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Impact of different HIV resistance interpretation by distinct systems on clinical utility of resistance testing.

机译:不同的系统对不同的HIV抗药性解释对抗药性测试的临床效用的影响。

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SUMMARY: PURPOSE OF REVIEW Genotypic assays are widely used tools for determining HIV-1 drug resistance and for guiding treatment. Several systems have been developed to interpret the complex influence of amino acid substitutions in HIV reverse transcriptase or protease on the phenotypic susceptibility or clinical response to the 18 available antiretroviral agents. In this review we analyse both studies comparing interpretations by different systems and studies showing correlation of interpretations with clinical outcome, in order to identify discordance and how this may affect prediction of subsequent therapy outcomes.RECENT FINDINGS During the last year, several studies analysing interpretation systems, individually or comparatively, have shown substantial variability of the predicted drug activities and therapeutic outcomes. Discrepant interpretation was detected mostly for nucleoside reverse transcriptase inhibitors and rarely for non-nucleoside reverse transcriptase inhibitors. Better correlation with treatment outcome was found with most recently updated systems, while a weaker prediction was found with systems interpreting activity of nucleoside reverse transcriptase inhibitors solely on the basis of phenotypic susceptibility. Virological, patient-related and treatment-related factors can all affect the results of systems' clinical validations. Refinement of resistance interpretation is possible by introducing rules derived from genotype-outcomes correlation or, at least for protease inhibitors, genotype-phenotype correlation.SUMMARY Papers showing clinical validation of the available interpretation systems are presented with a critical view to help the readers' evaluation of their possible use. There is a need for developing a consensus towards common interpretations. Large clinical and virological databases with quality data will be useful for future improvements.
机译:概述:审查的目的基因型测定法是确定HIV-1耐药性和指导治疗的广泛使用的工具。已经开发了几种系统来解释HIV逆转录酶或蛋白酶中氨基酸取代对表型敏感性或对18种可用抗逆转录病毒药物的临床反应的复杂影响。在这篇综述中,我们分析了比较不同系统的解释的研究和显示解释与临床结果之间相关性的研究,以便确定不一致之处以及这可能如何影响后续治疗结果的预测。最近发现去年,有几项分析解释系统的研究单独地或比较地,已经显示出预测的药物活性和治疗结果的显着差异。差异解释主要是针对核苷逆转录酶抑制剂,很少针对非核苷逆转录酶抑制剂。在最新更新的系统中发现与治疗结果的相关性更好,而仅根据表型敏感性来解释核苷逆转录酶抑制剂活性的系统则发现较弱的预测。病毒学,与患者有关和与治疗有关的因素都可能影响系统临床验证的结果。通过引入衍生自基因型-结果相关性的规则或至少对于蛋白酶抑制剂而言是基因型-表型相关性的规则,可以改进耐药性解释。总结本文对可用解释系统的临床验证进行了综述,并提出了批判性的观点,以帮助读者评估可能的用途。有必要就共同的解释达成共识。具有质量数据的大型临床和病毒学数据库将对将来的改进很有用。

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