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树突状细胞特异性细胞间黏附分子3结合非整合素/CD209在正常人淋巴结的巨噬细胞上大量存在,并且在混合淋巴细胞反应中树突状细胞刺激过程中并非必需。

Dendritic cell-specific intercellular adhesion molecule 3-grabbing nonintegrin/CD209 is abundant on macrophages in the normal human lymph node and is not required for dendritic cell stimulation of the mixed leukocyte reaction.

作者信息

Granelli-Piperno Angela, Pritsker Alla, Pack Maggi, Shimeliovich Irina, Arrighi Jean-Francois, Park Chae Gyu, Trumpfheller Christine, Piguet Vincent, Moran Thomas M, Steinman Ralph M

机构信息

Laboratory of Cellular Physiology and Immunology and Chris Browne Center for Immunology and Immune Diseases, Rockefeller University, New York, NY 10021, USA.

出版信息

J Immunol. 2005 Oct 1;175(7):4265-73. doi: 10.4049/jimmunol.175.7.4265.

Abstract

The C-type lectin dendritic cell-specific ICAM 3-grabbing nonintegrin (DC-SIGN)/CD209 efficiently binds several pathogens, including HIV-1. DC-SIGN is expressed on monocyte-derived DCs in culture, and importantly, it is able to sequester HIV-1 within cells and facilitate transmission of virus to CD4+ T cells. To investigate DC-SIGN function, we have generated new mAbs. We report in this study that these and prior anti-DC-SIGN mAbs primarily label macrophages in the medullary sinuses of noninflamed human lymph node. In contrast, expression is not detected on most DCs in the T cell area, except for occasional cells. We also noted that IL-4 alone can induce expression of DC-SIGN in CD14+ monocytes and circulating blood DCs. However, blockade of DC-SIGN with Abs and DC-SIGN small interfering RNA did not result in a major reduction in the capacity of these DCs to transfer HIV to T cells, confirming significant DC-SIGN-independent mechanisms. The blocking approaches did reduce HIV-1 transmission by DC-SIGN-transfected cells by >90%. DC-SIGN blockade also did not reduce the ability of DCs to stimulate T cell proliferation in the MLR. These results indicate that DC-SIGN has the potential to contribute to macrophage function in normal human lymph node, and that DCs do not require DC-SIGN to transmit HIV or to initiate T cell responses.

摘要

C型凝集素树突状细胞特异性细胞间黏附分子3抓取非整合素(DC-SIGN)/CD209能有效结合多种病原体,包括HIV-1。DC-SIGN在培养的单核细胞来源的树突状细胞上表达,重要的是,它能够将HIV-1隔离在细胞内,并促进病毒向CD4+ T细胞的传播。为了研究DC-SIGN的功能,我们制备了新的单克隆抗体。我们在本研究中报告,这些以及先前的抗DC-SIGN单克隆抗体主要标记未发炎的人类淋巴结髓窦中的巨噬细胞。相比之下,在T细胞区的大多数树突状细胞上未检测到表达,除了偶尔的细胞。我们还注意到,单独的IL-4可诱导CD14+单核细胞和循环血液树突状细胞中DC-SIGN的表达。然而,用抗体和DC-SIGN小干扰RNA阻断DC-SIGN并没有导致这些树突状细胞将HIV转移至T细胞的能力大幅降低,这证实了存在显著的不依赖DC-SIGN的机制。这些阻断方法确实使DC-SIGN转染细胞的HIV-1传播减少了>90%。DC-SIGN阻断也没有降低树突状细胞在混合淋巴细胞反应中刺激T细胞增殖的能力。这些结果表明,DC-SIGN有可能在正常人类淋巴结中发挥巨噬细胞功能,并且树突状细胞在传递HIV或启动T细胞反应时不需要DC-SIGN。

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