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重组蛋白 Sm29 的复性,是生产血吸虫病候选疫苗的一个步骤。

Refolding of the recombinant protein Sm29, a step toward the production of the vaccine candidate against schistosomiasis.

机构信息

Centro de Biotecnologia, Instituto Pesquisas Energéticas e Nucleares, São Paulo, SP, Brazil.

出版信息

J Biotechnol. 2013 Dec;168(4):511-9. doi: 10.1016/j.jbiotec.2013.09.017. Epub 2013 Sep 29.

Abstract

Schistosomiasis is an important parasitic disease, with about 240 million people infected worldwide. Humans and animals can be infected, imposing an enormous social and economic burden. The only drug available for chemotherapy, praziquantel, does not control reinfections, and an efficient vaccine for prophylaxis is still missing. However, the tegumental protein Sm29 of Schistosoma mansoni was shown to be a promising antigen to compose an anti-schistosomiasis vaccine. Though, recombinant Sm29 is expressed in Escherichia coli as insoluble inclusion bodies requiring an efficient process of refolding, thus, hampering its production in large scale. We present in this work studies to refold the recombinant Sm29 using high hydrostatic pressure, a mild condition to dissociate aggregated proteins, leading to refolding on a soluble conformation. Our studies resulted in high yield of rSm29 (73%) as a stably soluble and structured protein. The refolded antigen presented protective effect against S. mansoni development in immunized mice. We concluded that the refolding process by application of high hydrostatic pressure succeeded, and the procedure can be scaled-up, allowing industrial production of Sm29.

摘要

血吸虫病是一种重要的寄生虫病,全球约有 2.4 亿人感染。人类和动物都可能受到感染,给社会和经济带来巨大负担。唯一可用的化疗药物吡喹酮不能控制再感染,而有效的预防疫苗仍未出现。然而,曼氏血吸虫的表皮蛋白 Sm29 被证明是一种很有前途的抗原,可以用来制备抗血吸虫病疫苗。尽管如此,重组 Sm29 在大肠杆菌中表达为不溶性包涵体,需要有效的复性过程,因此限制了其大规模生产。在这项工作中,我们研究了使用高压(一种温和的条件,可以使聚集的蛋白质解离)来复性重组 Sm29,从而使其折叠成可溶的构象。我们的研究结果表明,rSm29(73%)的产量很高,是一种稳定可溶性和结构蛋白。该复性抗原在免疫小鼠中对曼氏血吸虫的发育具有保护作用。我们得出结论,应用高压的复性过程是成功的,并且该过程可以扩大规模,允许 Sm29 的工业化生产。

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