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新型重组前S1、前S2和S基因乙肝表面抗原疫苗(Hepagene)的T细胞和B细胞免疫反应特征;应答小鼠中诱导产生高效抗-HBs抗体的证据

Characterization of the T- and B-cell immune response to a new recombinant pre-S1, pre-S2 and SHBs antigen containing hepatitis B vaccine (Hepagene); evidence for superior anti-SHBs antibody induction in responder mice.

作者信息

Jones C D, Page M, Bacon A, Cahill E, Bentley M, Chatfield S N

机构信息

Department of Biochemistry, Imperial College of Science, Technology and Medicine, London, UK.

出版信息

J Viral Hepat. 1998 Nov;5 Suppl 2:5-8. doi: 10.1046/j.1365-2893.1998.0050s2005.x.

DOI:10.1046/j.1365-2893.1998.0050s2005.x
PMID:9857353
Abstract

Hepagene is a novel recombinant particle consisting of the pre-S1, pre-S2 and small surface (SHBs) antigens (Ag) of the hepatitis B virus (HBV) and is adjuvanted with alhydrogel in the final formulation. It has been primarily developed to enhance anti-SHBs antibody titres in inadequate responders, to conventional SHBsAg vaccines. Since non-compliance is also a problem with existing HBV vaccine schedules, the ability to accelerate current immunization regimens to provide more rapid protection has also been an important objective. Here we describe the T- and B-cell responses to Hepagene in two strains of responder mouse (BALB/c and SWR/J). Hepagene induced high in vitro spleen T-cell proliferative responses in both strains (max. Stimulation Index = 43), following intraperitoneal immunization. High concentrations of interferon-gamma (max. = 5000 pg/mL) were detected in the media of spleen cells cultured with non-adjuvanted Hepagene particles. SWR/J mice showed the highest serum antibody (Ab) titres to non-adjuvanted Hepagene. The presence of alhydrogel adjuvant in the vaccine formulation significantly improved the titres. Anti-pre-S1 Ab was detected in both strains of mouse but anti-pre-S2 Ab was only detected in the SWR/J strain. In BALB/c mice, the anti-Hepagene (non-adjuvanted) IgG1 Ab subclass was predominant but in SWR/J mice IgG1, IgG2a and IgG2b subclasses were of a similar magnitude. In BALB/c mice, Hepagene induced higher anti-SHBs Ab responses than Engerix-B (11097 IU/mL and 1276 IU/mL, respectively), following two doses of vaccine (10 micrograms/mouse). The vaccine therefore, induces strong cellular and humoral immune responses and these data suggest that Hepagene is an improved hepatitis B vaccine.

摘要

肝基因疫苗(Hepagene)是一种新型重组颗粒,由乙型肝炎病毒(HBV)的前S1、前S2和小表面(SHBs)抗原组成,在最终制剂中与铝佐剂混合。它主要用于提高对传统SHBsAg疫苗应答不足者的抗SHBs抗体滴度。由于现有乙肝疫苗接种方案中也存在不依从的问题,因此加快当前免疫方案以提供更快保护的能力也是一个重要目标。在此,我们描述了两种应答小鼠品系(BALB/c和SWR/J)对肝基因疫苗的T细胞和B细胞反应。腹腔免疫后,肝基因疫苗在两种品系中均诱导出较高的体外脾脏T细胞增殖反应(最大刺激指数=43)。在用无佐剂肝基因颗粒培养的脾细胞培养基中检测到高浓度的干扰素-γ(最大=5000 pg/mL)。SWR/J小鼠对无佐剂肝基因疫苗的血清抗体滴度最高。疫苗制剂中铝佐剂的存在显著提高了滴度。在两种小鼠品系中均检测到抗前S1抗体,但仅在SWR/J品系中检测到抗前S2抗体。在BALB/c小鼠中,抗肝基因疫苗(无佐剂)IgG1抗体亚类占主导,但在SWR/J小鼠中,IgG1、IgG2a和IgG2b亚类的水平相似。在BALB/c小鼠中,两剂疫苗(10微克/小鼠)接种后,肝基因疫苗诱导的抗SHBs抗体反应高于安在时(Engerix-B)(分别为11097 IU/mL和1276 IU/mL)。因此,该疫苗可诱导强烈的细胞免疫和体液免疫反应,这些数据表明肝基因疫苗是一种改良的乙型肝炎疫苗。

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