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抗逆转录病毒疗法对免疫重建的影响。

Effects of antiretroviral therapy on immune reconstitution.

作者信息

Autran B

机构信息

Laboratoire d'Immunologie Cellulaire et Tissulaire, Hôpital Pitié-Salpêtrière, Paris, France.

出版信息

Antivir Ther. 1999;4 Suppl 3:3-6.

PMID:16021864
Abstract

CD4 cell counts in human immunodeficiency virus (HIV)-infected patients increase under effective highly active antiretroviral therapy (HAART). Similar kinetics of response is observed irrespective of the stage of infection in which HAART is initiated. An early rise in memory cells is followed by a gradual and continual rise in naive cells, which reflects ongoing thymic production and these cells exhibit rediversification of the CD4 T cell repertoire damaged during HIV-1 infection. Studies in patients receiving HAART indicate that the responsiveness of memory CD4 T cells to opportunistic pathogens is restored. Although response to rare antigens or HIV-1 is generally not preserved in patients initiating HAART during established infection, the ability to detect Th1 response in vitro indicates that antigen-specific cells are not completely depleted in many cases. Strong response of tetanus toxoid-specific cells after administration of tetanus toxoid vaccine and strong HIV-1 p24-specific response after the re-exposure to viral antigen because of treatment interruption have been observed in the context of effective therapy initiated during advanced infection. These findings suggest that long-term immune recovery is feasible when HAART is given during chronic infection and might require immune intervention in addition to stable virus control.

摘要

在接受高效抗逆转录病毒疗法(HAART)治疗的人类免疫缺陷病毒(HIV)感染患者中,CD4细胞计数会增加。无论开始HAART时处于感染的哪个阶段,都会观察到类似的反应动力学。记忆细胞早期上升之后,幼稚细胞会逐渐持续上升,这反映了胸腺的持续生成,并且这些细胞表现出在HIV-1感染期间受损的CD4 T细胞库的重新多样化。对接受HAART治疗的患者的研究表明,记忆性CD4 T细胞对机会性病原体的反应性得以恢复。尽管在已确立感染期间开始接受HAART治疗的患者中,对稀有抗原或HIV-1的反应通常无法保留,但体外检测Th1反应的能力表明,在许多情况下抗原特异性细胞并未完全耗尽。在晚期感染期间开始有效治疗的背景下,观察到破伤风类毒素疫苗接种后破伤风类毒素特异性细胞的强烈反应,以及因治疗中断再次接触病毒抗原后HIV-1 p24特异性的强烈反应。这些发现表明,在慢性感染期间给予HAART时,长期免疫恢复是可行的,并且除了稳定的病毒控制外可能还需要免疫干预。

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