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在肯尼亚性工作者中,HIV中和免疫球蛋白A和HIV特异性增殖与HIV感染率降低独立相关。

HIV-neutralizing immunoglobulin A and HIV-specific proliferation are independently associated with reduced HIV acquisition in Kenyan sex workers.

作者信息

Hirbod Taha, Kaul Rupert, Reichard Camilla, Kimani Joshua, Ngugi Elizabeth, Bwayo Job J, Nagelkerke Nico, Hasselrot Klara, Li Bing, Moses Stephen, MacDonald Kelly S, Broliden Kristina

机构信息

Infectious Diseases Unit, Department of Medicine, Solna, Center for Molecular Medicine, Karolinska Institutet, Karolinska University Hospital, Solna, Sweden.

出版信息

AIDS. 2008 Mar 30;22(6):727-35. doi: 10.1097/QAD.0b013e3282f56b64.

Abstract

OBJECTIVES

HIV-neutralizing immunoglobulin A (IgA) and HIV-specific cellular immunity have been described in highly exposed, persistently seronegative (HEPS) individuals, but well controlled studies have not been performed. We performed a prospective, nested case-control study to examine the association of genital IgA and systemic cellular immune responses with subsequent HIV acquisition in high-risk Kenyan female sex workers (FSWs).

DESIGN AND METHODS

A randomized trial of monthly antibiotic prophylaxis to prevent sexually transmitted disease/HIV infection was performed from 1998 to 2002 in HIV-uninfected Kenyan FSWs. After the completion of trial, FSWs who had acquired HIV (cases) were matched 1: 4 with persistently uninfected controls based on study arm, duration of HIV-seronegative follow-up, and time of cohort enrolment. Blinded investigators assayed the ability at enrolment of genital IgA to neutralize primary HIV isolates as well as systemic HIV-specific cellular IFNgamma-modified enzyme-linked immunospot and proliferative responses.

RESULTS

The study cohort comprised 113 FSWs: 24 cases who acquired HIV and 89 matched controls. Genital HIV-neutralizing IgA was associated with reduced HIV acquisition (P = 0.003), as was HIV-specific proliferation (P = 0.002), and these associations were additive. HIV-specific IFNgamma production did not differ between case and control groups. In multivariable analysis, HIV-neutralizing IgA and HIV-specific proliferation each remained independently associated with lack of HIV acquisition. Genital herpes (HSV2) was associated with increased HIV risk and with reduced detection of HIV-neutralizing IgA.

CONCLUSION

Genital HIV-neutralizing IgA and systemic HIV-specific proliferative responses, assayed by blinded investigators, were prospectively associated with HIV nonacquisition. The induction of these immune responses may be an important goal for HIV vaccines.

摘要

目的

在高度暴露但持续血清学阴性(HEPS)个体中已发现有HIV中和性免疫球蛋白A(IgA)及HIV特异性细胞免疫,但尚未开展充分对照研究。我们开展了一项前瞻性巢式病例对照研究,以探究肯尼亚高危女性性工作者(FSW)的生殖道IgA和全身细胞免疫反应与后续HIV感染之间的关联。

设计与方法

1998年至2002年对未感染HIV的肯尼亚FSW进行了一项预防性病/HIV感染的每月抗生素预防随机试验。试验结束后,根据研究分组、HIV血清学阴性随访时间及队列入组时间,将已感染HIV的FSW(病例)与持续未感染的对照按1:4进行匹配。盲法研究者检测了入组时生殖道IgA中和原发性HIV分离株的能力以及全身HIV特异性细胞γ干扰素改良酶联免疫斑点试验和增殖反应。

结果

研究队列包括113名FSW:24例HIV感染者及89名匹配对照。生殖道HIV中和性IgA与HIV感染减少相关(P = 0.003),HIV特异性增殖也与之相关(P = 0.002),且这些关联具有相加性。病例组和对照组之间HIV特异性γ干扰素产生无差异。在多变量分析中,HIV中和性IgA和HIV特异性增殖各自仍独立与未感染HIV相关。生殖器疱疹(HSV2)与HIV感染风险增加及HIV中和性IgA检测减少相关。

结论

盲法研究者检测的生殖道HIV中和性IgA和全身HIV特异性增殖反应与未感染HIV呈前瞻性相关。诱导这些免疫反应可能是HIV疫苗的一个重要目标。

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