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1型人类免疫缺陷病毒感染者病毒载量及替代标志物与临床进展关系的前瞻性纵向分析。

Prospective longitudinal analysis of viral load and surrogate markers in relation to clinical progression in HIV type 1-infected persons.

作者信息

Bruisten S M, Frissen P H, Van Swieten P, Harrigan P R, Kinghorn I, Larder B, Weigel H M, De Vries E, Regez R M, Henrichs J H, Koot M, Huisman J G

机构信息

Department of Clinical Viro-Immunology, Central Laboratory of The Netherlands Red Cross Blood Transfusion Service, Amsterdam, The Netherlands.

出版信息

AIDS Res Hum Retroviruses. 1997 Mar 1;13(4):327-35. doi: 10.1089/aid.1997.13.327.

Abstract

The temporal relationship between viral and surrogate markers and clinical status was analyzed prospectively every 8 weeks in 34 asymptomatic HIV-1-infected persons. After 3 years, 25 persons remained clinically healthy whereas 9 persons showed clinical progression. In accordance with other reports we found that at study entry HIV-RNA load was predictive of clinical progression. All markers tested evolved significantly in time in both progressors and nonprogressors. The HIV RNA load in plasma and HIV DNA load in T cells were linearly related only in nonprogressors. In addition, the RNA/DNA ratio during follow-up was significantly higher in progressors, indicating a higher replication rate in progressors. The HIV DNA load correlated inversely with CD4+ T cell counts and positively with p24 antigenemia in both nonprogressors and progressors. A significant correlation of HIV DNA load with SI phenotype occurred in progressors only. HIV RNA levels correlated with beta 2-microglobulin level and with p24 antigenemia but not with SI phenotype. These three markers can all routinely be measured in plasma; however, only the HIV RNA levels appear to be informative for clinical progression. Six to 8 months before clinical progression, an SI phenotype switch, increased HIV RNA in plasma, and decreased CD4+ T cell counts were all indicative of an impending clinical event.

摘要

对34名无症状的HIV-1感染者每8周进行一次前瞻性分析,以研究病毒标志物、替代标志物与临床状态之间的时间关系。3年后,25人临床健康,而9人出现临床进展。与其他报告一致,我们发现研究开始时HIV-RNA载量可预测临床进展。在进展者和非进展者中,所有检测的标志物均随时间有显著变化。仅在非进展者中,血浆中的HIV RNA载量与T细胞中的HIV DNA载量呈线性相关。此外,随访期间进展者的RNA/DNA比值显著更高,表明进展者的复制率更高。在非进展者和进展者中,HIV DNA载量均与CD4+T细胞计数呈负相关,与p24抗原血症呈正相关。仅在进展者中,HIV DNA载量与SI表型存在显著相关性。HIV RNA水平与β2-微球蛋白水平及p24抗原血症相关,但与SI表型无关。这三种标志物均可在血浆中常规检测;然而,只有HIV RNA水平似乎对临床进展具有提示意义。在临床进展前6至8个月,SI表型转换、血浆中HIV RNA增加以及CD4+T细胞计数减少均表明即将发生临床事件。

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