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创伤性脑损伤的神经药理学:从临床前神经保护到临床?

Neuropharmacology in traumatic brain injury: from preclinical to clinical neuroprotection?

机构信息

UMR-S1144 - Optimisation Thérapeutique en Neuropsychopharmacologie, Faculté de Pharmacie de Paris, Université de Paris, Paris, France.

出版信息

Fundam Clin Pharmacol. 2021 Jun;35(3):524-538. doi: 10.1111/fcp.12656. Epub 2021 Mar 13.

Abstract

Traumatic brain injury (TBI) constitutes a major health problem worldwide and is a leading cause of death and disability in individuals, contributing to devastating socioeconomic consequences. Despite numerous promising pharmacological strategies reported as neuroprotective in preclinical studies, the translation to clinical trials always failed, albeit the great diversity of therapeutic targets evaluated. In this review, first, we described epidemiologic features, causes, and primary and secondary injuries of TBI. Second, we outlined the current literature on animal models of TBI, and we described their goals, their advantages and disadvantages according to the species used, the type of injury induced, and their clinical relevance. Third, we defined the concept of neuroprotection and discussed its evolution. We also identified the reasons that might explain the failure of clinical translation. Then, we reviewed post-TBI neuroprotective treatments with a focus on the following pleiotropic drugs, considered "low hanging fruit" with high probability of success: glitazones, glibenclamide, statins, erythropoietin, and progesterone, that were largely tested and demonstrated efficient in preclinical models of TBI. Finally, our review stresses the need to establish a close cooperation between basic researchers and clinicians to ensure the best clinical translation for neuroprotective strategies for TBI.

摘要

创伤性脑损伤(TBI)是一个全球性的主要健康问题,是导致个体死亡和残疾的主要原因,造成了破坏性的社会经济后果。尽管在临床前研究中报道了许多有希望的作为神经保护剂的药物策略,但它们总是未能转化为临床试验,尽管评估的治疗靶点多种多样。在这篇综述中,首先,我们描述了 TBI 的流行病学特征、原因以及原发性和继发性损伤。其次,我们概述了 TBI 动物模型的当前文献,并根据所使用的物种、诱导的损伤类型以及其临床相关性描述了它们的目标、优缺点。第三,我们定义了神经保护的概念,并讨论了它的演变。我们还确定了可能解释临床转化失败的原因。然后,我们回顾了 TBI 后的神经保护治疗,重点介绍了以下几种被认为是具有高成功率的“低挂果实”的多效药物:噻唑烷二酮类、格列本脲、他汀类药物、促红细胞生成素和孕酮,这些药物在 TBI 的临床前模型中得到了广泛的测试和证明是有效的。最后,我们的综述强调了基础研究人员和临床医生之间需要建立密切合作,以确保 TBI 的神经保护策略的最佳临床转化。

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