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[CTB-PROIN融合基因的克隆及其在大肠杆菌中的表达]

[Cloning of CTB-PROIN fusion gene and its expression in Escherichia coli].

作者信息

Chen Li, Ouyang Feng-Xiu, Qian Bing-Jun, Ren Hong, Wang Qiang, Jiang Qing-Wu, Wang Yu-Jiong, Liu Jing-Bo, Liang Wan-Qi, Zhang Da-Bing

机构信息

Life Science School of Ningxia University, Yinchuan 750021, China.

出版信息

Sheng Wu Gong Cheng Xue Bao. 2005 Mar;21(2):204-10.

Abstract

A fusion gene CTB-PROIN, in which Proinsulin gene was fused to the 3' end of CTB gene by a hinge peptide 'GPGP', was constructed and cloned into pET-30a(+) to obtain a prokaryotic expression vector pETCPI. Subsequently the recombinant plasmid pETCPI was transformed into E. coli stain BL21 (DE3). After induced by IPTG, the expression product was analyzed by sodium dodecyl sulphate-polyacrylamide gel (15%) electrophoresis (SDS-PAGE), and its result indicated that the recombinant protein CTB-PROIN was expressed and accumulated as inclusion bodies. The recombinant CTB-PROIN protein accumulated to the level of 25% of total bacterial proteins. After inclusion bodies was denaturalized and refolded in vitro, significant assembly of monomers had occurred, and the recombinant protein represented assembled pentamers. The results of western blotting analysis also demonstrated that the fusion protein could be recognized by the anti-CT and anti-insulin antibody, respectively. In addition, the result of the CTB-PROIN-GM1 binding assay, that the protein could bind to monosialoganglioside specifically, showed it possesed biological activity in vitro. These results provided the possibility of developing a cheaper and more efficient oral vaccine for type I diabetes using such constructs.

摘要

构建了一种融合基因CTB-PROIN,其中胰岛素原基因通过铰链肽“GPGP”与CTB基因的3'端融合,并克隆到pET-30a(+)中以获得原核表达载体pETCPI。随后将重组质粒pETCPI转化到大肠杆菌BL21(DE3)菌株中。经IPTG诱导后,通过十二烷基硫酸钠-聚丙烯酰胺凝胶(15%)电泳(SDS-PAGE)分析表达产物,结果表明重组蛋白CTB-PROIN以包涵体形式表达并积累。重组CTB-PROIN蛋白积累至细菌总蛋白的25%水平。包涵体经体外变性和复性后,单体发生了显著组装,重组蛋白呈现组装的五聚体形式。蛋白质印迹分析结果还表明,融合蛋白可分别被抗CT和抗胰岛素抗体识别。此外,CTB-PROIN-GM1结合试验结果表明该蛋白能特异性结合单唾液酸神经节苷脂,表明其在体外具有生物学活性。这些结果为使用此类构建体开发更便宜、更有效的I型糖尿病口服疫苗提供了可能性。

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