首页> 外文期刊>Infection and immunity >Construction, Characterization, and Immunogenicity of an Attenuated Salmonella enterica Serovar Typhimurium pgtE Vaccine Expressing Fimbriae with Integrated Viral Epitopes from the spiC Promoter
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Construction, Characterization, and Immunogenicity of an Attenuated Salmonella enterica Serovar Typhimurium pgtE Vaccine Expressing Fimbriae with Integrated Viral Epitopes from the spiC Promoter

机译:spiC启动子整合菌抗原决定簇表达菌毛的减毒小肠沙门氏菌鼠伤寒沙门氏菌pgtE疫苗的构建,表征和免疫原性

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Transmissible gastroenteritis virus (TGEV) is a porcine coronavirus that causes diarrhea, leading to near 100% mortality in neonatal piglets with corresponding devastating economic consequences. For the protection of neonatal and older animals, oral live vaccines present the attractive property of inducing desired mucosal immune responses, including colostral antibodies in sows—an effective means to passively protect suckling piglets. Newly attenuated Salmonella vaccine constructs expressing TGEV S protein epitopes were studied and evaluated for improved humoral immune response to TGEV. The macrophage-inducible Salmonella ssaH and spiC/ssaB promoters were compared for their ability to express the TGEV C and A epitopes in the context of the heterologous 987P fimbriae on Salmonella vaccines. Compared to the ssaH promoter, the Salmonella cya crp vector elicited significantly higher levels of mucosal and systemic antibodies in orally immunized mice when the chimeric fimbriae were expressed from the spiC promoter. The Salmonella spiC promoter construct induced the highest level of chimeric fimbriae after being taken up by the J774A.1 macrophagelike cells. The Salmonella cya crp vaccine vector was shown to incorporate into 987P partially degraded chimeric subunits lacking the TGEV epitopes. In contrast, its isogenic pgtE mutant produced fimbriae consisting exclusively of intact chimeric subunits. Mice immunized orally with the Salmonella pgtE vaccine expressing chimeric fimbriae from the spiC promoter elicited significantly higher systemic and mucosal antibody titers against the TGEV epitopes compared to the parental vaccine. This study indicates that the Salmonella cya crp pgtE vector and the spiC promoter can be used successfully to improve immune responses toward heterologous antigens.
机译:传染性胃肠炎病毒(TGEV)是一种猪冠状病毒,会引起腹泻,导致新生仔猪的死亡率接近100%,并带来严重的经济后果。为了保护新生儿和大龄动物,口服活疫苗具有诱导所需粘膜免疫反应(包括母猪中的初乳抗体)的吸引力,这是被动保护乳猪的有效手段。研究了新的减毒的表达TGEV S蛋白表位的 Salmonella 疫苗构建体,并评估了其对TGEV的体液免疫应答的改善。比较了巨噬细胞诱导的沙门氏菌ssaH spiC / ssaB 启动子在上异源987P菌毛中表达TGEV C和A表位的能力。沙门氏菌疫苗。与 ssaH 启动子相比,当 spiC表达嵌合菌毛时,沙门氏菌cya crp 载体在口服免疫小鼠中引起的粘膜和全身抗体水平明显升高。 启动子。沙门氏菌spiC 启动子构建体在被J774A.1巨噬细胞样细胞摄取后,诱导了最高水平的嵌合菌毛。已显示沙门氏菌Cya crp 疫苗载体可整合到缺少TGEV表位的987P部分降解的嵌合亚基中。相反,其同基因的 pgtE 突变体产生的菌毛完全由完整的嵌合亚基组成。与表达疫苗的小鼠相比,用表达来自 spiC 启动子的嵌合菌毛的沙门氏菌pgtE 疫苗口服免疫的小鼠对TGEV表位的全身和粘膜抗体滴度明显更高。这项研究表明,沙门氏菌crp pgtE 载体和 spiC 启动子可以成功用于改善对异源抗原的免疫反应。

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