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Position-specific automated processing of V3 env ultra-deep pyrosequencing data for predicting HIV-1 tropism

机译:V3 env超深焦测序数据的位置特定的自动化处理,可预测HIV-1向性

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摘要

HIV-1 coreceptor usage must be accurately determined before starting CCR5 antagonist-based treatment as the presence of undetected minor CXCR4-using variants can cause subsequent virological failure. Ultra-deep pyrosequencing of HIV-1 V3 env allows to detect low levels of CXCR4-using variants that current genotypic approaches miss. However, the computation of the mass of sequence data and the need to identify true minor variants while excluding artifactual sequences generated during amplification and ultra-deep pyrosequencing is rate-limiting. Arbitrary fixed cut-offs below which minor variants are discarded are currently used but the errors generated during ultra-deep pyrosequencing are sequence-dependant rather than random. We have developed an automated processing of HIV-1 V3 env ultra-deep pyrosequencing data that uses biological filters to discard artifactual or non-functional V3 sequences followed by statistical filters to determine position-specific sensitivity thresholds, rather than arbitrary fixed cut-offs. It allows to retain authentic sequences with point mutations at V3 positions of interest and discard artifactual ones with accurate sensitivity thresholds.
机译:在开始基于CCR5拮抗剂的治疗之前,必须准确确定HIV-1共受体的使用情况,因为存在未检测到的使用CXCR4的次要变体会导致随后的病毒学衰竭。 HIV-1 V3 env的超深度焦磷酸测序可检测出低水平的CXCR4,并使用当前基因型方法遗漏的变体。然而,序列数据质量的计算以及鉴定真正的次要变体,同时排除扩增和超深焦磷酸测序过程中产生的人为序列的需求是限速的。当前使用的是任意固定的临界值,在该临界值以下将删除较小的变体,但是在超深焦磷酸测序过程中产生的错误取决于序列,而不是随机的。我们开发了一种自动处理HIV-1 V3 env超深焦磷酸测序数据的方法,该方法使用生物过滤器丢弃虚假的或无功能的V3序列,然后使用统计过滤器确定特定于位置的敏感度阈值,而不是任意固定的临界值。它允许保留在感兴趣的V3位置具有点突变的真实序列,并丢弃具有准确灵敏度阈值的非自然序列。

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