Havlir D V, Bassett R, Levitan D, Gilbert P, Tebas P, Collier A C, Hirsch M S, Ignacio C, Condra J, Günthard H F, Richman D D, Wong J K
University of California, San Diego, 150 W Washington, Suite 100, San Diego, CA 92103, USA.
JAMA. 2001 Jul 11;286(2):171-9. doi: 10.1001/jama.286.2.171.
In HIV-infected patients having virologic suppression (plasma HIV RNA <50 copies/mL) with antiretroviral therapy, intermittent episodes of low-level viremia have been correlated with slower decay rates of latently infected cells and increased levels of viral evolution, but the clinical significance of these episodes is unknown.
To determine if HIV-infected patients with intermittent viremia have a higher risk of virologic failure (confirmed HIV RNA >200 copies/mL).
Retrospective analysis of subjects in well-characterized cohorts, the AIDS Clinical Trials Group (ACTG) 343 trial of induction-maintenance therapy (August 1997 to November 1998) and the Merck 035 trial (ongoing since March 1995).
Two hundred forty-one ACTG 343 patients, of whom 101 received triple-drug therapy throughout the study, and a small group of 13 patients from Merck 035 having virologic suppression after 6 months of indinavir-zidovudine-lamivudine.
Association of intermittent viremia (plasma HIV RNA >50 copies/mL with a subsequent measure <50 copies/mL) with virologic failure (2 consecutive plasma HIV RNA measures >200 copies/mL) in both study groups; evidence of drug resistance in 7 patients from the small (n = 13) study group with long-term follow-up.
Intermittent viremia occurred in 96 (40%) of the 241 ACTG 343 patients of whom 32 (13%) had 2 consecutive HIV RNA values >50 copies/mL during the median 84 weeks of observation (median duration of observation after first intermittent viremia episode was 46 weeks). Of the 101 individuals receiving triple-drug therapy throughout, 29% had intermittent viremia; the proportion of episodes occurring during the maintenance period was 64% for the entire cohort and 68% for the group not receiving triple-drug therapy throughout vs 55% for those who did (P =.25). Intermittent viremia did not predict virologic failure: 10 (10.4%) of 96 patients with and 20 (13.8%) of 145 patients without intermittent viremia had virologic failure (relative risk, 0.76; 95% confidence interval [CI], 0.29-1.72). In a Cox proportional hazards model, the risk for virologic failure was not significantly greater in the ACTG 343 patients with intermittent viremia (hazard ratio, 1.28; 95% CI, 0.59-2.79). Median viral load in 10 ACTG 343 patients assessed between 24 and 60 weeks of therapy using an ultrasensitive 2.5-copies/mL detection level assay was 23 copies/mL in those with intermittent viremia vs <2.5 copies/mL in those without (P =.15). Intermittent viremia occurred in 6 of 13 patients from the small study group assessed after 76 to 260 weeks of therapy (using the 2.5-copies/mL detection level assay) and was associated with a higher steady state of viral replication (P =.03), but not virologic failure over 4.5 years of observation. Viral DNA sequences from 7 patients did not show evolution of drug resistance.
Intermittent viremia occurred frequently and was associated with higher levels of replication (Merck 035), but was not associated with virologic failure in patients receiving initial combination therapy of indinavir-zidovudine-lamivudine (ACTG 343 and Merck 035). In this population, treatment changes may not be necessary to maintain long-term virologic suppression with low-level or intermittent viremia.
在接受抗逆转录病毒治疗且病毒学得到抑制(血浆HIV RNA<50拷贝/毫升)的HIV感染患者中,间歇性低水平病毒血症发作与潜伏感染细胞的较慢衰减率以及病毒进化水平升高相关,但这些发作的临床意义尚不清楚。
确定间歇性病毒血症的HIV感染患者发生病毒学失败(确诊HIV RNA>200拷贝/毫升)的风险是否更高。
对特征明确队列中的受试者进行回顾性分析,即艾滋病临床试验组(ACTG)343诱导-维持治疗试验(1997年8月至1998年11月)和默克035试验(自1995年3月起进行)。
241例ACTG 343患者,其中101例在整个研究过程中接受三联药物治疗,以及一小群来自默克035的13例患者,在接受茚地那韦-齐多夫定-拉米夫定治疗6个月后实现病毒学抑制。
两个研究组中间歇性病毒血症(血浆HIV RNA>50拷贝/毫升且随后测量值<50拷贝/毫升)与病毒学失败(连续两次血浆HIV RNA测量值>200拷贝/毫升)之间的关联;对13例长期随访的小研究组患者进行耐药性检测。
241例ACTG 343患者中有96例(40%)出现间歇性病毒血症,其中32例(13%)在中位84周的观察期内连续两次HIV RNA值>50拷贝/毫升(首次间歇性病毒血症发作后的中位观察持续时间为46周)。在整个研究过程中接受三联药物治疗的101例个体中,29%出现间歇性病毒血症;整个队列中维持期出现发作的比例为64%,未全程接受三联药物治疗的组为68%,而全程接受治疗的组为55%(P = 0.25)。间歇性病毒血症不能预测病毒学失败:96例有间歇性病毒血症的患者中有10例(10.4%)发生病毒学失败,145例无间歇性病毒血症的患者中有20例(13.8%)发生病毒学失败(相对风险,0.76;95%置信区间[CI],0.29 - 1.72)。在Cox比例风险模型中,ACTG 343中有间歇性病毒血症的患者发生病毒学失败的风险没有显著增加(风险比,1.28;95% CI,0.59 - 2.79)。在治疗24至60周期间使用超灵敏检测水平为2.5拷贝/毫升的检测方法评估的10例ACTG 343患者中,有间歇性病毒血症患者的中位病毒载量为23拷贝/毫升,无间歇性病毒血症患者的中位病毒载量<2.5拷贝/毫升(P = 0.15)。在治疗76至260周后评估的13例小研究组患者中有6例出现间歇性病毒血症(使用检测水平为2.5拷贝/毫升的检测方法),且与较高的病毒复制稳态相关(P = 0.03),但在4.5年的观察期内未出现病毒学失败。7例患者的病毒DNA序列未显示耐药性演变。
间歇性病毒血症频繁发生,且与较高的复制水平相关(默克035),但在接受茚地那韦-齐多夫定-拉米夫定初始联合治疗的患者中(ACTG 343和默克035)与病毒学失败无关。在该人群中,对于维持低水平或间歇性病毒血症的长期病毒学抑制,可能无需改变治疗方案。
