Structural determinants of human immunity to anthrax

人体炭疽免疫力的结构决定因素

• 批准号: 7073443
• 负责人: Donald C Reason
• 金额: $ 40.37万
• 依托单位: CHILDREN'S HOSPITAL & RES CTR AT OAKLAND
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-06-01 至 2009-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7073443
• 关键词: anthrax; anthrax toxin; anthrax vaccines; antigen antibody reaction; bioterrorism /chemical warfare; calorimetry; clinical research; human subject; immune response; immunity; immunogenetics; immunoglobulin structure; immunoglobulins; molecular cloning; monoclonal antibody; patient oriented research; protein engineering; protein sequence; vaccine development; vaccine evaluation

DESCRIPTION (provided by applicant): The recent, intentional dissemination of Bacillus anthracis caused significant morbidity and mortality, as well as widespread and costly disruption of essential public services. The resulting re-evaluation of current methods for the prevention and treatment of anthrax has revealed significant gaps in our knowledge of the basic immunobiology of this disease, and highlighted the need to develop methodologies for establishing vaccine efficacy in the absence of clinical trials. The research described in this proposal will define the molecular and structural characteristics of the protective antibody response elicited by the currently licensed human anthrax vaccine. Methods of repertoire cloning recently developed in our laboratory will be used to establish at the molecular level the structural diversity, variable gene usage, and somatic maturational history of the human antibody repertoire specific for the protective antigen (PA) of B. anthracis. The extent to which different individuals utilize the same immunoglobulin variable gene products to bind specific epitopes on the antigen will be determined. Through sequence analysis, the degree to which responding antibody clones have undergone somatic maturation will be ascertained. Clonally derived PA-specific binding domains will be expressed in vitro, the subset capable of blocking PA functional activity identified, and affinity and valence requirements for functionality established. Cloned antibody binding domains will be used to define the PA-associated antigenic epitopes recognized by the human immune response, and to pinpoint those PA-associated epitopes that elicit neutralizing antibodies. Our findings will be crucial for the rational design of PA subunit vaccines, and will aid in establishing in vitro correlates of protective immunity to B. anthracis infection. In addition, the antibodies isolated will constitute a panel of fully human monoclonal binding domains with potential for therapeutic use as passive immunogens.

描述（由申请人提供）：最近，炭疽杆菌的故意传播造成了显著的发病率和死亡率，以及基本公共服务的广泛和昂贵的中断。由此产生的对当前预防和治疗炭疽病方法的重新评估揭示了我们对这种疾病的基本免疫生物学知识的巨大差距，并强调需要开发在缺乏临床试验的情况下确定疫苗功效的方法。本提案中描述的研究将确定目前获得许可的人类炭疽疫苗引起的保护性抗体反应的分子和结构特征。我们实验室最近开发的库克隆方法将用于在分子水平上建立B保护性抗原（PA）特异性人抗体库的结构多样性、可变基因使用和体细胞成熟历史。炭疽病将确定不同个体利用相同免疫球蛋白可变基因产物结合抗原上的特异性表位的程度。通过序列分析，将确定应答抗体克隆经历体细胞成熟的程度。克隆衍生的PA特异性结合结构域将在体外表达，鉴定能够阻断PA功能活性的子集，并建立功能的亲和力和效价要求。克隆的抗体结合结构域将用于定义由人免疫应答识别的PA相关抗原表位，并精确定位那些引发中和抗体的PA相关表位。我们的研究结果将是至关重要的PA亚单位疫苗的合理设计，并将有助于建立在体外相关的保护性免疫B。炭疽感染。此外，分离的抗体将构成一组完全人单克隆结合结构域，具有作为被动免疫原的治疗用途的潜力。