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利用细胞 HIV DNA 预测马拉维若治疗的病毒学反应:基于人群和深度测序的性能。

Use of cellular HIV DNA to predict virologic response to maraviroc: performance of population-based and deep sequencing.

机构信息

BC Centre for Excellence in HIV/AIDS, Vancouver, Canada.

出版信息

Clin Infect Dis. 2013 Jun;56(11):1659-66. doi: 10.1093/cid/cit105. Epub 2013 Feb 21.

Abstract

BACKGROUND

A tropism test is required before administration of the antiretroviral drug maraviroc. However, plasma RNA testing is not possible in patients with undetectable plasma viral loads. Here we assess genotypic testing of cellular human immunodeficiency virus (HIV) DNA from peripheral blood mononuclear cells (PBMCs) to predict virologic responses in treatment-experienced patients beginning maraviroc-containing regimens.

METHODS

PBMC samples from 181 maraviroc recipients at study entry in MOTIVATE or A4001029 (51% R5 by original Trofile). The V3 loop was amplified in triplicate from cellular HIV DNA, and matching plasma RNA (n = 156). Sequencing was performed using standard population-based methods and next-generation deep sequencing, with tropism assessment as previously defined.

RESULTS

Genotypic DNA-based tropism testing from the cellular compartment had 78%-81% sensitivity relative to RNA-based Trofile at the same time point. Cell-based genotypic tropism methods and plasma-based phenotypic and genotypic methods were predictive of virologic response. However, when classifications were discordant, the outcomes favored the plasma predictions over the DNA ones.

CONCLUSIONS

Genotypic determination of HIV tropism can be performed using cell-derived viral DNA, and is a predictor of virologic success on maraviroc in therapy-experienced patients. However, the PBMC compartment appears to be a suboptimal predictor compared to plasma.

摘要

背景

在给予抗逆转录病毒药物马拉维若之前需要进行趋性测试。然而,对于血浆病毒载量不可检测的患者,无法进行血浆 RNA 检测。在此,我们评估外周血单个核细胞(PBMC)中细胞人类免疫缺陷病毒(HIV)DNA 的基因型检测,以预测开始含有马拉维若的治疗方案的治疗经验丰富的患者的病毒学反应。

方法

在 MOTIVATE 或 A4001029 研究中,181 名马拉维若接受者在研究入组时的 PBMC 样本(51% 为原始 Trofile 的 R5)。从细胞 HIV DNA 中重复扩增 3 次 V3 环,并匹配血浆 RNA(n=156)。使用标准基于人群的方法和下一代深度测序进行测序,趋性评估如前所述。

结果

相对于同时点的基于 RNA 的 Trofile,细胞内基于基因型的趋性检测具有 78%-81%的敏感性。细胞内基于基因型的趋性方法和基于血浆的表型和基因型方法可预测病毒学反应。然而,当分类不一致时,结果更倾向于血浆预测而非 DNA 预测。

结论

可以使用源自细胞的病毒 DNA 进行 HIV 趋性的基因型测定,并且是治疗经验丰富的患者在马拉维若治疗中病毒学成功的预测指标。然而,与血浆相比,PBMC 似乎是一个不理想的预测指标。

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