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HIV Type 1 pol Gene Diversity and Antiretroviral Drug Resistance Mutations in Santos, Brazil

机译:巴西桑托斯的HIV 1型pol基因多样性和抗逆转录病毒药物耐药性突变

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HIV-1 antiretroviral drug resistance mutations in subtype B, F, and recombinants B/F in Santos, Brazil were characterized. We studied 83 samples from individuals enrolled at the Brazilian HIV/AIDS programs from Santos. These patients have been treated with multiantiretroviral therapy. Samples were collected in 2006; RNA was extracted from plasma and used as a target to amplify the pol gene of HIV-1. PCR products were sequenced on both strands, phylogenetic analyses were performed by neighbor-joining, and recombination was evaluated by bootscan. pol gene sequencing of the samples revealed that 54 strains belonged to subtype B, 4 were subtype F, 1 was subtype C, and 24 were B/F recombinants. Recombinant break points in 20 samples are the same identified in CRF28_BF and CRF29_BF. Drug resistance mutations identified in common to subtypes B, F, and recombinants B/F were protease inhibitors M46I/L (29%), I54V (24%), A71V (22%), and V82A/F (31%); reverse transcriptase nucleoside resistance mutations M41L (52%), D67N (30%), K70R (26%), M184V (88%), L210W (29%), T215Y/I/F (65%), and K219Q/E/N (28%); and reverse transcriptase nonnucleoside resistance mutation K103N (52%). Our results suggest that, in general, the same amino acids are emerging in both subtypes B, F, and recombinant forms BF due to the selective pressure of antiretrovirals. Recombinant break points in samples are the same as identified in CRF28_BF and CRF29_BF and are recognized as important for the evolution of the local epidemic
机译:在巴西桑托斯,对B,F亚型和重组B / F中的HIV-1抗逆转录病毒药物耐药性突变进行了表征。我们研究了来自Santos参加巴西HIV / AIDS计划的个人的83个样本。这些患者已经接受了多种抗逆转录病毒治疗。 2006年收集了样本;从血浆中提取RNA,并将其用作扩增HIV-1 pol基因的靶标。在两条链上对PCR产物进行测序,通过邻居连接进行系统发育分析,并通过bootscan评估重组。样品的pol基因测序显示54株属于B亚型,4株属于F亚型,1株属于C亚型,24株是B / F重组体。 20个样本中的重组断裂点与CRF28_BF和CRF29_BF中鉴定的相同。 B,F和重组B / F亚型共有的耐药突变为蛋白酶抑制剂M46I / L(29%),I54V(24%),A71V(22%)和V82A / F(31%);逆转录酶核苷抗性突变M41L(52%),D67N(30%),K70R(26%),M184V(88%),L210W(29%),T215Y / I / F(65%)和K219Q / E / N(28%);逆转录酶非核苷抗性突变K103N(52%)。我们的结果表明,一般而言,由于抗逆转录病毒药物的选择性压力,相同的氨基酸同时出现在B,F亚型和重组形式BF中。样品中的重组断裂点与CRF28_BF和CRF29_BF中鉴定的断裂点相同,并被认为对于局部流行病的发展很重要

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