Most candidate HIV vaccines are directed at priming memory T cell responses and are being evaluated on their effects on post acquisition viremia and/or disease progression. These vaccines are being studied in areas of high HIV-1 prevalence. As such, we evaluated the frequency of CD4+ T cell decline and time course of opportunistic infections of patients presenting at a major metropolitan hospital in Lima, Peru, an area where such candidate vaccines are being tested. We examined 92 patients with untreated HIV-1 in calendar year 2002: 35% presented with CD4+ T cell counts of <200, 25% between 201 and 400, and 17% with >400 cells/mm3, 30 of 92 patients presented with overt AIDS, 6 were without an AIDS defining OI but CD4 counts <200. Over the course of follow-up, CD4 count decreased by a mean of 31 cells/mm3/year in women and 28 in men (p>0.5). Among persons presenting with CD4 counts >250 cells/mm3, the median time to first OI was 3.5 years. If clinical endpoints are required to evaluate the clinical effectiveness of T cell based vaccines, extended clinical follow-up of subjects enrolled in such trials will be required.

译文

大多数候选HIV疫苗都针对启动记忆T细胞反应,并正在评估其对获取后病毒血症和/或疾病进展的影响。这些疫苗正在HIV-1高流行的地区进行研究。因此,我们评估了在秘鲁利马的一家主要大都会医院就诊的患者的CD4 T细胞下降的频率和机会性感染的时间过程,该地区正在测试此类候选疫苗。我们在日历2002年中检查了92例未经治疗的HIV-1患者: 35% 例CD4 T细胞计数 <200,25% 201至400之间,17% 例> 400细胞/mm3,92例患者中有30例患有明显的AIDS,6例没有定义OI的AIDS,但CD4计数 <200。在随访过程中,女性CD4计数平均减少31个细胞/mm3/年,男性减少28个 (p>0.5)。在CD4计数> 250细胞/mm3的人中,首次OI的中位时间为3.5年。如果需要临床终点来评估基于T细胞的疫苗的临床有效性,则需要对参加此类试验的受试者进行长期的临床随访。

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