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首页> 外文期刊>Journal of cell biology >The Vitronectin Receptor and its Associated CD47 Molecule Mediates Proinflammatory Cytokine Synthesis in Human Monocytes by Interaction with Soluble CD23
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The Vitronectin Receptor and its Associated CD47 Molecule Mediates Proinflammatory Cytokine Synthesis in Human Monocytes by Interaction with Soluble CD23

机译:玻连蛋白受体及其相关的CD47分子通过与可溶性CD23相互作用介导人单核细胞促炎性细胞因子的合成。

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The vitronectin receptor, αvβ3 integrin, plays an important role in tumor cell invasion, angiogenesis, and phagocytosis of apoptotic cells. CD47, a member of the multispan transmembrane receptor family, physically and functionally associates with vitronectin receptor (VnR). Although vitronectin (Vn) is not a ligand of CD47, anti-CD47 and β3 mAbs suppress Vn, but not fibronectin (Fn) binding and function. Here, we show that anti-CD47, anti-β3 mAb and Vn, but not Fn, inhibit sCD23-mediated proinflammatory function (TNF-α, IL-12, and IFN-γ release). Surprisingly, anti-CD47 and β3 mAbs do not block sCD23 binding to αv+β3+ T cell lines, whereas Vn and an αv mAb (clone AMF7) do inhibit sCD23 binding, suggesting the VnR complex may be a functional receptor for sCD23. sCD23 directly binds αv+β3+/CD47? cell lines, but coexpression of CD47 increases binding. Moreover, sCD23 binds purified αv protein and a single human αv chain CHO transfectant. We conclude that the VnR and its associated CD47 molecule may function as a novel receptor for sCD23 to mediate its proinflammatory activity and, as such, may be involved in the inflammatory process of the immune response.
机译:玻连蛋白受体αvβ3整合素在肿瘤细胞侵袭,血管生成和凋亡细胞吞噬中起重要作用。 CD47是跨跨膜受体家族的成员,在物理上和功能上与玻连蛋白受体(VnR)相关。尽管玻连蛋白(Vn)不是CD47的配体,但抗CD47和β3mAb抑制Vn,但不抑制纤连蛋白(Fn)的结合和功能。在这里,我们显示抗CD47,抗β3mAb和Vn而非Fn抑制sCD23介导的促炎功能(TNF-α,IL-12和IFN-γ释放)。出乎意料的是,抗CD47和β3mAb不会阻断sCD23与αv+β3+ T细胞系的结合,而Vn和αvmAb(克隆AMF7)确实抑制sCD23结合,这表明VnR复合物可能是sCD23的功能受体。 sCD23直接结合αv+β3+ / CD47?细胞系,但CD47的共表达可增强结合。此外,sCD23结合纯化的αv蛋白和单个人αv链CHO转染子。我们得出的结论是,VnR及其相关的CD47分子可能充当sCD23的新受体,以介导其促炎活性,因此可能参与了免疫应答的炎症过程。

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