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利用重组cDNA文库对人血管性血友病因子抑制性单克隆抗体进行表位作图。

Epitope mapping of inhibitory monoclonal antibodies to human von Willebrand factor by using recombinant cDNA libraries.

作者信息

Piétu G, Ribba A S, Chérel G, Siguret V, Obert B, Rouault C, Ginsburg D, Meyer D

机构信息

INSERM U. 143, Hôpital Bicêtre, Paris, France.

出版信息

Thromb Haemost. 1994 Jun;71(6):788-92.

PMID:7974349
Abstract

Two recombinant expression libraries containing small (300-600 base pairs) cDNA fragments of von Willebrand Factor (vWF) were screened in order to map the epitope of monoclonal antibodies (MAbs) to vWF. Among eleven MAbs tested, seven were effectively mapped. The epitopes of MAbs 418 and 522, which inhibit the binding of vWF to Factor VIII (FVIII), were localized between Leu 2 and Arg 53 and between Glu 35 and Ile 81 of the vWF subunit respectively, within the N-terminal trypsin fragment called SpIII-T4 [amino acids (aa) 1-272] which contains a binding domain for FVIII. The epitope of MAb 710, which inhibits the binding of vWF to glycoprotein Ib (GPIb), was identified between Ser 593 and Ser 678 on the tryptic 52/48 kDa fragment (aa 449-728) which contains binding domains for GPIb, collagen, heparin, sulfatides and subendothelium extracellular matrices. The epitope of MAb 723, which does not interfere with any known function of vWF, was localized between Ser 523 and Gly 588. The epitopes of MAb 505 and MAb 400, which inhibit the binding of vWF to collagen, were identified between Leu 927 and Arg 1114 within the SPI fragment (aa 911-1365) corresponding to the central part of the vWF subunit. The epitope of MAb 9, which inhibits the binding of vWF to GPIIb/IIIa, was identified in the C-terminal part of the vWF subunit between Gln 1704 and Asp 1746, the latter being the third aa of the RGD sequence common to adhesive proteins and serving as a recognition site for integrin receptors.

摘要

为了绘制针对血管性血友病因子(vWF)的单克隆抗体(MAb)的表位图谱,筛选了两个包含vWF小(300 - 600个碱基对)cDNA片段的重组表达文库。在测试的11种MAb中,7种被有效地绘制了图谱。抑制vWF与因子VIII(FVIII)结合的MAb 418和522的表位分别定位在vWF亚基的Leu 2和Arg 53之间以及Glu 35和Ile 81之间,位于称为SpIII - T4的N端胰蛋白酶片段[氨基酸(aa)1 - 272]内,该片段包含FVIII的结合结构域。抑制vWF与糖蛋白Ib(GPIb)结合的MAb 710的表位在胰蛋白酶52/48 kDa片段(aa 449 - 728)上的Ser 593和Ser 678之间被鉴定出来,该片段包含GPIb、胶原蛋白、肝素、硫脂和内皮下细胞外基质的结合结构域。不干扰vWF任何已知功能的MAb 723的表位定位在Ser 523和Gly 588之间。抑制vWF与胶原蛋白结合的MAb 505和MAb 400的表位在对应于vWF亚基中部的SPI片段(aa 911 - 1365)内的Leu 927和Arg 1114之间被鉴定出来。抑制vWF与GPIIb/IIIa结合的MAb 9的表位在vWF亚基的C端部分Gln 1704和Asp 1746之间被鉴定出来,后者是粘附蛋白共有的RGD序列的第三个氨基酸,作为整合素受体的识别位点。

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