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Protective role of adenylate cyclase in the context of a live pertussis vaccine candidate

机译:腺苷酸环化酶在候选百日咳活疫苗中的保护作用

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Despite high vaccination coverage, pertussis remains an important respiratory infectious disease and the least-controlled vaccine-preventable infectious disease in children. Natural infection with Bordetella pertussis is known to induce strong and long-lasting immunity that wanes later than vaccine-mediated immunity. Therefore, a live attenuated B. pertussis vaccine, named BPZE1, has been developed and has recently completed a phase I clinical trial in adult human volunteers. In this study, we investigated the contribution of adenylate cyclase (CyaA) in BPZE1-mediated protection against pertussis. A CyaA-deficient BPZE1 mutant was thus constructed. Absence of CyaA did not compromise the adherence properties of the bacteria onto mammalian cells. However, the CyaA-deficient mutant displayed a slight impairment in the ability to survive within macrophages compared to the parental BPZE1 strain. In vivo, whereas the protective efficacy of the CyaA-deficient mutant was comparable to the parental strain at a vaccine dose of 5 x 10(5) colony forming units (CPU), it was significantly impaired at a vaccine dose of 5 x 10(3) CPU. This impairment correlated with impaired lung colonization ability, and impaired IFN-gamma production in the animal immunized with the CyaA-deficient BPZE1 mutant while the pertussis-specific antibody profile and Th17 response were comparable to those observed in BPZE1-immunized mice. Our findings thus support a role of CyaA in BPZE1-mediated protection through induction of cellular mediated immunity. (C) 2013 Institut Pasteur. Published by Elsevier Masson SAS. All rights reserved.
机译:尽管接种疫苗的覆盖率很高,但百日咳仍然是儿童的一种重要的呼吸道传染病和可控制的疫苗预防程度最低的传染病。已知百日咳博德特氏菌的自然感染可诱导强大而持久的免疫力,而这种免疫力要晚于疫苗介导的免疫力。因此,已开发出一种名为BPZE1的减毒百日咳博德特氏菌活疫苗,并已在成人志愿者中完成了I期临床试验。在这项研究中,我们调查了腺苷酸环化酶(CyaA)在BPZE1介导的百日咳保护中的作用。由此构建了CyaA缺陷的BPZE1突变体。缺少CyaA不会损害细菌对哺乳动物细胞的粘附特性。但是,与亲本BPZE1菌株相比,CyaA缺陷型突变体在巨噬细胞内的生存能力显示出轻微的损害。在体内,尽管在疫苗剂量为5 x 10(5)集落形成单位(CPU)的情况下,CyaA缺陷型突变体的保护功效与亲本菌株相当,但在疫苗剂量为5 x 10(5)的情况下却明显受损。 3)CPU。这种损害与肺定植能力受损和用CyaA缺陷型BPZE1突变体免疫的动物的IFN-γ产生受损有关,而百日咳特异性抗体谱和Th17反应与在BPZE1免疫的小鼠中观察到的相当。因此,我们的发现通过诱导细胞介导的免疫支持CyaA在BPZE1介导的保护中的作用。 (C)2013年巴斯德研究所。由Elsevier Masson SAS发布。版权所有。

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