首页> 美国卫生研究院文献>AIDS Research and Human Retroviruses >Genetic Diversity and Naturally Polymorphisms in HIV Type 1 Integrase Isolates from Maputo Mozambique: Implications for Integrase Inhibitors
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Genetic Diversity and Naturally Polymorphisms in HIV Type 1 Integrase Isolates from Maputo Mozambique: Implications for Integrase Inhibitors

机译:来自莫桑比克马普托的HIV 1型整合酶分离株的遗传多样性和自然多态性:对整合酶抑制剂的影响。

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摘要

HIV proviral DNA integration into the host chromosome is carried out by integrase becoming an important target antiretroviral therapy. Raltegravir was the first integrase inhibitor approved for use in HIV therapy and elvitegravir is in the late phase of clinical development; both show good results in monotherapy studies and may be used worldwide for rescue therapy. In this work we analyzed 57 integrase sequences obtained from samples from drug-naive and first line regime-failing patients from Maputo, Mozambique, to evaluate the presence of natural polymorphisms and resistance mutations associated with raltegravir and elvitegravir. No major mutations conferring resistance to integrase inhibitors were found and polymorphic accessory mutations were solely observed in low frequency among subtype C sequences—L74M (3.4%), T97A (1.8%), and E157Q (1.8%)—suggesting that this new antiretroviral drug class will be effective in Mozambique providing a good perspective to the introduction of this class of drugs in that country.
机译:HIV前病毒DNA整合入宿主染色体是通过整合酶进行的,该整合酶成为重要的抗逆转录病毒治疗靶标。 Raltegravir是第一个被批准用于HIV治疗的整合酶抑制剂,elvitegravir处于临床开发的后期。两者在单药治疗研究中均显示出良好的效果,并且可能在全球范围内用于抢救治疗。在这项工作中,我们分析了来自莫桑比克马普托的未经药物治疗和一线治疗失败的患者样本的57个整合酶序列,以评估与raltegravir和elvitegravir相关的天然多态性和耐药突变的存在。没有发现赋予整合酶抑制剂抗性的重大突变,仅在低频的C型亚型L74M(3.4%),T97A(1.8%)和E157Q(1.8%)中观察到多态性辅助突变,这表明该新抗逆转录病毒药物该类药物将在莫桑比克有效,为在该国引入此类药物提供良好的前景。

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