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中和抗体和 Fc 介导的抑制性抗体可抑制朗格汉斯细胞和间质树突状细胞中的 HIV-1 复制。

HIV-1 replication in Langerhans and interstitial dendritic cells is inhibited by neutralizing and Fc-mediated inhibitory antibodies.

机构信息

INSERM-UDS, Institute of Virology, Faculté de Médecine, 3 rue Koeberlé, F-67000 Strasbourg, France.

出版信息

J Virol. 2011 Jan;85(2):1077-85. doi: 10.1128/JVI.01619-10. Epub 2010 Nov 17.

Abstract

Langerhans cells (LCs) and interstitial dendritic cells (IDCs) may be among the first human immunodeficiency virus type 1 (HIV-1) targets after sexual transmission. We generated cells of these types by differentiation of purified CD34(+) cord blood cells. After in vitro infection with R5-tropic strains, we obtained similar percentages of infected cells for both dendritic cell (DC) subsets. Moreover, LC infection was not increased by blockage of langerin by antilangerin. These results indicate that, under our experimental conditions, there was no evidence of any preference of HIV replication in LCs versus IDCs. The inhibitory activity of HIV-1-specific IgAs and IgGs against HIV-1 replication in LCs and IDCs was analyzed. We found that neutralizing antibodies inhibit HIV-1 infection of both DC subsets. Interestingly, HIV-1 was inhibited more efficiently by the IgGs than the corresponding IgA, due to an Fcγ receptor-dependent mechanism. Moreover, nonneutralizing inhibitory IgGs were able to inhibit infection of both LCs and IDCs. These results underline the importance of HIV-1 inhibition by the binding of the Fc part of IgGs to Fcγ receptors and suggest that the induction of neutralizing and nonneutralizing inhibitory IgGs in addition to neutralizing IgAs at mucosal sites may contribute to protection against sexual transmission of HIV-1.

摘要

郎格汉斯细胞(LCs)和间质树突状细胞(IDCs)可能是人类免疫缺陷病毒 1 型(HIV-1)在性传播后最早的靶细胞之一。我们通过纯化的 CD34+脐血细胞的分化产生了这些类型的细胞。体外感染 R5 嗜性株后,我们获得了两种树突状细胞(DC)亚群的感染细胞比例相似。此外,抗 langerin 阻断 langerin 不会增加 LC 的感染。这些结果表明,在我们的实验条件下,没有证据表明 HIV 复制在 LCs 与 IDCs 之间存在任何偏好。分析了 HIV-1 特异性 IgA 和 IgG 对 LCs 和 IDCs 中 HIV-1 复制的抑制活性。我们发现中和抗体抑制两种 DC 亚群的 HIV-1 感染。有趣的是,由于 Fcγ 受体依赖性机制,IgG 比相应的 IgA 更有效地抑制 HIV-1 的感染。此外,非中和抑制性 IgG 能够抑制 LCs 和 IDCs 的感染。这些结果强调了 HIV-1 抑制的重要性,通过 IgG 的 Fc 部分与 Fcγ 受体的结合,并表明除了黏膜部位的中和性和非中和性抑制性 IgA 外,诱导中和性和非中和性抑制性 IgG 可能有助于防止 HIV-1 的性传播。

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