺乏统一的患者反应,该药物在2010年停止了进一步的临床开发,但最近发现了一些具有改善的免疫力的第二代MI,这些病毒对表现出Gag多态性介导的耐药性的病毒具有较高的活性HIV / AID患者的评估。在这篇综述中,描述了对HIV-1 MIs的当前理解,并综述了在阐明第二代MIs的作用机理,目标识别和发展方面的最新进展。

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