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混合性结缔组织病自身免疫患者亚群血清抗体对1型艾滋病毒感染性的中和作用。

Neutralization of HIV type 1 infectivity by serum antibodies from a subset of autoimmune patients with mixed connective tissue disease.

作者信息

Douvas A, Takehana Y, Ehresmann G, Chernyovskiy T, Daar E S

机构信息

Department of Medicine, University of Southern California School of Medicine, Los Angeles 90033, USA.

出版信息

AIDS Res Hum Retroviruses. 1996 Nov 1;12(16):1509-17. doi: 10.1089/aid.1996.12.1509.

DOI:10.1089/aid.1996.12.1509
PMID:8911576
Abstract

Mixed connective tissue disease (MCTD) is a rheumatic disorder with clinical similarities to HIV-1 infection, and with characteristic autoimmune anti-RNP antibodies specific for the U1 snRNP splicing complex. Anti-RNP antibodies cross-react with the HIV-1 surface, owing to multiple homologies between the gp120/41 envelope complex and the 70K protein of U1 snRNP. A key epitope of 70K, its RNA-binding site, is homologous to a dominant B and T cell epitope in the third variable loop (V3) of gp120. In this study, we tested the ability of anti-RNP sera to inhibit HIV-1 infectivity in vitro. Of nine sera tested, five were 70-99% effective in neutralizing one or more HIV-1 strains. One serum was > 99% effective in neutralizing HIV-1MN, and 86 and 77% effective against the primary isolates HIV-1(CO) and HIV-1(JR-FL), respectively, an efficacy equal to that of a pool of broadly neutralizing antibodies from HIV-1-infected subjects (HIVIG). The mean neutralizing titer of anti-RNP sera against HIV-1(JR-FL) was 3.9-fold higher than that of HIVIG. Neutralizing potency was associated with high reactivity to gp120 by ELISA, and with the presence of serum rheumatoid factor, known to enhance antibody neutralization of other viruses. The current findings provide further evidence that individuals unexposed to HIV-1 may develop immunologic resistance by alternative mechanisms, possibly including molecular mimicry, or exposure to as yet unidentified retroviruses. Thus MCTD, which involves both B and T cell reactivity to self-epitopes homologous to HIV-1, may elucidate new strategies for generating protective immunity to this virus.

摘要

混合性结缔组织病(MCTD)是一种风湿性疾病,在临床上与HIV-1感染相似,具有针对U1 snRNP剪接复合体的特征性自身免疫抗RNP抗体。抗RNP抗体与HIV-1表面发生交叉反应,这是由于gp120/41包膜复合体与U1 snRNP的70K蛋白之间存在多种同源性。70K的一个关键表位,即其RNA结合位点,与gp120第三个可变环(V3)中的一个显性B细胞和T细胞表位同源。在本研究中,我们测试了抗RNP血清在体外抑制HIV-1感染性的能力。在检测的9份血清中,5份对一种或多种HIV-1毒株的中和效力为70%-99%。一份血清对HIV-1MN的中和效力>99%,对原发性分离株HIV-1(CO)和HIV-1(JR-FL)的中和效力分别为86%和77%,其效力与来自HIV-1感染受试者的一组广泛中和抗体(HIVIG)相当。抗RNP血清对HIV-1(JR-FL)的平均中和滴度比HIVIG高3.9倍。中和效力与ELISA检测中对gp120的高反应性以及血清类风湿因子的存在有关,已知血清类风湿因子可增强对其他病毒的抗体中和作用。目前的研究结果进一步证明,未接触过HIV-1的个体可能通过其他机制产生免疫抗性,可能包括分子模拟,或接触尚未鉴定的逆转录病毒。因此,涉及B细胞和T细胞对与HIV-1同源的自身表位反应的MCTD,可能阐明产生针对该病毒的保护性免疫的新策略。

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