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Performance comparison of next-generation sequencing platforms for determining HIV-1 coreceptor use

机译:下一代测序平台确定HIV-1共受体使用情况的性能比较

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摘要

The coreceptor used by HIV-1 must be determined before a CCR5 antagonist, part of the arsenal of antiretroviral drugs, is prescribed because viruses that enter cells using the CXCR4 coreceptor are responsible for treatment failure. HIV-1 tropism is also correlated with disease progression and so must be determined for virological studies. Tropism can be determined by next-generation sequencing (NGS), but not all of these new technologies have been fully validated for use in clinical practice. The Illumina NGS technology is used in many laboratories but its ability to predict HIV-1 tropism has not been evaluated while the 454 GS-Junior (Roche) is used for routine diagnosis. The genotypic prediction of HIV-1 tropism is based on sequencing the V3 region and interpreting the results with an appropriate algorithm. We compared the performances of the MiSeq (Illumina) and 454 GS-Junior (Roche) systems with a reference phenotypic assay. We used clinical samples for the NGS tropism predictions and assessed their ability to quantify CXCR4-using variants. The data show that the Illumina platform can be used to detect minor CXCR4-using variants in clinical practice but technical optimization are needed to improve quantification.
机译:在开具CCR5拮抗剂(抗逆转录病毒药物的一部分)之前,必须确定HIV-1使用的共感受器,因为使用CXCR4共感受器进入细胞的病毒会导致治疗失败。 HIV-1的嗜性也与疾病进展相关,因此必须进行病毒学研究确定。可以通过下一代测序(NGS)来确定取向,但是并非所有这些新技术都已被完全验证可用于临床实践。 Illumina NGS技术已在许多实验室中使用,但是当使用454 GS-Junior(Roche)进行常规诊断时,其对HIV-1趋向性的预测能力尚未得到评估。 HIV-1向性的基因型预测基于对V3区域进行测序,并使用适当的算法解释结果。我们将MiSeq(Illumina)和454 GS-Junior(Roche)系统的性能与参考表型分析进行了比较。我们将临床样本用于NGS向性预测,并评估了其使用变体量化CXCR4的能力。数据表明,Illumina平台可在临床实践中用于检测较小的CXCR4使用变体,但需要进行技术优化以提高定量。

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