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首页> 外文期刊>Vaccine >Concomitant administration of Yersinia pestis specific monoclonal antibodies with plague vaccine has a detrimental effect on vaccine mediated immunity
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Concomitant administration of Yersinia pestis specific monoclonal antibodies with plague vaccine has a detrimental effect on vaccine mediated immunity

机译:鼠疫耶尔森氏菌特异性单克隆抗体与鼠疫疫苗的同时使用会对疫苗介导的免疫产生不利影响

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Antibodies can be used to confer rapid immunity against infectious agents for short periods of time. By comparison, vaccine induced immunity is more protective, but takes a relatively long time to develop. Concomitant administration of antibody and vaccine by different routes was evaluated as a means of providing both rapid and long-term protection against plague. BALB/c mice were treated intraperitoneally with monoclonal antibodies, with specificities for Yersinia pestis LcrV and F1 antigens. A cohort of these mice was simultaneously vaccinated with rF1 and rLcrV by the intramuscular route. Antibody co-administration with vaccine reduced the level of vaccine mediated protection afforded against a high level Y. pestis challenge. Conversely, antibody-mediated protection was unaffected by vaccine co-administration and lasted for at least 8 weeks post administration. We also evaluated the effect of administering vaccine intradermally and antibody intratracheally and observed that, irrespective of administration route, concomitant administration of antibody reduced the effectiveness of vaccine mediated immunity. The results of passive transfer experiments supported the thesis that the development of protective antibody responses following vaccination is impaired by the presence of circulating monoclonal antibodies with specificities for important B-cell epitopes in the vaccine. We also noted that intradermal injection of LcrV antigen and cholera toxin adjuvant afforded good levels of protection against systemic and aerosol challenge with Y. pestis: intradermal injection might therefore be considered as a potential minimally invasive method of plague vaccine administration. These data have implications for the design of therapeutic strategies against plague infection.
机译:抗体可用于在短时间内赋予针对传染原的快速免疫力。相比之下,疫苗诱导的免疫更具保护性,但需要相对较长的时间才能开发出来。评估了通过不同途径同时给予抗体和疫苗的情况,将其作为提供快速和长期的抗鼠疫保护的手段。用单克隆抗体腹膜内处理BALB / c小鼠,该抗体对鼠疫耶尔森菌LcrV和F1抗原具有特异性。通过肌肉内途径同时向这些小鼠的组接种rF1和rLcrV。与疫苗共同施用的抗体降低了疫苗介导的针对高水平鼠疫耶尔森氏菌攻击的保护水平。相反,抗体介导的保护不受疫苗共同给药的影响,并在给药后至少持续8周。我们还评估了皮内和气管内施用疫苗的效果,并观察到,与施用途径无关,抗体的同时施用降低了疫苗介导的免疫的有效性。被动转移实验的结果支持了这样的论点,即疫苗中重要的B细胞表位具有特异性的循环单克隆抗体的存在会削弱疫苗接种后保护性抗体应答的发展。我们还注意到,皮内注射LcrV抗原和霍乱毒素佐剂可提供良好的保护水平,以抵抗鼠疫耶尔森氏菌的全身性和气溶胶性攻击:因此皮内注射可能被视为潜在的微创鼠疫疫苗接种方法。这些数据对抗鼠疫感染的治疗策略的设计有影响。

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