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基于表达异源抗原的杂交沙门氏菌的抗产肠毒素细菌病原体疫苗。

Vaccines against enterotoxigenic bacterial pathogens based on hybrid Salmonella that express heterologous antigens.

作者信息

Clements J D, Cárdenas L

机构信息

Department of Microbiology and Immunology, Tulane University School of Medicine, New Orleans, LA 70112.

出版信息

Res Microbiol. 1990 Sep-Oct;141(7-8):981-93. doi: 10.1016/0923-2508(90)90138-g.

Abstract

In this report, we examine two aspects in the development of a vaccine against enterotoxigenic bacterial pathogens based on hybrid Salmonella that express heterologous antigens. First, we describe the construction of a non-toxic fusion peptide for immunization against Escherichia coli that produce heat-labile (LT) and heat-stable (ST) enterotoxins. For that construction, the 5' terminus of the gene coding for ST was fused to the 3' terminus of the gene coding for the binding subunit of LT(LT-B). The ST gene was constructed synthetically with appropriate restriction sites to permit in-frame, downstream insertion. Maximum expression of ST antigenicity was obtained when a seven-amino-acid proline-containing linker was included between the LT-B and ST moieties. The purified LT-B/ST fusion peptide consisted of a single polypeptide chain with an apparent molecular weight of 18,000. The LT-B/ST fusion peptide was non-toxic and immunologic determinants of both LT and ST were recognized by antibodies directed against the native toxins. Animals immunized with either crude or purified preparations containing the hybrid molecule produced antibodies that were able to recognize native toxin in vitro. Significantly, these antibodies were able to neutralize the biological activity of native ST. The second aspect reported here examines a mechanism for stabilizing expression of heterologous antigens in attenuated Salmonella mutants by integration of the heterologous gene (LT-B) into the chromosome of the carrier. A comparative in vitro study of the levels of expression of LT-B between the cointegrate strain and an isogenic strain carrying the LT-B gene on a multicopy plasmid demonstrated that the initial levels of expression of both strains is similar, that the plasmid-carrying strain loses the ability to express the heterologous antigen very quickly and that the cointegrate continues to maintain and express the antigen without the requirement for a stabilizing antibiotic.

摘要

在本报告中,我们研究了基于表达异源抗原的杂交沙门氏菌开发抗产肠毒素细菌病原体疫苗的两个方面。首先,我们描述了一种用于免疫产热不稳定(LT)和热稳定(ST)肠毒素的大肠杆菌的无毒融合肽的构建。为此构建,编码ST的基因的5'末端与编码LT结合亚基(LT-B)的基因的3'末端融合。ST基因通过合适的限制性位点合成构建,以允许框内下游插入。当在LT-B和ST部分之间包含含七个氨基酸的脯氨酸连接子时,获得了ST抗原性的最大表达。纯化的LT-B/ST融合肽由一条表观分子量为18,000的单多肽链组成。LT-B/ST融合肽无毒,针对天然毒素的抗体可识别LT和ST的免疫决定簇。用含有杂交分子的粗制品或纯化制品免疫的动物产生的抗体能够在体外识别天然毒素。重要的是,这些抗体能够中和天然ST的生物活性。本文报道的第二个方面研究了通过将异源基因(LT-B)整合到载体染色体中来稳定减毒沙门氏菌突变体中异源抗原表达的机制。对共整合菌株和携带多拷贝质粒上LT-B基因的同基因菌株之间LT-B表达水平的体外比较研究表明,两种菌株的初始表达水平相似,携带质粒的菌株很快失去表达异源抗原的能力,而共整合菌株继续维持并表达抗原,无需使用稳定抗生素。

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