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首页> 外文期刊>Data in Brief >Frequent detection of CXCR4-using viruses among Brazilian blood donors with HIV-1 long-standing infection and unknown clinical stage: Analysis of massive parallel sequencing data
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Frequent detection of CXCR4-using viruses among Brazilian blood donors with HIV-1 long-standing infection and unknown clinical stage: Analysis of massive parallel sequencing data

机译:在具有HIV-1长期感染和未知临床阶段的巴西献血者中频繁检测使用CXCR4的病毒:大规模并行测序数据分析

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The determination of viral tropism is critically important and highly recommended to guide therapy with the CCR5 antagonist, which does not inhibit the effect of X4-tropic viruses. Here, we report the prevalence of HIV-1×4 HIV strains in 84 proviral DNA massively parallel sequencing “MPS” data from well-defined non-recently infected first-time Brazilian blood donors. The MPS data covering the entire V3 region of the env gene was extracted from our recently generated HIV-1 genomes sequenced by a paired-end protocol (Illumina). Of the 84 MPS data samples, 63 (75%) were derived from donors with long-standing infection and 21 (25%) were lacking stage information. HIV‐1 tropism was inferred using Geno2pheno (g2p) [454] algorithm (FPR=1%, 2.5%, and 3.75%). Among the 84 data samples for which tropism was defined by g2p 2.5% , 13 (15.5%) participants had detectable CXCR4-using viruses in their MPS reads. Mixed infections with R5 and X4 were observed in 11.9% of the study subjects and minority X4 viruses were detected in 7 (8.3%) of participants. Nine of the 63 (14.3%) subjects with LS infection were predicted by g2p 2.5% to harbor proviral CXCR4-using viruses. Our findings of a high proportion of blood donors (15.5%) harboring CXCR4-using viruses in PBMCs may indicate that this phenomenon is common. These findings may have implications for clinical and therapeutic aspects and may benefit individuals who plan to receive CCR5 antagonists.
机译:病毒向性的确定至关重要,强烈建议使用CCR5拮抗剂指导治疗,该抑制剂不抑制X4嗜性病毒的作用。在这里,我们报告了来自定义明确的近期未感染的巴西首次献血者的84个前病毒DNA大规模并行测序“ MPS”数据中的HIV-1×4 HIV菌株的患病率。覆盖env基因整个V3区域的MPS数据是从我们最近生成的HIV-1基因组中提取的,该基因组已通过配对末端协议(Illumina)进行了测序。在84个MPS数据样本中,63个(75%)来自长期感染的供体,而21个(25%)缺乏阶段信息。使用Geno2pheno(g2p)[454]算法(FPR = 1%,2.5%和3.75%)推断出HIV-1的向性。在84个数据样本中,向心性定义为g2p 2.5%,其中13个(15.5%)参与者在其MPS读取中具有可检测到的使用CXCR4的病毒。在11.9%的研究对象中观察到R5和X4的混合感染,在7名(8.3%)的参与者中检测到少数X4病毒。通过g2p 2.5%预测63名LS感染受试者中的9名(14.3%)会携带使用前病毒CXCR4的病毒。我们的研究发现,PBMC中使用CXCR4的供血者比例很高(占15.5%),这可能表明这种现象很普遍。这些发现可能会对临床和治疗方面产生影响,并且可能使计划接受CCR5拮抗剂的患者受益。

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