Hecht Frederick M, Wang Lei, Collier Ann, Little Susan, Markowitz Martin, Margolick Joseph, Kilby J Michael, Daar Eric, Conway Brian, Holte Sarah
University of California San Francisco, San Francisco, CA 94110, USA.
J Infect Dis. 2006 Sep 15;194(6):725-33. doi: 10.1086/506616. Epub 2006 Aug 15.
Uncontrolled studies have suggested a benefit, after treatment discontinuation, of initiating highly active antiretroviral therapy (HAART) during primary human immunodeficiency virus (HIV) infection. We assessed whether initiation of HAART within 2 weeks of (acute treatment) or between 2 weeks and 6 months after (early treatment) HIV seroconversion was associated with improvements in the viral load and the CD4+ T cell count after discontinuation of treatment in an observational cohort.
Subjects from the multicenter Acute Infection and Early Disease Research Program cohort were enrolled in the present study within 6 months of HIV seroconversion and self-selected whether to initiate HAART. Subjects who received acute (n=13) or early (n=45) treatment received HAART for at least 12 weeks and then subsequently stopped treatment, whereas untreated subjects (n=337) declined treatment. HIV RNA levels and CD4+ T cell counts at 24, 48, and 72 weeks after treatment cessation in the 2 treatment groups were compared with those noted in the untreated group during the same periods of observation after enrollment.
The acute treatment group had lower mean HIV RNA levels at 24 weeks without therapy (-0.48 log(10) copies/mL [95% confidence interval {CI}, -0.82 to -0.13 log(10) copies/mL]) and higher mean CD4+ T cell counts (112 cells/ mu L [95% CI, 20-205 cells/ microL]), compared with the untreated group at 24 weeks. The differences in the laboratory values for the acute treatment group versus the untreated group at 72 weeks without therapy were as follows: for the HIV RNA level, -0.35 log(10) copies/mL (95% CI, -0.91 to 0.21 log(10) copies/mL) and, for the CD4 T+ cell count, 112 cells/ microL (95% CI, -15 to 213 cells/ microL). The early treatment group had lower HIV RNA levels at 24 weeks than did the untreated group, but differences were no longer apparent by week 48; CD4+ T cell counts were higher in the early treatment group at week 24 (116 cells/ microL [95% CI, 75-157 cells/ microL]) and week 72 (70 cells/ microL [95% CI, 2-138 cells/ microL]).
Initiation of HAART within 2 weeks of antibody seroconversion was associated with viral load and CD4+ T cell count benefits for 24 weeks after termination of HAART, with there being trends toward a longer-term benefit. Later initiation of HAART was associated with a persistent but decreasing CD4+ T cell count benefit and a loss of the viral load benefit by week 72 after discontinuation of treatment.
非对照研究表明,在原发性人类免疫缺陷病毒(HIV)感染期间停止治疗后,启动高效抗逆转录病毒疗法(HAART)具有益处。我们评估了在HIV血清转化后2周内(急性治疗)或2周后至6个月内(早期治疗)启动HAART是否与观察性队列中治疗中断后病毒载量和CD4 + T细胞计数的改善相关。
多中心急性感染和早期疾病研究项目队列中的受试者在HIV血清转化后6个月内纳入本研究,并自行选择是否启动HAART。接受急性治疗(n = 13)或早期治疗(n = 45)的受试者接受HAART至少12周,然后停止治疗,而未治疗的受试者(n = 337)拒绝治疗。将两个治疗组在停止治疗后24、48和72周时的HIV RNA水平和CD4 + T细胞计数与未治疗组在入组后相同观察期内记录的水平进行比较。
与未治疗组在24周时相比,急性治疗组在停止治疗24周时的平均HIV RNA水平较低(-0.48 log(10)拷贝/毫升[95%置信区间{CI},-0.82至-0.13 log(10)拷贝/毫升]),平均CD4 + T细胞计数较高(112个细胞/微升[95% CI,20 - 205个细胞/微升])。急性治疗组与未治疗组在停止治疗72周时实验室值的差异如下:对于HIV RNA水平,为-0.35 log(10)拷贝/毫升(95% CI,-0.91至0.21 log(10)拷贝/毫升),对于CD4 T +细胞计数,为112个细胞/微升(95% CI,-15至213个细胞/微升)。早期治疗组在24周时的HIV RNA水平低于未治疗组,但到48周时差异不再明显;早期治疗组在24周(116个细胞/微升[95% CI,75 - 157个细胞/微升])和72周(70个细胞/微升[95% CI,2 - 138个细胞/微升])时的CD4 + T细胞计数较高。
在抗体血清转化后2周内启动HAART与HAART终止后24周的病毒载量和CD4 + T细胞计数益处相关,并有长期益处的趋势。HAART启动较晚与CD4 + T细胞计数持续但逐渐减少的益处相关,且在停止治疗72周时病毒载量益处丧失。
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