Gupta Amita, Saple Dattaray G, Nadkarni Girish, Shah Bijal, Vaidya Satish, Hingankar Nitin, Chaturbhuj Devidas, Deshmukh Praveen, Walshe Louise, Hudelson Sarah E, James Maria, Paranjape Ramesh S, Eshleman Susan H, Tripathy Srikanth
Johns Hopkins University School of Medicine, Baltimore, Maryland 21287, USA.
AIDS Res Hum Retroviruses. 2010 Jan;26(1):25-31. doi: 10.1089/aid.2009.0102.
HIV-infected patients receiving antiretroviral (ARV) therapy (ART) in India are not all adequately virally suppressed. We analyzed ARV drug resistance in adults receiving ART in three private clinics in Mumbai, India. HIV viral load was measured in 200 patients with the Roche AMPLICOR HIV-1 Monitor Test, v1.5. HIV genotyping was performed with the ViroSeq HIV-1 Genotyping System for 61 participants who had HIV-1 RNA >1000 copies/ml. Genotyping results were obtained for 51 samples. The participants with resistance results were on ART for a median of 24 months and were on their current regimen for a median of 12 months (median CD4 cell count: 217 cells/mm(3); median HIV viral load: 28,200 copies/ml). ARV regimens included nonnucleoside reverse transcriptase inhibitor (NNRTI)-based regimens (n = 27), dual nucleoside reverse transcriptase inhibitors (NRTIs, n = 19), protease inhibitor (PI)-based regimens (n = 3), and other regimens (n = 2). Twenty-six participants (51.0%) were on their first ARV regimen and 24 (47%) reported >95% adherence. Forty-nine participants (96.1%) had resistance to at least one ARV drug; 47 (92.2%) had NRTI resistance, 32 (62.7%) had NNRTI resistance, and four (7.8%) had PI resistance. Thirty (58.8%) had two-class resistance and three (5.9%) had three-class resistance. Four (8%) had three or more resistance mutations associated with etravirine resistance and two (4%) had two mutations associated with reduced darunavir susceptibility. Almost all patients with HIV-1 RNA >1000 copies/ml had NRTI resistance and nearly two-thirds had NNRTI resistance; PI resistance was uncommon. Nearly 60% and 6% had two- and three-class resistance, respectively. This emphasizes the need for greater viral load and resistance monitoring, use of optimal ART combinations, and increased availability of second- and third-line agents for patients with ARV resistance.
在印度,接受抗逆转录病毒(ARV)治疗(ART)的HIV感染患者并非都能实现充分的病毒抑制。我们分析了印度孟买三家私立诊所中接受ART治疗的成年患者的ARV耐药情况。使用罗氏AMPLICOR HIV-1监测检测v1.5对200名患者进行了HIV病毒载量检测。对61名HIV-1 RNA>1000拷贝/毫升的参与者使用ViroSeq HIV-1基因分型系统进行了HIV基因分型。获得了51个样本的基因分型结果。有耐药结果的参与者接受ART治疗的中位数为24个月,目前治疗方案的使用时间中位数为12个月(CD4细胞计数中位数:217个细胞/立方毫米;HIV病毒载量中位数:28200拷贝/毫升)。ARV治疗方案包括基于非核苷类逆转录酶抑制剂(NNRTI)的方案(n = 27)、双核苷类逆转录酶抑制剂(NRTIs,n = 19)、基于蛋白酶抑制剂(PI)的方案(n = 3)以及其他方案(n = 2)。26名参与者(51.0%)使用的是首个ARV治疗方案,24名(47%)报告依从性>95%。49名参与者(96.1%)对至少一种ARV药物耐药;47名(92.2%)有NRTI耐药,32名(62.7%)有NNRTI耐药,4名(7.8%)有PI耐药。30名(58.8%)有两类耐药,3名(5.9%)有三类耐药。4名(8%)有三个或更多与依曲韦林耐药相关的耐药突变,2名(4%)有两个与达芦那韦敏感性降低相关的突变。几乎所有HIV-1 RNA>1000拷贝/毫升的患者都有NRTI耐药,近三分之二有NNRTI耐药;PI耐药不常见。分别有近60%和6%的患者有两类和三类耐药。这强调了对病毒载量和耐药情况进行更密切监测的必要性,使用最佳的ART联合方案,以及为有ARV耐药的患者增加二线和三线药物的可及性。
