接受单剂量奈韦拉平治疗的女性中持续存在的少数K103N突变以及对基于非核苷类逆转录酶抑制剂疗法的病毒学反应。
Persistent minority K103N mutations among women exposed to single-dose nevirapine and virologic response to nonnucleoside reverse-transcriptase inhibitor-based therapy.
作者信息
Coovadia Ashraf, Hunt Gillian, Abrams Elaine J, Sherman Gayle, Meyers Tammy, Barry Gill, Malan Eloise, Marais Belinda, Stehlau Renate, Ledwaba Johanna, Hammer Scott M, Morris Lynn, Kuhn Louise
机构信息
Empilweni Clinic, Coronation Women and Children Hospital, Johannesburg, South Africa.
出版信息
Clin Infect Dis. 2009 Feb 15;48(4):462-72. doi: 10.1086/596486.
OBJECTIVE
We investigated whether there are long-lasting effects of exposure to single-dose nevirapine (sdNVP) treatment on virologic response to nonnucleoside reverse-transcriptase inhibitor (NNRTI)-based therapy among human immunodeficiency virus (HIV)-infected women.
METHODS
An observational epidemiologic study was conducted in Johannesburg, South Africa. Initial and sustained virologic response to NNRTI-based therapy was compared between 94 HIV-infected women who had received sdNVP 18-36 months earlier and 60 unexposed, HIV-infected women who had been pregnant 12-36 months earlier. Viral load was measured every 4 weeks up to week 24 and then every 12 weeks up to week 78. Time to viral suppression (viral load, <50 copies/mL) and confirmed rebound in the viral load (viral load, >400 copies/mL) were compared. Drug resistance was assessed using K103N allele-specific real-time polymerase chain reaction assay and population sequencing.
RESULTS
Almost all women (97.5% of sdNVP-exposed women and 91.3% of sdNVP-unexposed women; P = .21) achieved viral suppression by week 24, and similar percentages of sdNVP-exposed and -unexposed women (19.4% and 15.1%, respectively) experienced viral rebound within 78 weeks after treatment (P = .57). K103N was detected with the K103N allele-specific real-time polymerase chain reaction assay among sdNVP-exposed and -unexposed women before treatment; detection was strongly predictive of inadequate viral response: 60.9% of women for whom K103N was detected in either viral RNA or DNA did not experience viral suppression or experienced viral rebound, compared with 15.1% of women for whom K103N was not detected (P < .001). After treatment, the M184V mutation occurred less frequently among sdNVP-exposed women than among sdNVP-unexposed women, but the frequency of NNRTI-associated mutations was similar between these groups of women with inadequate virologic response.
CONCLUSIONS
Exposure to sdNVP in the prior 18-36 months was not associated with a reduced likelihood of achieving and sustaining viral suppression while receiving NNRTI-based therapy. However, women with minority K103N mutations before treatment had a reduced durability of virologic suppression.
目的
我们调查了单剂量奈韦拉平(sdNVP)治疗对感染人类免疫缺陷病毒(HIV)的女性基于非核苷类逆转录酶抑制剂(NNRTI)治疗的病毒学反应是否有长期影响。
方法
在南非约翰内斯堡进行了一项观察性流行病学研究。比较了94名在18 - 36个月前接受过sdNVP治疗的HIV感染女性和60名未接受过治疗、在12 - 36个月前怀孕的HIV感染女性对基于NNRTI治疗的初始和持续病毒学反应。在第24周前每4周测量一次病毒载量,然后在第78周前每12周测量一次。比较了病毒抑制时间(病毒载量<50拷贝/毫升)和病毒载量确认反弹(病毒载量>400拷贝/毫升)情况。使用K103N等位基因特异性实时聚合酶链反应测定法和群体测序评估耐药性。
结果
几乎所有女性(接受sdNVP治疗的女性中有97.5%,未接受sdNVP治疗的女性中有91.3%;P = 0.21)在第24周时实现了病毒抑制,接受sdNVP治疗组和未接受治疗组中出现病毒反弹的女性比例相似(分别为19.4%和15.1%),在治疗后78周内出现病毒反弹(P = 0.57)。在治疗前,通过K103N等位基因特异性实时聚合酶链反应测定法在接受sdNVP治疗组和未接受治疗组的女性中均检测到K103N;该检测结果强烈预示病毒反应不足:在病毒RNA或DNA中检测到K103N的女性中有60.9%未实现病毒抑制或出现病毒反弹,而未检测到K103N的女性中这一比例为15.1%(P < 0.001)。治疗后,接受sdNVP治疗的女性中M184V突变的发生率低于未接受sdNVP治疗的女性,但在这些病毒学反应不足的女性组中,NNRTI相关突变的频率相似。
结论
在过去18 - 36个月内接触过sdNVP与在接受基于NNRTI治疗时实现和维持病毒抑制的可能性降低无关。然而,治疗前携带少数K103N突变的女性病毒学抑制的持久性降低。
Zotero 插件