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在NS1蛋白初免-口服重组沙门氏菌疫苗加强免疫后,两性霉素B增强免疫反应可保护小鼠免受登革病毒攻击。

Enhanced immune response by amphotericin B following NS1 protein prime-oral recombinant Salmonella vaccine boost vaccination protects mice from dengue virus challenge.

作者信息

Liu Wen-Tssann, Lin Wei-Ting, Tsai Chung-Chin, Chuang Chuan-Chang, Liao Chin-Len, Lin Huang-Chi, Hung Yao-Wen, Huang Shih-Shiung, Liang Chung-Chih, Hsu Hui-Ling, Wang Hsian-Jenn, Liu Yu-Tien

机构信息

Institute of Preventive Medicine, National Defense Medical Center, P.O. Box 90048-505, Neihu, Taipei, Taiwan.

出版信息

Vaccine. 2006 Jul 26;24(31-32):5852-61. doi: 10.1016/j.vaccine.2006.04.066. Epub 2006 May 16.

DOI:10.1016/j.vaccine.2006.04.066
PMID:16759760
Abstract

A recombinant vaccine strain SL3261/pLT105 of attenuated aroA Salmonella enterica serovar Typhimurium SL3261 strain expressing a secreted dengue virus type 2 non-structural NS1 and Yersinia pestis F1 (Caf1) fusion protein, rNS1:Caf1, was generated. Immunological evaluation was performed by prime-boost vaccine regimen. Oral immunization of mice with 1 x 10(9)cfu of SL3261/pLT105 only induced low levels of NS1-specific antibody response and protective immunity following dengue virus challenge. The parenteral NS1 protein priming-oral Salmonella boosting protocol enhanced both NS1-specific serum IgG response and protective efficacy as compared to mice immunized with each type vaccine alone. Addition of an antifungal antibiotic amphotericin B (AmB) to Salmonella vaccine further enhanced the synergic effects of prime-boost vaccine regimen on the elicited NS1-specific serum IgG response and the protective efficacy. Together, the results demonstrated that the rNS1:Caf1 producing Salmonella SL3261/pLT105 strain fails to provide effective protection as an oral vaccine alone despite co-administration of AmB as an adjuvant capable of enhancing the immune responses, and moreover, the protein priming-oral Salmonella vaccine boosting approach in combination with AmB as an immunization regimen may have the potential to be further explored as an alternative approach for dengue vaccine development.

摘要

构建了一种重组疫苗菌株,即减毒的鼠伤寒沙门氏菌肠炎血清型鼠伤寒杆菌SL3261菌株SL3261/pLT105,其表达分泌型登革病毒2型非结构NS1和鼠疫耶尔森菌F1(Caf1)融合蛋白rNS1:Caf1。通过初免-加强疫苗方案进行免疫评估。用1×10⁹ cfu的SL3261/pLT105口服免疫小鼠,在登革病毒攻击后仅诱导低水平的NS1特异性抗体反应和保护性免疫。与单独用每种疫苗免疫的小鼠相比,肠外NS1蛋白初免-口服沙门氏菌加强方案增强了NS1特异性血清IgG反应和保护效果。向沙门氏菌疫苗中添加抗真菌抗生素两性霉素B(AmB)进一步增强了初免-加强疫苗方案对诱导的NS1特异性血清IgG反应和保护效果的协同作用。总之,结果表明,尽管联合使用AmB作为能够增强免疫反应的佐剂,但产生rNS1:Caf1的沙门氏菌SL3261/pLT105菌株单独作为口服疫苗不能提供有效的保护,此外,蛋白初免-口服沙门氏菌疫苗加强方法与AmB作为免疫方案可能有潜力作为登革热疫苗开发的替代方法进一步探索。

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