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在接受过治疗的个体中,基于基因型指导的抗逆转录病毒治疗成功的预测因素:一项队列研究。

Predictors of successful genotype-guided antiretroviral therapy in treatment-experienced individuals over calendar years: a cohort study.

机构信息

Catholic University of Sacred Heart, Department of Clinical Infectious Diseases, Rome, Italy.

出版信息

J Clin Virol. 2009 Nov;46(3):290-4. doi: 10.1016/j.jcv.2009.07.013. Epub 2009 Aug 21.

Abstract

BACKGROUND

The continuous development of new drugs for use in triple-drug combination antiretroviral therapy (cART) has dramatically decreased morbidity and mortality in HIV-1 infected individuals. However, increasing drug resistance could be associated with a poor outcome.

OBJECTIVES

To determine the efficacy of resistance genotype-guided antiretroviral regimens in combination antiretroviral therapy (cART)-failing patients over calendar years and its predictors.

STUDY DESIGN

Patients, with an available resistance genotype performed between 1999 and 2008, who failed a highly active antiretroviral therapy (HAART) regimen, changed therapy within 6 months from genotype and maintained the same salvage regimen, were selected from a clinical cohort database. Virologic efficacy was analyzed using time-to virologic suppression (VS, HIV-1 RNA<50 copies/ml).

RESULTS

In 270 sequences analyzed from 212 patients, after a median follow-up of 23 weeks, there were 160 patients with VS (59.3%). Mean regimens' genotypic sensitivity score (GSS) increased from 1.86 (SD+/-0.92) in 1999-2001, to 2.29 (SD+/-0.96) in 2005-2008 (p=0.001 for trend). VS was achieved in 39% of those patients genotyped in 1999-2001, and increased to 69% for patients with genotyping performed between 2005 and 2008 (p<0.001). More recent calendar year, younger age and less use of suboptimal therapy were predictors of more effective HAART regimens but only more recent calendar year maintained a trend toward significance in a multivariable model. More recent genotyping calendar year, younger age, lower number of HAART regimens experienced, lower HIV-1 RNA and higher GSS independently conveyed and increased the probability of VS.

CONCLUSIONS

Resistance-guided salvage antiretroviral therapy was more effective during more recent calendar years, independent from other measurable confounders, including the GSS of the employed regimen. Convenience and tolerability of newer agents should account for the observed effect.

摘要

背景

新型三药复方抗逆转录病毒疗法(cART)药物的不断发展,显著降低了 HIV-1 感染者的发病率和死亡率。然而,耐药性的增加可能与不良预后相关。

目的

确定耐药基因指导的抗逆转录病毒方案在日历年内对 cART 失败患者的疗效及其预测因素。

研究设计

从临床队列数据库中选择了 1999 年至 2008 年间进行了耐药基因型检测且对高效抗逆转录病毒治疗(HAART)方案失败的患者,他们在 6 个月内根据基因型改变了治疗方案,并维持相同的挽救治疗方案。使用病毒学抑制时间(VS,HIV-1 RNA<50 拷贝/ml)分析病毒学疗效。

结果

在 212 名患者的 270 个序列分析中,中位随访 23 周后,有 160 名患者达到 VS(59.3%)。平均方案的基因型敏感评分(GSS)从 1999-2001 年的 1.86(SD+/-0.92)增加到 2005-2008 年的 2.29(SD+/-0.96)(趋势 p=0.001)。1999-2001 年进行基因分型的患者中,有 39%达到 VS,而 2005-2008 年进行基因分型的患者中,有 69%达到 VS(p<0.001)。更接近当前的日历年度、更年轻的年龄和较少使用非最佳治疗方案是更有效的 HAART 方案的预测因素,但只有更接近当前的日历年度在多变量模型中仍保持显著趋势。更接近当前的基因分型日历年度、更年轻的年龄、更少的 HAART 方案、更低的 HIV-1 RNA 和更高的 GSS 独立并增加了 VS 的可能性。

结论

耐药基因指导的挽救性抗逆转录病毒治疗在更近的日历年内更为有效,独立于其他可测量的混杂因素,包括所采用方案的 GSS。新型药物的便利性和耐受性可能解释了观察到的效果。

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