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血友病患者中HIV抗原及p24和gp41抗体的长期评估。潜在的临床意义。

Long-term evaluation of HIV antigen and antibodies to p24 and gp41 in patients with hemophilia. Potential clinical importance.

作者信息

Allain J P, Laurian Y, Paul D A, Verroust F, Leuther M, Gazengel C, Senn D, Larrieu M J, Bosser C

机构信息

Department of Medical Affairs, Abbott Laboratories, Abbott Park, IL 60064.

出版信息

N Engl J Med. 1987 Oct 29;317(18):1114-21. doi: 10.1056/NEJM198710293171804.

Abstract

To investigate the relation between human immunodeficiency virus (HIV) antigenemia and clinical manifestations of HIV infections, we studied 96 patients with hemophilia who were positive for HIV antibody, for a median of 34 months. Every 4 to 10 months a clinical and laboratory examination was performed and serum samples were tested for three HIV markers: HIV antigen, antibody to p24, and antibody to gp41. Twenty-two subjects (23 percent) were found to be positive for HIV antigen: 8 were positive upon entry and remained so (Group 1), and 14 became positive during the study, 4 to 26 months after HIV antibody appeared (seroconversion), 13 of whom remained positive for HIV antigen (Group 2). Most subjects positive for HIV antigen had low or undetectable titers of antibody to p24, whereas the antibody titer to gp41 remained high. In Group 2, patients with low p24 antibody titers had further decreases in their titers before or at the time HIV antigen appeared. Once present, HIV antigen persisted and tended to increase in concentration. In contrast to Group 3 (negative for HIV antigen, low anti-p24 titer) and 4 (negative for HIV antigen, high anti-p24 titer), the groups positive for HIV antigen had significantly higher incidences of acquired immunodeficiency syndrome (P = 0.05), immunodeficiency-related infections (P less than 0.001), and immune thrombocytopenia (P = 0.001), and had more severe disease as measured by the Walter Reed staging system (P less than 0.001). In this study, HIV antigen appeared to be a better predictive marker of HIV-related complications than the absolute T4+ count. These results suggest that HIV antigenemia indicates a poor clinical prognosis.

摘要

为了研究人类免疫缺陷病毒(HIV)抗原血症与HIV感染临床表现之间的关系,我们对96例HIV抗体呈阳性的血友病患者进行了研究,研究时间中位数为34个月。每4至10个月进行一次临床和实验室检查,并检测血清样本中的三种HIV标志物:HIV抗原、p24抗体和gp41抗体。发现22名受试者(23%)HIV抗原呈阳性:8名在入组时呈阳性并一直保持(第1组),14名在研究期间呈阳性,即在HIV抗体出现(血清转化)后4至26个月呈阳性,其中13名HIV抗原持续呈阳性(第2组)。大多数HIV抗原呈阳性的受试者p24抗体滴度较低或检测不到,而gp41抗体滴度仍然较高。在第2组中,p24抗体滴度较低的患者在HIV抗原出现之前或之时其滴度进一步下降。一旦出现,HIV抗原持续存在且浓度有升高趋势。与第3组(HIV抗原阴性,p24抗体滴度低)和第4组(HIV抗原阴性,p24抗体滴度高)相比,HIV抗原呈阳性的组获得性免疫缺陷综合征的发病率显著更高(P = 0.05),免疫缺陷相关感染的发病率显著更高(P < 0.001),免疫性血小板减少症的发病率显著更高(P = 0.001),并且根据沃尔特·里德分期系统衡量病情更严重(P < 0.001)。在本研究中,HIV抗原似乎是比绝对T4 +细胞计数更好的HIV相关并发症预测标志物。这些结果表明,HIV抗原血症预示着不良的临床预后。

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