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首页> 外文期刊>Frontiers in Microbiology >Antibody Immunity Induced by H7N9 Avian Influenza Vaccines: Evaluation Criteria, Affecting Factors, and Implications for Rational Vaccine Design
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Antibody Immunity Induced by H7N9 Avian Influenza Vaccines: Evaluation Criteria, Affecting Factors, and Implications for Rational Vaccine Design

机译:H7N9禽流感疫苗诱导的抗体免疫:评价标准,影响因素和合理疫苗设计的影响。

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Severe H7N9 avian influenza virus (AIV) infections in humans have public health authorities around the world on high alert for the potential development of a human influenza pandemic. Currently, the newly-emerged highly pathogenic avian influenza A (H7N9) virus poses a dual challenge for public health and poultry industry. Numerous H7N9 vaccine candidates have been generated using various platforms. Immunization trials in animals and humans showed that H7N9 vaccines are apparently poorly immunogenic because they induced low hemagglutination inhibition and virus neutralizing antibody titers. However, H7N9 vaccines elicit comparable levels of total hemagglutinin (HA)-reactive IgG antibody as the seasonal influenza vaccines, suggesting H7N9 vaccines are as immunogenic as their seasonal counterparts. A large fraction of overall IgG antibody is non-neutralizing antibody and they target unrecognized epitopes outside of the traditional antigenic sites in HA. Further, the Treg epitope identified in H7 HA may at least partially contribute to regulation of antibody immunity. Here, we review the latest advances for the development of H7N9 vaccines and discuss the influence of serological criteria on evaluation of immunogenicity of H7N9 vaccines. Next, we discuss factors affecting antibody immunity induced by H7N9 vaccines, including the change in antigenic epitopes in HA and the presence of the Treg epitope. Last, we present our perspectives for the unique features of antibody immunity of H7N9 vaccines and propose some future directions to improve or modify antibody response induced by H7N9 vaccines. This perspective would provide critical implications for rational design of H7N9 vaccines for human and veterinary use.
机译:人类的严重H7N9禽流感病毒(AIV)感染已引起世界各地公共卫生部门的高度关注,有关人类流感大流行的潜在发展。当前,新出现的高致病性甲型禽流感(H7N9)病毒对公共卫生和家禽业提出了双重挑战。使用各种平台已经产生了许多H7N9疫苗候选物。在动物和人类中进行的免疫试验表明,H7N9疫苗的免疫原性很差,因为它们诱导了较低的血凝抑制作用和病毒中和抗体的效价。但是,H7N9疫苗引起的总血凝素(HA)反应性IgG抗体水平与季节性流感疫苗相当,这表明H7N9疫苗与季节性流感疫苗具有相同的免疫原性。总体IgG抗体的很大一部分是非中和抗体,它们靶向HA中传统抗原位点之外无法识别的表位。此外,在H7HA中鉴定的Treg表位可以至少部分地有助于抗体免疫的调节。在这里,我们审查H7N9疫苗开发的最新进展,并讨论血清学标准对H7N9疫苗免疫原性评估的影响。接下来,我们讨论影响H7N9疫苗诱导的抗体免疫的因素,包括HA中抗原表位的变化和Treg表位的存在。最后,我们提出了H7N9疫苗抗体免疫的独特特征的观点,并提出了一些未来的方向,以改善或修改H7N9疫苗诱导的抗体反应。该观点将为合理设计用于人类和兽医学的H7N9疫苗提供关键意义。

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