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基于 ASD 的减毒迟钝爱德华氏菌的平衡致死系统表达一种异源抗原用于多价细菌疫苗。

Asd-based balanced-lethal system in attenuated Edwardsiella tarda to express a heterologous antigen for a multivalent bacterial vaccine.

机构信息

State Key Laboratory of Bioreactor Engineering, East China University of Science and Technology, 130 Meilong Rd., Shanghai 200237, PR China.

出版信息

Fish Shellfish Immunol. 2013 May;34(5):1188-94. doi: 10.1016/j.fsi.2013.01.027. Epub 2013 Feb 27.

DOI:10.1016/j.fsi.2013.01.027
PMID:23454428
Abstract

Edwardsiella tarda is an enteric Gram-negative invasive intracellular pathogen, which causes enteric septicemia in fish. It could be potentially used to develop a recombinant attenuated E. tarda vaccine for the aquaculture industry. Because live vaccine strains can potentially be released into the environment upon vaccination, medical and environmental safety issues must be considered. Deletion of the asdB gene in E. tarda resulted in a diaminopimelic acid (DAP)-dependent mutant. The wild type asdB gene was inserted in place of the antibiotic-resistance gene in the plasmid, and the resultant non-antibiotic resistant vector was transformed into the attenuated and DAP-dependent E. tarda vaccine strain (WEDΔasdB) to obtain a balanced-lethal system for heterologous antigen expression. The balanced-lethal expression system was further optimized by comparing plasmid replicons with different Shine-Dalgarno sequences and start codons for the asdB gene. Utilizing the optimized balanced-lethal expression system, the protective antigen gene gapA34 from the fish pathogen Aeromonas hydrophila LSA34 was expressed in the attenuated E. tarda to generate the multivalent vaccine candidate WEDΔasdB/pUTta4DGap. This vaccine was shown to evoke an effective immune response against both E. tarda and A. hydrophila LSA34 by vaccinating turbot via a simple immersion route. This multivalent E. tarda vector vaccine has great potential for broad applications in aquaculture.

摘要

迟缓爱德华氏菌是一种肠道革兰氏阴性侵袭性细胞内病原体,可引起鱼类肠道败血症。它有可能被开发为水产养殖业的重组减毒迟缓爱德华氏菌疫苗。由于活疫苗株在接种后可能会释放到环境中,因此必须考虑医疗和环境安全问题。迟缓爱德华氏菌中 asdB 基因的缺失导致二氨基庚二酸(DAP)依赖性突变体。将野生型 asdB 基因插入质粒中的抗生素抗性基因位置,并用非抗生素抗性载体转化减毒和 DAP 依赖性迟缓爱德华氏菌疫苗株(WEDΔasdB),以获得用于异源抗原表达的平衡致死系统。通过比较不同 Shine-Dalgarno 序列和 asdB 基因起始密码子的质粒复制子,进一步优化了平衡致死表达系统。利用优化的平衡致死表达系统,在减毒迟缓爱德华氏菌中表达了来自鱼类病原体嗜水气单胞菌 LSA34 的保护性抗原基因 gapA34,生成了多价疫苗候选物 WEDΔasdB/pUTta4DGap。通过简单的浸泡途径给大菱鲆接种该疫苗,证明它能有效针对迟缓爱德华氏菌和嗜水气单胞菌 LSA34 产生免疫应答。这种多价迟缓爱德华氏菌载体疫苗在水产养殖中有广泛应用的巨大潜力。

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