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首页> 外文期刊>EBioMedicine >Immunotherapy With the PreS-based Grass Pollen Allergy Vaccine BM32 Induces Antibody Responses Protecting Against Hepatitis B Infection
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Immunotherapy With the PreS-based Grass Pollen Allergy Vaccine BM32 Induces Antibody Responses Protecting Against Hepatitis B Infection

机译:基于PreS的草花粉过敏疫苗BM32的免疫疗法可诱导抗体反应,预防乙型肝炎感染。

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Background: We have constructed and clinically evaluated a hypoallergenic vaccine for grass pollen allergy, BM32, which is based on fusion proteins consisting of peptides from the IgE binding sites of the major grass pollen allergens fused to preS (preS1+preS2), a domain of the hepatitis B virus (HBV) large envelope protein which mediates the viral attachment and entry. Aim of this study was the characterization of the HBV-specific immune response induced by vaccination of allergic patients with BM32 and the investigation of the vaccines' potential to protect against infection with HBV. Methods: Hepatitis B-specific antibody and T cell responses of patients vaccinated with BM32 were studied using recombinant preS and synthetic overlapping peptides spanning the preS sequence. The specificities of the antibody responses were compared with those of patients with chronic HBV infection. Furthermore, the capacity of BM32-induced antibodies, to inhibit HBV infection was investigated using HepG2-hNTCP cell-based in vitro virus neutralization assays. Findings: IgG antibodies from BM32-vaccinated but not of HBV-infected individuals recognized the sequence motif implicated in NTCP (sodium-taurocholate co-transporting polypeptide)-receptor interaction of the hepatitis B virus and inhibited HBV infection. Interpretation: Our study demonstrates that the recombinant hypoallergenic grass pollen allergy vaccine BM32 induces hepatitis B-specific immune responses which protect against hepatitis B virus infection in vitro.
机译:背景:我们已经构建并临床评估了草花粉过敏的低变应原性疫苗BM32,该疫苗基于融合蛋白,该融合蛋白由主要草花粉过敏原与preS(preS1 + preS2)融合的主要IgE结合位点的肽组成。乙型肝炎病毒(HBV)大包膜蛋白,介导病毒附着和进入。这项研究的目的是表征由BM32过敏性患者的疫苗接种引起的HBV特异性免疫反应的特征,并研究疫苗预防HBV感染的潜力。方法:使用重组preS和跨越preS序列的合成重叠肽,研究了接种了BM32的患者的乙型肝炎特异性抗体和T细胞反应。将抗体应答的特异性与慢性HBV感染患者的特异性进行了比较。此外,使用基于HepG2-hNTCP细胞的体外病毒中和试验研究了BM32诱导的抗体抑制HBV感染的能力。结果:接种了BM32疫苗但未感染HBV个体的IgG抗体识别了与乙型肝炎病毒的NTCP(牛磺胆酸钠共转运多肽)-受体相互作用有关的序列基序,并抑制了HBV感染。解释:我们的研究表明,重组低变应原性草花粉过敏疫苗BM32可以诱导B型肝炎特异性免疫反应,从而在体外保护免受B型肝炎病毒感染。

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