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阿尔茨海默病的转化动物模型:阿尔茨海默病协会商业联盟智囊团

Translational animal models for Alzheimer's disease: An Alzheimer's Association Business Consortium Think Tank.

作者信息

Vitek Michael P, Araujo Joseph A, Fossel Michael, Greenberg Barry D, Howell Gareth R, Rizzo Stacey J Sukoff, Seyfried Nicholas T, Tenner Andrea J, Territo Paul R, Windisch Manfred, Bain Lisa J, Ross April, Carrillo Maria C, Lamb Bruce T, Edelmayer Rebecca M

机构信息

Cognosci, Inc Durham North Carolina USA.

InterVivo Solutions Inc Fergus Ontario Canada.

出版信息

Alzheimers Dement (N Y). 2021 Jan 11;6(1):e12114. doi: 10.1002/trc2.12114. eCollection 2020.

Abstract

Over 5 million Americans and 50 million individuals worldwide are living with Alzheimer's disease (AD). The progressive dementia associated with AD currently has no cure. Although clinical trials in patients are ultimately required to find safe and effective drugs, animal models of AD permit the integration of brain pathologies with learning and memory deficits that are the first step in developing these new drugs. The purpose of the Alzheimer's Association Business Consortium Think Tank meeting was to address the unmet need to improve the discovery and successful development of Alzheimer's therapies. We hypothesize that positive responses to new therapies observed in validated models of AD will provide predictive evidence for positive responses to these same therapies in AD patients. To achieve this goal, we convened a meeting of experts to explore the current state of AD animal models, identify knowledge gaps, and recommend actions for development of next-generation models with better predictability. Among our findings, we all recognize that models reflecting only single aspects of AD pathogenesis do not mimic AD. Models or combinations of new models are needed that incorporate genetics with environmental interactions, timing of disease development, heterogeneous mechanisms and pathways, comorbidities, and other pathologies that lead to AD and related dementias. Selection of the best models requires us to address the following: (1) which animal species, strains, and genetic backgrounds are most appropriate; (2) which models permit efficient use throughout the drug development pipeline; (3) the translatability of behavioral-cognitive assays from animals to patients; and (4) how to match potential AD therapeutics with particular models. Best practice guidelines to improve reproducibility also need to be developed for consistent use of these models in different research settings. To enhance translational predictability, we discuss a multi-model evaluation strategy to de-risk the successful transition of pre-clinical drug assets to the clinic.

摘要

全球有超过500万美国人以及5000万人患有阿尔茨海默病(AD)。目前,与AD相关的进行性痴呆尚无治愈方法。尽管最终需要在患者身上进行临床试验以找到安全有效的药物,但AD动物模型能够将脑部病变与学习和记忆缺陷联系起来,这是开发这些新药的第一步。阿尔茨海默病协会商业联盟智库会议的目的是解决在改善AD治疗方法的发现和成功开发方面尚未满足的需求。我们假设,在经过验证的AD模型中观察到的对新疗法的积极反应将为AD患者对这些相同疗法的积极反应提供预测性证据。为实现这一目标,我们召集了一次专家会议,以探讨AD动物模型的现状,识别知识差距,并为开发具有更好预测性的下一代模型推荐行动方案。在我们的研究结果中,我们都认识到仅反映AD发病机制单一方面的模型并不能模拟AD。需要新的模型或模型组合,将遗传学与环境相互作用、疾病发展的时间、异质性机制和途径、合并症以及导致AD和相关痴呆的其他病理因素结合起来。选择最佳模型要求我们解决以下问题:(1)哪种动物物种、品系和遗传背景最合适;(2)哪些模型能够在整个药物开发流程中高效使用;(3)行为认知检测从动物到患者的可转化性;(4)如何将潜在的AD治疗方法与特定模型相匹配。还需要制定最佳实践指南,以提高这些模型在不同研究环境中使用的可重复性。为了提高转化预测性,我们讨论了一种多模型评估策略,以降低临床前药物资产成功转化为临床药物的风险。

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