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Recombinant live attenuated foot-and-mouth disease (FMD) vaccine containing mutations in the L protein coding region

机译:在L蛋白编码区含有突变的重组减毒口蹄疫活疫苗

摘要

Previously we have identified a conserved domain (SAP, for SAF-A/B, Acinus, and PIAS) in the foot-and-mouth disease virus (FMDV) leader (L) protein coding region that is required for proper sub-cellular localization and function. Mutation of isoleucine 55 and leucine 58 to alanine (I55A, L58A) within the SAP domain resulted in a viable virus that displayed a mild attenuated phenotype in cell culture, along with altered sub-cellular distribution of L and failure to induce degradation of the transcription factor nuclear factor kappa-B. Here we report that inoculation of swine and cattle with this mutant virus results in the absence of clinical disease, the induction of a significant FMDV-specific neutralizing antibody response, and protection against subsequent homologous virus challenge. Remarkably, swine vaccinated with SAP mutant virus are protected against wild type virus challenge as early as two days post-vaccination suggesting that a strong innate as well as adaptive immunity is elicited. This variant could serve as the basis for construction of a live-attenuated FMD vaccine candidate.
机译:以前,我们已经在口蹄疫病毒(FMDV)前导(L)蛋白编码区中确定了保守结构域(SAP,用于SAF-A / B,Acinus和PIAS),这是正确进行亚细胞定位所必需的和功能。 SAP结构域中异亮氨酸55和亮氨酸58突变为丙氨酸(I55A,L58A)导致了一种活病毒,该病毒在细胞培养物中表现出轻度的减毒表型,同时改变了L的亚细胞分布,并且无法诱导转录降解核因子κB。在这里我们报告说,用这种突变病毒接种猪和牛会导致缺乏临床疾病,不会引起明显的FMDV特异性中和抗体反应,并能抵抗随后的同源病毒攻击。值得注意的是,接种SAP突变病毒的猪早在接种后两天就受到了针对野生型病毒攻击的保护,这表明它具有很强的先天免疫力和适应性免疫力。该变体可以用作构建减毒的FMD活疫苗候选物的基础。

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