Orrell Catherine, Walensky Rochelle P, Losina Elena, Pitt Jennifer, Freedberg Kenneth A, Wood Robin
Desmond Tutu HIV Foundation, Institute of Infectious Disease and Molecular Medicine, Faculty of Health Sciences, University of Cape Town, Cape Town, South Africa.
Antivir Ther. 2009;14(4):523-31.
This study aimed to evaluate HIV type-1 (HIV-1) drug resistance pretreatment and in those failing first-line non-nucleoside reverse transcriptase inhibitor (NNRTI)-based antiretroviral therapy (ART) in South Africa.
This was an observational cohort. Genotypic resistance testing was performed on treatment-naive individuals and those failing first-line ART (confirmed HIV-1 RNA>1,000 copies/ml) from public sector clinics in Cape Town (2002-2007). Resistance profiles and mutations relative to timing of known virological failure were examined.
In total, 230 patients (120 treatment-naive and 110 with virological failure) were included: 98% had clade C virus. Among treatment-naive patients, prevalence of primary resistance was 2.5% (95% confidence interval 0.0-5.3). Three patients had one significant reverse transcriptase mutation: K65R, Y181C and G190A. Among treatment-experienced patients, 95 (86%) individuals had therapy-limiting NNRTI mutations, including K103N (55%), V106M (31%) and Y181C (9%). The M184V mutation was the most common mutation, found in 86 (78%) patients. In total, 10 (9%) patients had the K65R mutation. More individuals tended to develop thymidine analogue mutations when sampling occurred after 6 months of detected therapy failure (10/31 [32%] individuals) compared with those who had genotyping before 6 months (15/79 [19%] patients; P=0.246).
Prevalence of primary resistance in a sample of ART-naive clade C HIV-1-infected individuals in South Africa was low during the study period. Patients failing first-line ART most often developed resistance to NNRTIs and nucleoside reverse transcriptase inhibitors, the two drug classes used in first-line therapy. Viral load monitoring in this setting is crucial and individual genotypes in those failing first-line therapy should be considered.
本研究旨在评估南非HIV-1型(HIV-1)耐药性的治疗前情况以及一线基于非核苷类逆转录酶抑制剂(NNRTI)的抗逆转录病毒疗法(ART)失败患者的耐药情况。
这是一项观察性队列研究。对来自开普敦公共部门诊所的初治个体以及一线ART治疗失败(确诊HIV-1 RNA>1000拷贝/ml)的患者进行了基因型耐药性检测(2002 - 2007年)。研究了与已知病毒学失败时间相关的耐药谱和突变情况。
总共纳入了230例患者(120例初治患者和110例病毒学失败患者):98%感染的是C亚型病毒。在初治患者中,原发耐药率为2.5%(95%置信区间0.0 - 5.3)。3例患者有一个显著的逆转录酶突变:K65R、Y181C和G190A。在接受过治疗的患者中,95例(86%)个体有限制治疗的NNRTI突变,包括K103N(55%)、V106M(31%)和Y181C(9%)。M184V突变是最常见的突变,在86例(78%)患者中发现。总共有10例(9%)患者有K65R突变。与在治疗失败6个月前进行基因分型的患者(15/79 [19%])相比,在检测到治疗失败6个月后进行采样的患者中,更多个体倾向于发生胸苷类似物突变(10/31 [32%])(P = 0.246)。
在研究期间,南非初治的C亚型HIV-1感染个体样本中的原发耐药率较低。一线ART治疗失败的患者最常对NNRTIs和核苷类逆转录酶抑制剂产生耐药,这两类药物用于一线治疗。在这种情况下,病毒载量监测至关重要,对于一线治疗失败的患者应考虑其个体基因型。
