首页> 外文期刊>JAMA: the Journal of the American Medical Association >Intermittent HIV-1 viremia (Blips) and drug resistance in patients receiving HAART.
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Intermittent HIV-1 viremia (Blips) and drug resistance in patients receiving HAART.

机译:接受HAART的患者间断性HIV-1病毒血症(Blips)和耐药性。

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CONTEXT: Many patients infected with human immunodeficiency virus type 1 (HIV-1) and receiving highly active antiretroviral therapy experience intermittent episodes of detectable viremia ("blips"), which may raise concerns about drug resistance, lead to costly repeat measurements of viral RNA, and sometimes trigger alterations in therapy. OBJECTIVE: To test the hypothesis that blips represent random biological and statistical variation around mean steady-state HIV-1 RNA levels slightly below 50 copies/mL rather than biologically significant elevations in viremia. DESIGN, SETTING, AND PATIENTS: Between June 19, 2003, and February 9, 2004, patients receiving therapy underwent intensive sampling (every 2-3 days) over 3 to 4 months to define the frequency, magnitude, and duration of blips and their association with drug levels and other clinical variables. Blips were defined as HIV-1 RNA measurements greater than or equal to 50 copies/mL preceded and followed by measurements less than 50 copies/mL without a change in treatment. To determine whether blips result from or lead to drug resistance, an ultrasensitive genotyping assay was used to detect drug resistance mutations before, during, and after blips. Patients were 10 HIV-1-infected asymptomatic adults recruited by clinicians and followed up in the Moore Clinic at the Johns Hopkins Hospital. Patients had suppression of viremia to below 50 copies/mL while receiving a stable antiretroviral regimen for 6 months or longer. MAIN OUTCOME MEASURES: At each time point, plasma HIV-1 RNA levels were measured in 2 independent laboratories and drug resistance mutations were analyzed by clonal sequencing. RESULTS: With the intensive sampling, blips were detected in 9 of 10 patients. Statistical analysis was consistent with random assay variation around a mean viral load below 50 copies/mL. Blips were not concordant on independent testing and had a short duration (median, <3 days) and low magnitude (median, 79 copies/mL). Blip frequency was not associated with demographic, clinical, or treatment variables. Blips did not occur in relation to illness, vaccination, or directly measured antiretroviral drug concentrations. Blips were marginally associated (P = .08) with reported episodes of nonadherence. Most importantly, in approximately 1000 independent clones sequenced for both protease and reverse transcriptase, no new resistance mutations were seen before, during, or shortly after blips. CONCLUSION: Most blips in this population appear to represent random biological and statistical variation around mean HIV-1 levels below 50 copies/mL rather than clinically significant elevations in viremia.
机译:背景:许多感染了1型人类免疫缺陷病毒(HIV-1)并接受高活性抗逆转录病毒治疗的患者经历了间歇性可检测病毒血症发作(“斑点”),这可能引起人们对药物耐药性的担忧,导致重复进行病毒RNA的昂贵检测,有时会触发疗法的改变。目的:检验假说代表平均稳态HIV-1 RNA水平略低于50拷贝/ mL,而不是生物学上病毒血症的明显升高,斑点代表随机的生物学和统计学差异。设计,地点和患者:在2003年6月19日至2004年2月9日之间,接受治疗的患者会在3到4个月内接受密集采样(每2-3天),以确定红斑的频率,大小和持续时间及其与药物水平和其他临床变量相关。出现斑点的定义是:先进行HIV-1 RNA的测定,其值大于或等于50拷贝/ mL,然后进行测定,其值小于50拷贝/ mL,且治疗方法不变。为了确定斑点是否是由耐药性引起或导致的,使用超灵敏基因分型测定法检测斑点之前,期间和之后的耐药性突变。患者是由临床医生招募的10名感染HIV-1的无症状成人,并在约翰霍普金斯医院的摩尔诊所进行了随访。患者接受稳定的抗逆转录病毒治疗6个月或更长时间后,病毒血症被抑制至50拷贝/ mL以下。主要观察指标:在每个时间点,在2个独立实验室中测定血浆HIV-1 RNA水平,并通过克隆测序分析耐药性突变。结果:经过大量采样,在10例患者中有9例检测到斑点。统计分析与低于50拷贝/ mL的平均病毒载量周围的随机测定变化一致。斑点在独立测试中不一致,持续时间短(中位数,<3天),幅度小(中位数,79拷贝/毫升)。发生频率与人口统计学,临床或治疗变量无关。没有出现与疾病,疫苗接种或直接测量的抗逆转录病毒药物浓度有关的斑点。斑点与报道的不依从事件之间有轻微关联(P = 0.08)。最重要的是,在大约1000个针对蛋白酶和逆转录酶进行测序的独立克隆中,在斑点之前,期间或之后没有发现新的抗性突变。结论:该人群中的大多数斑点似乎代表低于50拷贝/ mL的平均HIV-1水平的随机生物学和统计学差异,而不是病毒血症的临床显着升高。

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