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首页> 外文期刊>Virology Journal >Multiple linear B-cell epitopes of classical swine fever virus glycoprotein E2 expressed in E.coli as multiple epitope vaccine induces a protective immune response
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Multiple linear B-cell epitopes of classical swine fever virus glycoprotein E2 expressed in E.coli as multiple epitope vaccine induces a protective immune response

机译:在大肠杆菌中表达的经典猪瘟病毒糖蛋白E2的多个线性B细胞表位,因为多个表位疫苗诱导保护性免疫应答

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摘要

Classical swine fever is a highly contagious disease of swine caused by classical swine fever virus, an OIE list A pathogen. Epitope-based vaccines is one of the current focuses in the development of new vaccines against classical swine fever virus (CSFV). Two B-cell linear epitopes rE2-ba from the E2 glycoprotein of CSFV, rE2-a (CFRREKPFPHRMDCVTTTVENED, aa844-865) and rE2-b (CKEDYRYAISSTNEIGLLGAGGLT, aa693-716), were constructed and heterologously expressed in Escherichia coli as multiple epitope vaccine. Fifteen 6-week-old specified-pathogen-free (SPF) piglets were intramuscularly immunized with epitopes twice at 2-week intervals. All epitope-vaccinated pigs could mount an anamnestic response after booster vaccination with neutralizing antibody titers ranging from 1:16 to 1:256. At this time, the pigs were subjected to challenge infection with a dose of 1 × 106 TCID50 virulent CSFV strain. After challenge infection, all of the rE2-ba-immunized pigs were alive and without symptoms or signs of CSF. In contrast, the control pigs continuously exhibited signs of CSF and had to be euthanized because of severe clinical symptoms at 5 days post challenge infection. The data from in vivo experiments shown that the multiple epitope rE2-ba shown a greater protection (similar to that of HCLV vaccine) than that of mono-epitope peptide(rE2-a or rE2-b). Therefore, The results demonstrated that this multiple epitope peptide expressed in a prokaryotic system can be used as a potential DIVA (differentiating infected from vaccinated animals) vaccine. The E.coli-expressed E2 multiple B-cell linear epitopes retains correct immunogenicity and is able to induce a protective immune response against CSFV infection.
机译:古典猪瘟是由猪瘟病毒引起的高度传染性疾病,它是OIE列出的一种病原体。基于表位的疫苗是针对经典猪瘟病毒(CSFV)的新疫苗开发中的当前重点之一。构建了来自CSFV E2糖蛋白的两个B细胞线性表位rE2-ba,rE2-a(CFRREKPFPHRMDCVTTTVENED,aa844-865)和rE2-b(CKEDYRYAISSTNEIGLLGAGGLT,aa693-716),并在大肠杆菌中作为多种表位疫苗异源表达。 15个6周龄的无指定病原(SPF)仔猪以2周间隔两次肌内免疫表位免疫。加强免疫接种后,所有抗原表位疫苗接种的猪都可产生记忆消除反应,中和抗体滴度范围为1:16至1:256。此时,将猪用1×10 6 TCID 50 强毒CSFV株进行激发感染。激发感染后,所有接受rE2-ba免疫的猪都活着,没有CSF症状或体征。相反,对照猪在激发感染后5天由于严重的临床症状而连续表现出CSF的迹象并且必须被安乐死。体内实验数据表明,多个表位rE2-ba比单表位肽(rE2-a或rE2-b)具有更好的保护作用(类似于HCLV疫苗)。因此,该结果证明了在原核系统中表达的这种多表位肽可以用作潜在的DIVA(从疫苗接种的动物中分化感染)疫苗。大肠杆菌表达的E2多个B细胞线性表位保留正确的免疫原性,并能够诱导针对CSFV感染的保护性免疫应答。

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