HIV-1遗传变异及其临床意义。

ISRN Microbiology Pub Date : 2013-06-17 Print Date: 2013-01-01 DOI:10.1155/2013/481314
Maria Mercedes Santoro, Carlo Federico Perno
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引用次数: 148

摘要

尽管抗逆转录病毒疗法取得了进展,使艾滋病毒疾病管理发生了革命性的变化,但对艾滋病毒感染的有效控制仍然难以捉摸。除了典型的非B型流行地区,HIV-1非B亚型感染在以前的B亚型同质地区(如欧洲和北美)急剧增加。众所周知,几项研究表明,在非B亚型中,C和D亚型在疾病进展方面更具攻击性。幸运的是,不同亚型对抗逆转录病毒药物对HIV-1的反应似乎相似,但这些结果主要基于小型或设计拙劣的研究。另一方面,已经观察到非B亚型之间耐药性获得率的差异。这种不同的倾向,除了所使用的治疗方案类型之外,以及在非B流行地区进行病毒载量测试的机会,似乎是由于HIV-1分支的特殊性。事实上,与B亚型相比,一些非B亚型更容易产生耐药性。这种现象可能与亚型特异性多态性的存在、不同的密码子使用和/或亚型特异的RNA模板有关。这篇综述旨在全面了解HIV-1基因多样性及其对HIV-1疾病传播、治疗有效性和耐药性发展的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

HIV-1 Genetic Variability and Clinical Implications.

HIV-1 Genetic Variability and Clinical Implications.

HIV-1 Genetic Variability and Clinical Implications.

Despite advances in antiretroviral therapy that have revolutionized HIV disease management, effective control of the HIV infection pandemic remains elusive. Beyond the classic non-B endemic areas, HIV-1 non-B subtype infections are sharply increasing in previous subtype B homogeneous areas such as Europe and North America. As already known, several studies have shown that, among non-B subtypes, subtypes C and D were found to be more aggressive in terms of disease progression. Luckily, the response to antiretrovirals against HIV-1 seems to be similar among different subtypes, but these results are mainly based on small or poorly designed studies. On the other hand, differences in rates of acquisition of resistance among non-B subtypes are already being observed. This different propensity, beyond the type of treatment regimens used, as well as access to viral load testing in non-B endemic areas seems to be due to HIV-1 clade specific peculiarities. Indeed, some non-B subtypes are proved to be more prone to develop resistance compared to B subtype. This phenomenon can be related to the presence of subtype-specific polymorphisms, different codon usage, and/or subtype-specific RNA templates. This review aims to provide a complete picture of HIV-1 genetic diversity and its implications for HIV-1 disease spread, effectiveness of therapies, and drug resistance development.

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