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首页> 外文期刊>Journal of Clinical Microbiology >A Diagnostic HIV-1 Tropism System Based on Sequence Relatedness
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A Diagnostic HIV-1 Tropism System Based on Sequence Relatedness

机译:基于序列相关性的HIV-1诊断系统

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Key clinical studies for HIV coreceptor antagonists have used the phenotyping-based Trofile test. Meanwhile various simpler-to-do genotypic tests have become available that are compatible with standard laboratory equipment and Web-based interpretation tools. However, these systems typically analyze only the most prominent virus sequence in a specimen. We present a new diagnostic HIV tropism test not needing DNA sequencing. The system, XTrack, uses physical properties of DNA duplexes after hybridization of single-stranded HIV-1 env V3 loop probes to the clinical specimen. Resulting “heteroduplexes” possess unique properties driven by sequence relatedness to the reference and resulting in a discrete electrophoretic mobility. A detailed optimization process identified diagnostic probe candidates relating best to a large number of HIV-1 sequences with known tropism. From over 500 V3 sequences representing all main HIV-1 subtypes (Los Alamos database), we obtained a small set of probes to determine the tropism in clinical samples. We found a high concordance with the commercial TrofileES test (84.9%) and the Web-based tool Geno2Pheno (83.0%). Moreover, the new system reveals mixed virus populations, and it was successful on specimens with low virus loads or on provirus from leukocytes. A replicative phenotyping system was used for validation. Our data show that the XTrack test is favorably suitable for routine diagnostics. It detects and dissects mixed virus populations and viral minorities; samples with viral loads (VL) of <200 copies/ml are successfully analyzed. We further expect that the principles of the platform can be adapted also to other sequence-divergent pathogens, such as hepatitis B and C viruses.
机译:HIV共受体拮抗剂的关键临床研究已使用基于表型的Trofile测试。同时,已经有了与标准实验室设备和基于Web的解释工具兼容的各种更简单的基因型测试。但是,这些系统通常仅分析样本中最突出的病毒序列。我们提出了不需要DNA测序的新的诊断性爱滋病性测试。 XTrack系统将单链HIV-1 env V3环探针与临床样本杂交后,利用DNA双链体的物理特性。所得的“异源双链体”具有独特的特性,该特性由与参考序列的相关性驱动,并导致离散的电泳迁移率。详细的优化过程确定了与具有已知向性的大量HIV-1序列最相关的诊断探针候选物。从代表所有主要HIV-1亚型的500多个V3序列(Los Alamos数据库)中,我们获得了一小套探针以确定临床样本中的向性。我们发现与商业TrofileES测试(84.9%)和基于Web的工具Geno2Pheno(83.0%)高度一致。此外,新系统揭示了混合的病毒种群,并且在病毒载量低的标本或白细胞的原病毒上成功了。复制表型系统用于验证。我们的数据表明,XTrack测试非常适合常规诊断。它检测并解剖混合的病毒种群和病毒少数群体;成功分析了病毒载量(VL)<200拷贝/ ml的样品。我们进一步期望该平台的原理也可以适应其他具有序列差异的病原体,例如乙型和丙型肝炎病毒。

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