Poveda Eva, de Mendoza Carmen, Parkin Neil, Choe Sunny, García-Gasco Pilar, Corral Angélica, Soriano Vincent
Department of Infectious Diseases, Hospital Carlos III, Madrid, Spain.
AIDS. 2008 Mar 12;22(5):611-6. doi: 10.1097/QAD.0b013e3282f51eb9.
Tipranavir (TPV) and darunavir (DRV) are potent against protease inhibitor (PI)-resistant viruses. Efficacy of these compounds when confronting distinct HIV subtypes is not known.
All clinical specimens from HIV-positive patients sent to our institution for drug resistance testing between 1999 and 2006 were analysed. The prevalence of TPV and DRV resistance mutations was assessed based on the latest International AIDS Society-USA panel list. Phenotypic susceptibility to DRV and TPV was examined in a subset of these samples using the PhenoSense assay.
A total of 1364 genotypes were analysed, including 1178 from individuals infected with clade B (285 drug naive) and 186 with non-B subtypes (137 drug naive). The mean number (+/-SD) of DRV resistance-associated mutations was higher in clade B than non-B (0.4 +/- 0.9 versus 0.06 +/- 0.3; P < 0.001), and more frequent among PI-experienced than drug-naive patients (0.6 +/- 1.02 versus 0.02 +/- 0.21; P < 0.001). In contrast, the mean number of TPV resistance-associated mutations was higher in non-B than B subtypes (2.7 +/- 1 versus 1.2 +/- 1.6; P < 0.001), regardless of PI experience. Susceptibility to TPV and DRV was examined in 29 drug-naive patients infected with non-B subtypes (1A, 3C, 2CRF01_AE, 9CRF02_AG, 1CRF12_BF, 3CRF14_BG, 3F and 7G). All showed susceptibility to DRV and 93% to TPV. Interestingly, two subtype F specimens showed reduced TPV susceptibility, with fold-changes of 2.7 and 2.1, respectively.
Non-B subtypes show a greater number of TPV resistance-associated mutations than B viruses, regardless of PI exposure. While HIV clade has no influence on DRV susceptibility, some F subtypes may show reduced TPV susceptibility.
替拉那韦(TPV)和达芦那韦(DRV)对蛋白酶抑制剂(PI)耐药病毒有效。这些化合物在面对不同的HIV亚型时的疗效尚不清楚。
分析了1999年至2006年间送至我们机构进行耐药性检测的HIV阳性患者的所有临床标本。根据最新的美国国际艾滋病协会专家组列表评估TPV和DRV耐药突变的流行情况。使用PhenoSense检测法在这些样本的一个子集中检测对DRV和TPV的表型敏感性。
共分析了1364个基因型,包括1178个来自B亚型感染者(285个未接受过治疗)和186个来自非B亚型感染者(137个未接受过治疗)。B亚型中与DRV耐药相关的突变平均数(±标准差)高于非B亚型(0.4±0.9对0.06±0.3;P<0.001),且在接受过PI治疗的患者中比未接受过治疗的患者更常见(0.6±1.02对0.02±0.21;P<0.001)。相比之下,无论PI治疗经历如何,非B亚型中与TPV耐药相关的突变平均数高于B亚型(2.7±1对1.2±1.6;P<0.001)。对29例感染非B亚型(1A、3C、2CRF01_AE、9CRF02_AG、1CRF12_BF、3CRF14_BG、3F和7G)的未接受过治疗的患者检测了对TPV和DRV的敏感性。所有患者对DRV敏感,93%对TPV敏感。有趣的是,两个F亚型标本显示对TPV的敏感性降低,倍数变化分别为2.7和2.1。
无论PI暴露情况如何,非B亚型显示出比B病毒更多的与TPV耐药相关的突变。虽然HIV亚型对DRV敏感性没有影响,但一些F亚型可能显示出对TPV的敏感性降低。
