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Expression of Avian Influenza Virus (H5N1) Hemagglutinin and Matrix Protein 1 in Pichia pastoris and Evaluation of their Immunogenicity in Mice

机译:禽流感病毒(H5N1)血凝素和基质蛋白1在毕赤酵母中的表达及其在小鼠中的免疫原性评价

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The conventional avian influenza vaccines rely on development of neutralizing antibodies against the HA and NA antigens. However, these antigens are highly variable, and hence there is a need for better vaccine candidates which would offer broader protection in animals. The M1 of avian influenza is another major structural protein that has conserved epitopes that are reported to induce CD8+ T cells and can contribute to protection against morbidity and mortality from influenza. Hence in an effort to study the immune response of rM1 either alone or in combination with rHA, the hemagglutinin (HA) and matrix protein (M1) of A/Hatay/2004/H5N1 strain of avian influenza were expressed in Pichia pastoris as his-tagged proteins and purified through Ni-NTA chromatography. The His-tag was removed using TEV protease cleavage site and the immunogenicity of purified rHA and rM1 either alone or in combination was determined in mice. One group of mice was immunized with 5 μg of purified rHA, the other group was immunized with rM1, and a third group of mice were immunized with 5 μg of rHA and rM1. All the animals were boosted twice, once on 28 days postimmunization (dpi) and the second on 42 dpi. The immune response was evaluated by enzyme-linked immunosorbent assay (ELISA) and hemagglutination inhibition (HI) assay. The group of mice immunized with rHA and rM1 together showed significantly higher immune response against rHA and rM1 than mice immunized with either HA or M1 antigens. The addition of rM1 with rHA resulted in increased HI titer in animals immunized with both the antigens. These results suggest that the HA and M1 expressed in P. pastoris can be utilized in combination for the development of faster and cost-effective vaccines for circulating and newer strains of avian influenza and would aid in combating the disease in a pandemic situation, in which production time matters greatly.
机译:常规禽流感疫苗依赖于针对HA和NA抗原的中和抗体的开发。然而,这些抗原是高度可变的,因此需要在动物中提供更广泛保护的更好的候选疫苗。禽流感的M1是另一种主要的结构蛋白,具有保守的表位,据报道可诱导CD8 + T细胞,并有助于预防流感的发病和死亡。因此,为了研究rM1单独或与rHA结合使用的免疫反应,禽流感A / Hatay / 2004 / H5N1菌株的血凝素(HA)和基质蛋白(M1)在毕赤酵母中表达为his-标记的蛋白质,并通过Ni-NTA色谱纯化。使用TEV蛋白酶切割位点去除His-tag,并在小鼠中测定纯化的rHA和rM1的免疫原性(单独或组合使用)。一组小鼠用5μg纯化的rHA免疫,另一组小鼠用rM1免疫,第三组小鼠用5μgrHA和rM1免疫。将所有动物加强免疫两次,一次在免疫后28天(dpi),第二次在42 dpi。通过酶联免疫吸附测定(ELISA)和血凝抑制(HI)测定评估免疫应答。用rHA和rM1一起免疫的小鼠组显示出比用HA或M1抗原免疫的小鼠明显更高的针对rHA和rM1的免疫反应。在rHA和rHA中添加rM1导致用两种抗原免疫的动物的HI滴度增加。这些结果表明,在巴斯德毕赤酵母中表达的HA和M1可组合用于开发更快和更具成本效益的疫苗,用于循环和更新的禽流感毒株,并有助于在大流行情况下与该疾病作斗争。生产时间非常重要。

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