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首页> 外文期刊>BMC Microbiology >Analysis of HIV-1 drug resistant mutations by line probe assay and direct sequencing in a cohort of therapy naive HIV-1 infected Italian patients
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Analysis of HIV-1 drug resistant mutations by line probe assay and direct sequencing in a cohort of therapy naive HIV-1 infected Italian patients

机译:在未接受过HIV-1感染的意大利初治患者队列中通过线探针分析和直接测序分析HIV-1耐药性突变

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The routine determination of drug resistance in newly HIV-1 infected individuals documents a potential increase in the transmission of drug-resistant variants. Plasma samples from twenty seven therapy naive HIV-1 infected Italian patients were analyzed by the line probe assay (LIPA) and the TruGene HIV-1 assay for the detection of mutations conferring resistance to HIV-1. Both tests disclosed amino-acid substitutions associated with resistance in a variable number of patients. In particular, two mutations (K70R and V118I), detectable by LIPA and by sequencing analysis respectively, revealed resistance to NRTIs in two plasma samples. At least three mutations conferring resistance to NNRTIs, not detectable by commercial LIPA, able to reveal mutations associated only with nucleoside reverse transcriptase analogues, were disclosed by viral sequence analysis. Moreover, most samples showed mutations correlated with resistance to protease inhibitors. Remarkably, a key mutation, like V82A (found as a mixture), and some "indeterminate" results (9 samples), due the absence of signal on the lines corresponding to a specific probe, was revealed only by LIPA, while a variable number of secondary mutations was detectable only by TruGene HIV-1 assay. Even if further studies are necessary to establish the impact of different tests on the evaluation of drug-resistant strains transmission, LIPA might be useful in a wide population analysis, where bulk results are needed in a short time, while sequencing analysis, able to detect mutations conferring resistance to both NRTIs and NNRTIs, might be considered a more complete assay, albeit more expensive and more technically complex.
机译:在新感染HIV-1的个体中常规检测耐药性表明耐药性变异的传播可能增加。通过线探针测定法(LIPA)和TruGene HIV-1测定法分析了来自27名接受过HIV-1初始治疗的意大利患者的血浆样品,以检测赋予对HIV-1的抗性的突变。两项测试均揭示了在可变数量的患者中与耐药相关的氨基酸取代。特别地,分别通过LIPA和测序分析可检测到的两个突变(K70R和V118I)揭示了在两个血浆样品中对NRTI的抗性。通过病毒序列分析公开了至少三种赋予对NNRTIs抗性的突变,其不能被商业LIPA检测到,其能够揭示仅与核苷逆转录酶类似物相关的突变。而且,大多数样品显示出与蛋白酶抑制剂抗性相关的突变。值得注意的是,只有LIPA揭示了关键突变,如V82A(作为混合物)和一些“不确定”结果(9个样品),这是由于对应于特定探针的线上没有信号,而可变数是仅通过TruGene HIV-1检测可检测到二次突变。即使需要进一步的研究来确定不同测试对耐药菌株传播评估的影响,LIPA仍可用于广泛的人群分析,在短时间内需要大量结果的同时,测序分析可以检测赋予NRTIs和NNRTIs耐药性的突变,尽管更昂贵,技术也更复杂,但可以认为是更完整的检测方法。

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