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Analysis of strategies to successfully vaccinate infants in developing countries against enterotoxigenic E. coli (ETEC) disease

机译:对发展中国家婴儿成功接种产肠毒素的大肠杆菌(ETEC)疾病的策略分析

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Enterotoxigenic Escherichia coli (ETEC) is the most common bacterial cause of diarrhoea in the world, annually affecting up to 400,000,000 children under 5 years of age living in developing countries (DCs). Although ETEC possesses numerous antigens, the relatively conserved colonization factor (CF) antigens and the heat labile enterotoxin (LT) have been associated with protection and most vaccine candidates have exploited these antigens. A safe and effective vaccine against ETEC is a feasible goal as supported by the acquisition of protective immunity. The success of an ETEC vaccine targeting infants and children in DCs will depend on a combination of maximally antigenic vaccine preparations and regimens for their delivery which will produce optimal immune responses to these antigens. Vaccine candidates having a high priority for accelerated development and clinical testing for eventual use in infants would include inactivated ETEC or Shigella hybrids expressing ETEC antigens as well as attenuated ETEC strains which express the major CF antigens and LT toxin B-subunit, as well as attenuated Shigella, Vibrio cholerae and Salmonella typhi hybrids engineered to deliver antigens of ETEC. Candidates for an ETEC vaccine would have to meet the minimal requirement of providing at least 50% protection against severe disease in DCs during the first 2 years of life. The critical roadblock to achieving this goal has not been the science as much as the lack of a sufficiently funded and focused effort to bring it to realization. However, a Product Development Partnership to overcome this hurdle could accelerate the time lines towards when control of ETEC disease in DCs is substantially closer.
机译:肠毒素性大肠杆菌(ETEC)是世界上最常见的腹泻细菌病因,每年影响到生活在发展中国家(DC)的4亿以下5岁以下儿童。尽管ETEC拥有众多抗原,但相对保守的定居因子(CF)抗原和热不稳定肠毒素(LT)已与保护相关,大多数候选疫苗已利用这些抗原。获得保护性免疫支持,针对ETEC的安全有效疫苗是可行的目标。针对DC中婴儿和儿童的ETEC疫苗的成功取决于最大抗原性疫苗制剂和给药方案的组合,以产生对这些抗原的最佳免疫反应。对于加速发展和最终用于婴儿的临床测试,高度优先考虑的候选疫苗包括表达ETEC抗原的灭活ETEC或志贺氏菌杂种,以及表达主要CF抗原和LT毒素B亚基的弱毒ETEC菌株,以及弱毒志贺氏菌,霍乱弧菌和伤寒沙门氏菌杂交种经过工程设计以传递ETEC抗原。 ETEC疫苗的候选人必须满足最低要求,即在生命的头2年内提供至少50%的预防DC严重疾病的保护。实现这一目标的关键障碍并不是科学,而是缺乏足够的资金和专注的努力来实现它。但是,建立产品开发合作伙伴关系以克服这一障碍可能会加快接近控制DC中ETEC疾病的时间表。

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