首页> 外文期刊>The Lancet >Long-lasting recovery in CD4 T-cell function and viral-load reduction after highly active antiretroviral therapy in advanced HIV-1 disease (see comments)
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Long-lasting recovery in CD4 T-cell function and viral-load reduction after highly active antiretroviral therapy in advanced HIV-1 disease (see comments)

机译:高活性抗逆转录病毒疗法治疗晚期HIV-1疾病后,CD4 T细胞功能得以长期恢复并减少病毒载量(请参阅评论)

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BACKGROUND: Highly active antiretroviral therapy (HAART) decreases viral load and increases CD4 T-cell counts in patients with advanced HIV-1 infection. Whether HAART can improve CD4 T-cell function, and the biological characteristics affecting immune reconstitution, remain unclear. We undertook an open prospective pilot study to address these issues. Both treatment-naive and previously treated patients were included. METHODS: 20 patients (seven naive, 13 previously treated) were treated with one protease inhibitor and two reverse-transcriptase inhibitors and followed up for 12 months. We measured CD4-cell proliferation in response to cytomegalovirus and tuberculin antigens and counted subsets of CD4 cells at baseline and months 1, 3, 6, 9, and 12. Patients who had no antigen-specific reactivity at baseline but developed it while receiving HAART were classified as immunological responders. FINDINGS: Four patients had antigen-specific reactivity at baseline compared with 14 at month 12 (p <0.001). Between month 3 and month 12 viral load fell by a median of 1.5 log copies/mL from baseline (4.6 log copies/mL) and CD4-cell count increased by a median of 63/microL (from 93/microL). Ten patients (six of seven naive, four of 13 previously treated) were immunological responders. They differed significantly from the ten non-responders in that their viral-load reduction was sustained for 12 months, the increase in CD4 count was greater, and they showed an early increase in memory CD4 T cells with an increase of naive T cells. INTERPRETATION: HAART can induce sustained recovery of CD4 T-cell reactivity against opportunistic pathogens in severely immunosuppressed patients. This recovery depends not on baseline values but on the amplitude and duration of viral-load reduction and the increase of memory CD4 T cells.
机译:背景:高活性抗逆转录病毒疗法(HAART)可以降低晚期HIV-1感染患者的病毒载量并增加CD4 T细胞计数。 HAART是否可以改善CD4 T细胞功能以及影响免疫重建的生物学特性尚不清楚。我们进行了公开的前瞻性试点研究,以解决这些问题。包括未接受过治疗和先前接受过治疗的患者。方法:20例患者(7例为幼稚,13例先前接受过治疗)分别接受一种蛋白酶抑制剂和两种逆转录酶抑制剂的治疗,并随访12个月。我们测量了响应巨细胞病毒和结核菌素抗原的CD4细胞增殖,并在基线以及第1、3、6、9和12个月时计数了CD4细胞的亚群。在基线时无抗原特异性反应性但在接受HAART时出现抗原特异性反应的患者被归类为免疫应答者。结果:4名患者在基线时具有抗原特异性反应性,而在12个月时为14名(p <0.001)。在第3个月到第12个月之间,病毒载量从基线下降了1.5个日志拷贝/mL(4.6个日志拷贝/ mL),中位数下降了,而CD4细胞计数的中位数增加了63个/微升(从93个/微升)。十名患者(七名天真儿童中的六名,先前治疗的十三名中的四名)是免疫应答者。它们与十个无反应者的显着不同之处在于,它们的病毒载量持续降低了12个月,CD4计数的增加更大,并且它们显示记忆性CD4 T细胞随着幼稚T细胞的增加而早期增加。解释:在严重免疫抑制的患者中,HAART可以诱导针对机会性病原体的CD4 T细胞反应性持续恢复。这种恢复不取决于基线值,而是取决于病毒载量减少的幅度和持续时间以及记忆CD4 T细胞的增加。

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