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硕大利什曼原虫:重组糖蛋白63的产生、其在小鼠中的抗原性和免疫原性

Leishmania major: production of recombinant gp63, its antigenicity and immunogenicity in mice.

作者信息

Handman E, Button L L, McMaster R W

机构信息

Walter and Eliza Hall Institute of Medical Research, Royal Melbourne Hospital, Victoria, Australia.

出版信息

Exp Parasitol. 1990 May;70(4):427-35. doi: 10.1016/0014-4894(90)90127-x.

Abstract

The Mr 63,000 membrane polypeptide (gp63) is one of the Leishmania receptors for host macrophages and has been shown to protect mice from infection. The gene encoding gp63, the major Mr 63,000 surface glycoprotein of L. major promastigotes, has been expressed as a fusion protein with the enzyme glutathione S- transferase encoded by the parasitic helminth Schistosoma japonicum. This fusion protein was recognized by polyclonal antibodies to the native Leishmania gp63 polypeptide. The insoluble gp63 fusion protein was purified by SDS-PAGE and electroelution and was used to raise antibodies in rabbits. These rabbit anti-gp63 antibodies recognized the fusion protein and the denatured parasite gp63 on immunoblots and by immunofluorescence on fixed promastigotes, but did not recognize the native molecule on live organisms. However, antibodies raised against native promastigote glycoproteins, affinity purified on solid-phase gp63 fusion protein, recognized both native and denatured gp63, suggesting the presence of native determinants in the recombinant protein. The gp63 fusion protein did not protect mice of either healer or nonhealer phenotype from challenge infection with live promatigotes. The implications of these results for the engineering of recombinant DNA-produced molecular vaccines are discussed.

摘要

分子量为63000的膜多肽(gp63)是利什曼原虫宿主巨噬细胞的受体之一,已证明其可保护小鼠免受感染。编码gp63的基因,即硕大利什曼原虫前鞭毛体主要的分子量为63000的表面糖蛋白,已与日本血吸虫编码的谷胱甘肽S -转移酶融合表达为融合蛋白。该融合蛋白可被针对天然利什曼原虫gp63多肽的多克隆抗体识别。不溶性gp63融合蛋白通过SDS - PAGE和电洗脱进行纯化,并用于在兔体内产生抗体。这些兔抗gp63抗体在免疫印迹上以及通过对固定前鞭毛体的免疫荧光识别融合蛋白和变性的寄生虫gp63,但不能识别活生物体上的天然分子。然而,针对天然前鞭毛体糖蛋白产生的抗体,经固相gp63融合蛋白亲和纯化后,可识别天然和变性的gp63,这表明重组蛋白中存在天然决定簇。gp63融合蛋白不能保护愈合型或非愈合型表型的小鼠免受活前鞭毛体的攻击感染。讨论了这些结果对重组DNA生产的分子疫苗工程的意义。

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