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植物合成的大肠杆菌CFA/I菌毛蛋白可保护Caco-2细胞免受细菌附着。

Plant-synthesized E. coli CFA/I fimbrial protein protects Caco-2 cells from bacterial attachment.

作者信息

Lee Jin-Yong, Yu Jie, Henderson David, Langridge William H R

机构信息

Center for Molecular Biology and Gene Therapy, School of Medicine, 161, Mortensen Hall, Loma Linda University, Loma Linda CA, 92350, USA.

出版信息

Vaccine. 2004 Nov 25;23(2):222-31. doi: 10.1016/j.vaccine.2004.05.026.

Abstract

A DNA fragment encoding the cholera toxin A2 subunit (CTA2) linked to the enterotoxigenic Escherichia coli (ETEC) colony forming fimbrial antigen CFA/I was inserted into a plant expression vector containing the cholera toxin B subunit (CTB) fused to the rotavirus enterotoxin 22 amino acid epitope NSP422. Anti-CFA/I antibodies recognized a single band of approximately 72-kDa in transformed potato tuber tissue consistent with CFA/I-CTA2 and CTB-NSP4 fusion protein assembly into a cholera holotoxin-like structure. Enzyme-linked immunosorbent assay (GM1 ELISA) indicated that the CFA/I-CTA2 fusion protein bound specific GM1 ganglioside membrane receptors and made up approximately 0.002% of the total soluble tuber protein. Oral immunization of BALB/c mice with transformed tuber tissues generated anti-CFA/I serum and intestinal IgG and IgA secretory antibodies. Attachment of ETEC H10407 to enterocyte-like Caco-2 human colon carcinoma cells incubated with antiserum from immunized mice was reduced by 15% in comparison with Caco-2 cells incubated with serum from unimmunized mice. Immunogold staining of bacterial preparations revealed deposition of gold particles on E. coli H10407 fimbria incubated with immune serum but not on fimbria treated with sera from unimmunized mice demonstrating the specificity of antibodies in the immune serum for binding to CFA/I protein containing fimbria. The protection against toxic E. coli binding to Caco-2 cells generated by antisera from mice immunized with plant-synthesized CFA/I antigen demonstrates the feasibility of plant-based multi-component vaccine protection against enterotoxigenic E. coli, rotavirus and cholera, three enteric diseases that together exert the highest levels of child morbidity and mortality in economically emerging countries.

摘要

将编码霍乱毒素A2亚基(CTA2)并与产肠毒素大肠杆菌(ETEC)菌毛抗原CFA/I相连的DNA片段插入到一个植物表达载体中,该载体含有与轮状病毒肠毒素22个氨基酸表位NSP422融合的霍乱毒素B亚基(CTB)。抗CFA/I抗体在转化的马铃薯块茎组织中识别出一条约72 kDa的单带,这与CFA/I-CTA2和CTB-NSP4融合蛋白组装成霍乱全毒素样结构一致。酶联免疫吸附测定(GM1 ELISA)表明,CFA/I-CTA2融合蛋白结合特异性GM1神经节苷脂膜受体,约占块茎总可溶性蛋白的0.002%。用转化的块茎组织对BALB/c小鼠进行口服免疫,产生了抗CFA/I血清以及肠道IgG和IgA分泌抗体。与用未免疫小鼠血清孵育的Caco-2细胞相比,用免疫小鼠抗血清孵育的ETEC H10407对肠上皮样Caco-2人结肠癌细胞的黏附减少了15%。细菌制剂的免疫金染色显示,金颗粒沉积在用免疫血清孵育的大肠杆菌H10407菌毛上,而在用未免疫小鼠血清处理的菌毛上则没有,这证明了免疫血清中抗体与含CFA/I蛋白菌毛结合的特异性。用植物合成的CFA/I抗原免疫小鼠产生的抗血清对有毒大肠杆菌与Caco-2细胞结合的保护作用,证明了基于植物的多组分疫苗预防产肠毒素大肠杆菌、轮状病毒和霍乱这三种肠道疾病的可行性,在经济新兴国家,这三种肠道疾病共同导致儿童发病率和死亡率居高不下。

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