Omega-3 fatty acids and acute neurological trauma: a perspective on clinical translation

Stacy J. Gladman, Siew-Na Lim, S. Dyall, M. Knight, J. Priestley, A. Michael-Titus
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Abstract

Acute neurological trauma remains one of the clinical areas with the most significant unmet needs worldwide. In the central nervous system, acute trauma has two stages: the primary injury and the secondary injury. The former is irreversible, and is a direct consequence of the impact. In the aftermath of the injury, a complex series of processes exacerbate the injury and amplify tissue damage. Some of these processes are local, others involve a systemic response. It is these processes which ultimately determine the clinical outcome. The aim of the treatments is a) to confer neuroprotection and b) to promote neuroregeneration. The results reported so far with omega-3 fatty acids in animal models of neurotrauma suggest that these compounds have the potential to offer a novel therapeutic approach and target both protection and regeneration. They lead to increased neuronal and glial survival, they can limit the damaging neuroinflammation and they can also protect neurites. Long chain omega-3 fatty acids such as eicosapentaenoic acid and docosahexaenoic acid have a complex pharmacodynamics, which leads potentially to the activation of a multitude of targets, including voltage and ligand-gated ion channels, transcription factors and G-protein coupled receptors. They can produce tissue-specific metabolites which have intrinsic activity, either on the same or on different cellular targets. The apparent large therapeutic window of omega-3 fatty acids is an advantage in the context of trauma, with patients in an unstable state, with multiple injuries. The specific use of omega-3 fatty acids in spinal cord injury and peripheral nerve injury will be discussed, focusing on issues which need to be addressed in order to translate successfully to the clinic the efficacy reported in the initial proof of concept animal studies.
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欧米伽-3脂肪酸和急性神经创伤:对临床翻译的看法
急性神经创伤仍然是世界范围内未满足需求最多的临床领域之一。在中枢神经系统中,急性创伤有两个阶段:原发性损伤和继发性损伤。前者是不可逆转的,是气候变化影响的直接后果。在损伤之后,一系列复杂的过程加剧了损伤并扩大了组织损伤。其中一些过程是局部的,另一些则涉及到系统性的反应。正是这些过程最终决定了临床结果。治疗的目的是a)赋予神经保护,b)促进神经再生。到目前为止,在动物神经损伤模型中报道的omega-3脂肪酸的结果表明,这些化合物有可能提供一种新的治疗方法,并以保护和再生为目标。它们可以增加神经元和神经胶质的存活率,它们可以限制破坏性的神经炎症,它们也可以保护神经突。长链omega-3脂肪酸,如二十碳五烯酸和二十二碳六烯酸具有复杂的药理学,这可能导致多种靶标的激活,包括电压和配体门控离子通道、转录因子和g蛋白偶联受体。它们可以产生具有内在活性的组织特异性代谢物,无论是对相同的还是对不同的细胞目标。omega-3脂肪酸明显的大治疗窗口在创伤的情况下是一个优势,患者处于不稳定的状态,有多重损伤。将讨论omega-3脂肪酸在脊髓损伤和周围神经损伤中的具体应用,重点讨论需要解决的问题,以便将初步概念证明动物研究中报告的疗效成功转化为临床。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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