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将Siglec-H鉴定为一种在小鼠浆细胞样树突状细胞前体上表达的新型内吞受体。

Characterization of Siglec-H as a novel endocytic receptor expressed on murine plasmacytoid dendritic cell precursors.

作者信息

Zhang Jiquan, Raper Anna, Sugita Noriko, Hingorani Ravi, Salio Mariolina, Palmowski Michael J, Cerundolo Vincenzo, Crocker Paul R

机构信息

Division of Cell Biology and Immunology, School of Life Sciences, Wellcome Trust Biocentre at Dundee, University of Dundee, Dundee DD1 5EH, United Kingdom.

出版信息

Blood. 2006 May 1;107(9):3600-8. doi: 10.1182/blood-2005-09-3842. Epub 2006 Jan 5.

DOI:10.1182/blood-2005-09-3842
PMID:16397130
Abstract

We describe the cloning and characterization of Siglec-H, a novel murine CD33-related siglec-like molecule with 2 immunoglobulin domains. Unlike other CD33-related siglecs, Siglec-H lacks tyrosine-based signaling motifs in its cytoplasmic tail. Although Siglec-H has the typical structural features required for sialic acid binding, no evidence for carbohydrate recognition was obtained. Specific monoclonal and polyclonal antibodies (Abs) were raised to Siglec-H and used to define its cellular expression pattern and functional properties. By flow cytometry, Siglec-H was expressed specifically on plasmacytoid dendritic cell (pDC) precursors in bone marrow, spleen, blood, and lymph nodes. Staining of tissue sections showed that Siglec-H was also expressed in a subset of marginal zone macrophages in the spleen and in medullary macrophages in lymph nodes. Using bone marrow-derived pDC precursors that express Siglec-H, addition of Abs did not influence cytokine production, either in the presence or absence of synthetic oligodeoxynucleotides containing unmethylated cytosine-guanine motifs (CpG). In comparison, Siglec-H functioned as an endocytic receptor and mediated efficient internalization of anti-Siglec-H Abs. By immunizing mice with ovalbumin-conjugated anti-Siglec-H Ab in the presence of CpG, we demonstrate generation of antigen-specific CD8 T cells in vivo. Targeting Siglec-H may therefore be a useful way of delivering antigens to pDC precursors for cross-presentation.

摘要

我们描述了Siglec-H的克隆和特性,它是一种新型的小鼠CD33相关的类似唾液酸结合凝集素的分子,具有2个免疫球蛋白结构域。与其他CD33相关的唾液酸结合凝集素不同,Siglec-H在其细胞质尾部缺乏基于酪氨酸的信号基序。尽管Siglec-H具有唾液酸结合所需的典型结构特征,但未获得碳水化合物识别的证据。针对Siglec-H制备了特异性单克隆和多克隆抗体(Abs),并用于确定其细胞表达模式和功能特性。通过流式细胞术,Siglec-H在骨髓、脾脏、血液和淋巴结中的浆细胞样树突状细胞(pDC)前体上特异性表达。组织切片染色显示,Siglec-H也在脾脏边缘区巨噬细胞的一个亚群以及淋巴结髓样巨噬细胞中表达。使用表达Siglec-H的骨髓来源的pDC前体,无论是否存在含有未甲基化胞嘧啶-鸟嘌呤基序(CpG)的合成寡脱氧核苷酸,添加抗体均不影响细胞因子的产生。相比之下,Siglec-H作为一种内吞受体,介导抗Siglec-H抗体的有效内化。通过在CpG存在的情况下用卵清蛋白偶联的抗Siglec-H抗体免疫小鼠,我们证明了体内抗原特异性CD8 T细胞的产生。因此,靶向Siglec-H可能是将抗原递送至pDC前体进行交叉呈递的一种有用方法。

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