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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Mechanisms of Vaccine-Induced Protective Immunity against Coxiella burnetii Infection in BALB/c Mice.
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Mechanisms of Vaccine-Induced Protective Immunity against Coxiella burnetii Infection in BALB/c Mice.

机译:疫苗诱导的针对BALB / c小鼠的柯氏杆菌感染的保护性免疫的机制。

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To elucidate the mechanisms of vaccine-induced protective immunity against Coxiella burnetii infection, we compared the protective efficacy and immunogenicity between formalin-inactivated phase I vaccine (PI-V) and phase II vaccine (PII-V) in BALB/c mice. PI-V generated significant protection while PII-V did not confer measurable protection. Analysis of cytokine and subclass Ab responses indicated that both PI-V and PII-V were able to induce a Th1-dominant immune response but did not identify the component of host response that distinguished their ability to induce protective immunity. Interestingly, immunoblot analysis identified a difference between PI-V and PII-V vaccinates in antigenic recognition by specific Ab isotypes. The observation that PI-LPS elicited significant protection but PII-LPS did not confer measurable protection suggests PI-LPS may play a key role in PI-V-induced protection. Adoptive transfer of either immune sera or splenocytes mediated significant protection in naive BALB/c mice,supporting the notion that both humoral and cellular immunity are important for development of protective immunity. However, the evidence that immune sera and B cells were unable to control infection while T cells conferred significant protection in SCID mice supports the hypothesis that T cell-mediated immunity is critical for host defense against C. burnetii infection. This report presents novel evidence to highlight the importance of PI-LPS and Abs in protective immunity and has important implications for the design of new generation vaccines against Q fever.
机译:为了阐明疫苗诱导的针对伯氏柯氏杆菌感染的保护性免疫的机制,我们比较了福尔马林灭活的I期疫苗(PI-V)和II期疫苗(PII-V)在BALB / c小鼠中的保护效果和免疫原性。 PI-V产生了显着的保护,而PII-V没有提供可测量的保护。细胞因子和亚类Ab反应的分析表明,PI-V和PII-V都能够诱导Th1为主的免疫反应,但未鉴定出宿主反应的成分,从而区分了它们诱导保护性免疫的能力。有趣的是,免疫印迹分析确定了PI-V和PII-V疫苗之间在通过特异性Ab同种型进行抗原识别方面的差异。 PI-LPS引发了显着的保护,但PII-LPS没有赋予可测量的保护,这一观察表明PI-LPS可能在PI-V诱导的保护中起关键作用。在幼稚的BALB / c小鼠中,免疫血清或脾细胞的过继转移介导了显着的保护,支持体液免疫和细胞免疫对保护性免疫的发展都很重要的观点。但是,有证据表明免疫血清和B细胞无法控制感染,而T细胞在SCID小鼠中赋予了重要的保护作用,这支持了T细胞介导的免疫对于宿主抵抗Burnetii感染至关重要的假说。该报告提供了新的证据来强调PI-LPS和Abs在保护性免疫中的重要性,并且对设计针对Q热的新一代疫苗具有重要意义。

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