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The way forward for ETEC controlled human infection models (CHIMs)

机译:ETEC控制人类感染模型(CHIMS)的前进方式

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In the absence of good animal models, Controlled Human Infection Models (CHIMs) are useful to assess efficacy of new vaccine candidates against Enterotoxic Escherichia coli (ETEC), as well as other preventive or therapeutic interventions. At the 2018Vaccines Against Shigella and ETEC (VASE) conference, a workshop was held to further review and discuss new challenge model developments and key issues related to further model standardization. During the workshop, invited speakers briefly summarized forattendees recent developments and main agenda issues before workshop participants were divided into four groups for more focused discussions. The main issues discussed were: (1) whether there is a need for more ETEC strains to test a diversity of vaccine candidates, and if so, what criteria/qualities are desirable in strain selection; (2) how ETEC CHIMs could be more standardized to better support ETEC vaccine development; (3) how volunteer selection criteria and screening should be performed, and; (4)how an expanded sample collection schema and collaborative analysis plan may facilitate a more in-depth assessment of the role of antigen-specific humoral and cellular immune responses in ETEC infection, and provide better insights into ETEC pathogenesis and correlates of protection. The workshop concluded that additional challenge strains may need to be developed to better support new vaccines and therapeutics that are advancing in the development pipeline. In this regard, the need for a well characterized ST-only expressing ETEC strain was highlighted as a priority given that promising new heat stable toxoid based vaccine candidates are on the horizon. In addition, further standardization of the ETEC CHIMs was strongly encouraged, noting that it maynot be realistic to standardize across all strains. Also, intensified volunteer screening may result in higher attack rates, although more stringent eligibility criteria may contribute to a more limited application of the model and diminish its representativeness. Finally, a sampling schedule and priority list for minimum set of samples was also proposed. Future workshops could be held to further refine standards for ETEC CHIMS and to facilitate more collaborative work on stored sample sets from previous and future ETEC CHIMs to maximize the contribution of these trials to our understanding of ETEC pathogenesis and our development of better prevention and control measures for this important pathogen.
机译:在没有良好的动物模型的情况下,受控人感染模型(CHIMS)可用于评估新疫苗候选者对肠毒性大肠杆菌(ETEC)以及其他预防或治疗干预的疗效。在2018年对志贺卡和ETEC(花瓶)会议上的2018Vaccines,举办了一个研讨会,进一步审查并讨论了新的挑战模型发展和与进一步模范标准化相关的关键问题。在研讨会期间,邀请发言者简要概述了追求近期的发展和主要议程问题,并在研讨会参与者分为四组以获得更多的重点讨论。讨论的主要问题是:(1)是否需要更多ETEC菌株来测试疫苗候选的多样性,如果是,则需要哪些标准/品质; (2)如何更加标准化ETEC Chims以更好地支持ETEC疫苗开发; (3)应如何进行志愿选择标准和筛选,以及; (4)展开的样品收集架构和协作分析计划如何有助于更深入地评估抗原特异性体液和细胞免疫反应在ETEC感染中的作用,并为ETEC发病机制提供更好的见解和保护。该研讨会得出结论,可能需要开发额外的挑战菌株以更好地支持在开发管道推进的新疫苗和治疗方法。在这方面,突出了对仅表达良好表达的STC表达的ETEC菌株的优先级作为优先考虑到基于新的热稳定类毒素的疫苗候选候选。此外,强烈鼓励了ETEC Chims的进一步标准化,并指出它可能会在所有菌株中标准化。此外,加强的志愿者筛选可能导致更高的攻击率,尽管更严格的资格标准可能有助于更有限的模型应用并减少其代表性。最后,还提出了最小样本集合的采样时间表和优先级列表。未来的研讨会可以举行进一步细化ETEC Chims的标准,并促进从之前和未来的ETEC Chims储存样本集的更多协作工作,以最大限度地提高这些试验对我们对ETEC发病机制的理解和更好预防和控制措施的发展的贡献对于这个重要病原体。

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