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有症状的原发性HIV-1感染患者血浆中存在高滴度的细胞病变病毒。

High titers of cytopathic virus in plasma of patients with symptomatic primary HIV-1 infection.

作者信息

Clark S J, Saag M S, Decker W D, Campbell-Hill S, Roberson J L, Veldkamp P J, Kappes J C, Hahn B H, Shaw G M

机构信息

Department of Medicine, University of Alabama, Birmingham 35294.

出版信息

N Engl J Med. 1991 Apr 4;324(14):954-60. doi: 10.1056/NEJM199104043241404.

Abstract

BACKGROUND

Primary infection with the human immunodeficiency virus (HIV-1) frequently causes an acute, self-limited viral syndrome. To examine the relations among viral replication, the immune response of the host, and clinical illness during this initial phase of infection, we undertook a quantitative, molecular, and biologic analysis of infectious HIV-1 in the blood and plasma of three patients with symptomatic primary infection and of a sexual partner of one of them.

METHODS

During an eight-week period of primary infection, HIV-1 was cultured frequently in dilutions of plasma and peripheral-blood mononuclear cells (PBMC), and levels of HIV-1 antigen and antibody were determined sequentially by enzyme-linked immunosorbent assay and immunoblotting. Replication-competent HIV-1 proviruses were cloned and characterized biologically.

RESULTS

Six to 15 days after the onset of symptoms, high titers of infectious HIV-1 (from 10 to 10(3) tissue-culture-infective doses per milliliter of plasma) and viral p24 antigen were detected in the plasma of all three patients. These titers fell precipitously by day 27, and the decline coincided with an increase in the levels of antiviral antibodies and the resolution of symptoms. Sequential isolates of virus from plasma and PBMC obtained throughout the period of primary infection, as well as virus derived from two molecular proviral clones, were highly cytopathic for normal-donor PBMC and immortalized T cells, despite the marked reduction in the titers of virus in plasma.

CONCLUSIONS

Primary, symptomatic HIV-1 infection is associated with high titers of cytopathic, replication-competent viral strains, and during such infection potential infectivity is enhanced. Effective control of HIV-1 replication during primary infection implies the activation of clinically important mechanisms of immune defense that merit further examination in relation to the development of antiviral therapy and vaccines.

摘要

背景

人类免疫缺陷病毒1型(HIV-1)的初次感染常引发一种急性、自限性病毒综合征。为了研究感染初始阶段病毒复制、宿主免疫反应和临床疾病之间的关系,我们对三名有症状初次感染患者及其一名性伴侣的血液和血浆中的传染性HIV-1进行了定量、分子和生物学分析。

方法

在初次感染的八周期间,经常对血浆和外周血单个核细胞(PBMC)的稀释液进行HIV-1培养,并通过酶联免疫吸附测定和免疫印迹法依次测定HIV-1抗原和抗体水平。具有复制能力的HIV-1前病毒被克隆并进行生物学特性分析。

结果

症状出现后6至15天,在所有三名患者的血浆中检测到高滴度的传染性HIV-1(每毫升血浆10至10³组织培养感染剂量)和病毒p24抗原。这些滴度在第27天急剧下降,且下降与抗病毒抗体水平的升高及症状的缓解同时发生。在初次感染期间从血浆和PBMC中连续分离得到的病毒,以及来自两个分子前病毒克隆的病毒,尽管血浆中病毒滴度显著降低,但对正常供体PBMC和永生化T细胞具有高度细胞病变效应。

结论

有症状的HIV-1初次感染与高滴度的具有细胞病变效应、有复制能力的病毒株相关,且在此类感染期间潜在传染性增强。初次感染期间对HIV-1复制的有效控制意味着激活了临床上重要的免疫防御机制,这在抗病毒治疗和疫苗的研发方面值得进一步研究。

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