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首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Soluble Domain 1 of Platelet–Endothelial Cell Adhesion Molecule (PECAM) Is Sufficient to Block Transendothelial Migration In Vitro and In Vivo
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Soluble Domain 1 of Platelet–Endothelial Cell Adhesion Molecule (PECAM) Is Sufficient to Block Transendothelial Migration In Vitro and In Vivo

机译:血小板-内皮细胞粘附分子(PECAM)的可溶性域1足以阻止体内和体外的跨内皮迁移。

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摘要

The inflammatory response involves sequential adhesive interactions between cell adhesion molecules of leukocytes and the endothelium. Unlike the several adhesive steps that precede it, transendothelial migration (diapedesis), the step in which leukocytes migrate between apposed endothelial cells, appears to involve primarily one adhesion molecule, platelet–endothelial cell adhesion molecule (PECAM, CD31). Therefore, we have focused on PECAM as a target for antiinflammatory therapy. We demonstrate that soluble chimeras made of the entire extracellular portion of PECAM, or of only the first immunoglobulin domain of PECAM, fused to the Fc portion of IgG, block diapedesis in vitro and in vivo. Furthermore, the truncated form of the PECAM-IgG chimera does not bind stably to its cellular ligand. This raises the possibility of selective anti-PECAM therapies that would not have the untoward opsonic or cell-activating properties of antibodies directed against PECAM.
机译:炎症反应涉及白细胞的细胞粘附分子与内皮之间的顺序粘附相互作用。与之前的几个粘附步骤不同,跨内皮迁移(透血作用)是白细胞在相对的内皮细胞之间迁移的步骤,似乎主要涉及一个粘附分子,即血小板-内皮细胞粘附分子(PECAM,CD31)。因此,我们将PECAM作为抗炎治疗的目标。我们证明,由PECAM的整个胞外部分或仅由PECAM的第一个免疫球蛋白结构域融合到IgG的Fc部分制成的可溶性嵌合体,在体外和体内均可阻止尿布分离。此外,PECAM-IgG嵌合体的截短形式不能稳定地与其细胞配体结合。这就增加了选择性抗PECAM治疗的可能性,这种治疗不会具有针对PECAM的抗体所不希望的调理或细胞活化特性。

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