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将受损内皮细胞中暴露的抗原鉴定为层粘连蛋白结合蛋白的遗传学方法。

Genetic identification of antigens exposed in damaged endothelial cells as laminin-binding proteins.

作者信息

Ireland D C, Spring E L, Moiseeva E, de Bono D P

机构信息

Department of Medicine, University of Leicester Clinical Sciences Wing, Glenfield Hospital, UK.

出版信息

Clin Exp Immunol. 1998 May;112(2):255-61. doi: 10.1046/j.1365-2249.1998.00567.x.

Abstract

A monoclonal antibody, D5G2, which reacts in a balloon angioplasty damage model with unfixed damaged but not with unfixed undamaged human endothelial cells, was used to screen a human endothelial cDNA library in an Escherichia coli/lambda gt11 expression system. Sequences of DNA inserts in D5G2+ phage clones matched those reported for a laminin-binding protein, LBP-32. Both D5G2 and purified laminin bound to a polypeptide of 55 kD on PVDF membranes carrying electrophoretically separated endothelial cell lysates, D5G2 also bound to recombinant LBP expressed in E. coli, and showed similar staining patterns on human and bovine endothelial cells to another characterized anti-LBP antibody. Increased staining of unfixed endothelial cells on detergent permeabilization suggests that D5G2 binds to intracellular laminin-binding protein made accessible by cell membrane injury. Antibodies to intracellular targets exposed by cell damage may be useful in anchoring therapeutic agents at sites of vascular damage.

摘要

一种单克隆抗体D5G2,在球囊血管成形术损伤模型中,它能与未固定的受损人内皮细胞发生反应,但不与未固定的未受损人内皮细胞发生反应,利用该抗体在大肠杆菌/λgt11表达系统中筛选人内皮细胞cDNA文库。D5G2 +噬菌体克隆中的DNA插入片段序列与报道的层粘连蛋白结合蛋白LBP - 32的序列相匹配。D5G2和纯化的层粘连蛋白都与携带经电泳分离的内皮细胞裂解物的PVDF膜上的55 kD多肽结合,D5G2也与在大肠杆菌中表达的重组LBP结合,并且在人和牛内皮细胞上与另一种已鉴定的抗LBP抗体显示出相似的染色模式。去污剂通透处理后未固定内皮细胞染色增强,表明D5G2与因细胞膜损伤而可及的细胞内层粘连蛋白结合蛋白结合。针对细胞损伤后暴露的细胞内靶点的抗体可能有助于将治疗剂锚定在血管损伤部位。

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