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A Poly-N-acetylglucosamine-Shiga toxin broad-spectrum conjugate vaccine for Shiga toxin-producing Escherichia coli.

机译:一种用于产生志贺毒素的大肠杆菌的聚-N-乙酰氨基葡糖-志贺毒素广谱结合疫苗。

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摘要

Many pathogens produce the β-(1-6)-linked poly-N-acetylglucosamine (PNAG) surface polysaccharide that is being developed as a broadly protective antimicrobial vaccine. However, it is unknown whether systemically injected PNAG vaccines or antibodies would provide protective immunity against pathogens confined to the gastrointestinal tract such as Shiga toxin (Stx)-producing Escherichia coli (STEC), an important group of gastrointestinal (GI) pathogens for which effective immunotherapeutics are lacking. To ascertain whether systemic IgG antibody to PNAG impacts this infectious situation, a vaccine consisting of a synthetic nonamer of nonacetylated PNAG, 9GlcNH2, conjugated to the Shiga toxin 1b subunit (9GlcNH2-Stx1b) was produced. Rabbit antibodies raised to the conjugate vaccine were tested for bacterial killing and toxin neutralization in vitro and protection against infection in infant mice. Cell surface PNAG was detected on all 9 STEC isolates tested, representing 6 STEC serogroups, including E. coli O157:H7. Antibody to the 9GlcNH2-Stx1b conjugate neutralized Stx1 potently and Stx2 modestly. For O157:H7 and O104:H4 STEC strains, antibodies elicited by the 9GlcNH2-Stx1b conjugate possessed opsonic killing and bactericidal activity. Following intraperitoneal injection, antibodies to both PNAG and Stx were needed for infant mouse protection against O157 STEC. These antibodies also mediated protection against the Stx2-producing O104:H4 strain that was the cause of a recent outbreak in Germany, although sufficient doses of antibody to PNAG alone were protective against this strain in infant mice. Our observations suggest that vaccination against both PNAG and Stx, using a construct such as the 9GlcNH2-Stx1b conjugate vaccine, would be protective against a broad range of STEC serogroups. IMPORTANCE The presence of poly-N-acetylglucosamine (PNAG) on many pathogens presents an opportunity to target this one structure with a multispecies vaccine. Whether antibodies to PNAG can protect against pathogens confined to the gastrointestinal tract is not known. As Shiga toxin (Stx)-producing Escherichia coli (STEC) bacteria are serious causes of infection whose virulence is dependent on elaboration of Stx, we prepared a vaccine containing a synthetic nonamer of PNAG (9GlcNH2) conjugated to Shiga toxin 1b subunit (9GlcNH2-Stx1b) to evaluate bacterial killing, toxin neutralization, and protective efficacy in infant mice. All nine (100%) clinical strains of STEC from different serogroups expressed PNAG. Vaccine-induced antibody mediated in vitro killing of STEC and neutralization of both Stx1 and Stx2. Passive administration of antibody to the conjugate showed protection requiring immunity to both PNAG and Stx for O157 strains, although for an O104 strain, antibody to PNAG alone was protective. Immunity to PNAG may contribute to protection against STEC infections.
机译:许多病原体会产生β-(1-6)-连接的聚N-乙酰氨基葡糖(PNAG)表面多糖,这种多糖正被开发为具有广泛保护性的抗菌疫苗。但是,尚不知道全身注射的PNAG疫苗或抗体是否能提供针对胃肠道病原体(例如产生志贺毒素(Stx)的大肠杆菌(STEC))的保护性免疫力,这是重要的胃肠道病原体组,对其有效缺乏免疫疗法。为了确定针对PNAG的全身性IgG抗体是否会影响这种感染情况,生产了一种疫苗,该疫苗由与志贺毒素1b亚基(9GlcNH2-Stx1b)偶联的非乙酰化PNAG的合成九聚体9GlcNH2组成。测试了针对缀合物疫苗的兔抗体的体外细菌杀灭和毒素中和以及对婴儿小鼠的感染防护。在所有9个STEC分离株中检测到细胞表面PNAG,代表6个STEC血清群,包括大肠杆菌O157:H7。 9GlcNH2-Stx1b共轭物抗体有效中和Stx1,并适度中和Stx2。对于O157:H7和O104:H4 STEC菌株,由9GlcNH2-Stx1b共轭物引发的抗体具有调理性杀灭和杀菌活性。腹膜内注射后,需要针对PNAG和Stx的抗体来保护O157 STEC的婴儿小鼠。这些抗体还介导了针对产生Stx2的O104:H4菌株的保护,这是德国最近爆发的原因,尽管仅足够剂量的PNAG抗体在婴儿小鼠中可以抵抗该菌株。我们的观察结果表明,使用9GlcNH2-Stx1b共轭疫苗等构建体针对PNAG和Stx进行疫苗接种将对广泛的STEC血清群具有保护作用。重要事项许多病原体上都存在聚N-乙酰氨基葡萄糖(PNAG),这提供了使用多种疫苗针对这种结构的机会。 PNAG的抗体是否能抵抗局限于胃肠道的病原体尚不清楚。由于产生志贺毒素(Stx)的大肠杆菌(STEC)细菌是严重的感染原因,其毒力取决于Stx的加工,因此我们制备了一种疫苗,该疫苗包含与志贺毒素1b亚基(9GlcNH2-)结合的PNAG(9GlcNH2)合成九聚体。 Stx1b)评估婴儿小鼠的细菌杀灭,毒素中和和保护功效。来自不同血清群的所有九种(100%)STEC临床菌株均表达PNAG。疫苗诱导的抗体介导STEC的体外杀伤和Stx1和Stx2的中和。抗体对缀合物的被动给药显示出对O157菌株需要同时对PNAG和Stx免疫的保护作用,尽管对于O104菌株,仅针对PNAG的抗体具有保护作用。 PNAG的免疫力可能有助于预防STEC感染。

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