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D-丙氨酸-D-亮氨酸脑啡肽诱导的药物性低温对脑损伤的神经保护和神经再生潜力

Neuroprotective and neuroregenerative potential of pharmacologically-induced hypothermia with D-alanine D-leucine enkephalin in brain injury.

作者信息

Liska M Grant, Crowley Marci G, Tuazon Julian P, Borlongan Cesar V

机构信息

Center of Excellence for Aging and Brain Repair, University of South Florida College of Medicine, Tampa, FL, USA.

出版信息

Neural Regen Res. 2018 Dec;13(12):2029-2037. doi: 10.4103/1673-5374.241427.

Abstract

Neurovascular disorders, such as traumatic brain injury and stroke, persist as leading causes of death and disability - thus, the search for novel therapeutic approaches for these disorders continues. Many hurdles have hindered the translation of effective therapies for traumatic brain injury and stroke primarily because of the inherent complexity of neuropathologies and an inability of current treatment approaches to adapt to the unique cell death pathways that accompany the disorder symptoms. Indeed, developing potent treatments for brain injury that incorporate dynamic and multiple disorder-engaging therapeutic targets are likely to produce more effective outcomes than traditional drugs. The therapeutic use of hypothermia presents a promising option which may fit these criteria. While regulated temperature reduction has displayed great promise in preclinical studies of brain injury, clinical trials have been far less consistent and associated with adverse effects, especially when hypothermia is pursued via systemic cooling. Accordingly, devising better methods of inducing hypothermia may facilitate the entry of this treatment modality into the clinic. The use of the delta opioid peptide D-alanine D-leucine enkephalin (DADLE) to pharmacologically induce temperature reduction may offer a potent alternative, as DADLE displays both the ability to cause temperature reduction and to confer a broad profile of other neuroprotective and neuroregenerative processes. This review explores the prospect of DADLE-mediated hypothermia to treat neurovascular brain injuries, emphasizing the translational steps necessary for its clinical translation.

摘要

神经血管疾病,如创伤性脑损伤和中风,仍然是导致死亡和残疾的主要原因——因此,针对这些疾病的新型治疗方法的探索仍在继续。许多障碍阻碍了创伤性脑损伤和中风有效治疗方法的转化,主要是因为神经病理学固有的复杂性以及当前治疗方法无法适应伴随疾病症状的独特细胞死亡途径。事实上,开发包含动态和多个与疾病相关治疗靶点的有效脑损伤治疗方法可能比传统药物产生更有效的结果。低温疗法的治疗应用提供了一个可能符合这些标准的有前景的选择。虽然在脑损伤的临床前研究中,调节体温降低已显示出巨大的前景,但临床试验的结果却远不一致,且与不良反应相关,尤其是通过全身降温进行低温治疗时。因此,设计更好的诱导低温的方法可能会促进这种治疗方式进入临床。使用δ阿片肽D-丙氨酸D-亮氨酸脑啡肽(DADLE)进行药理学诱导体温降低可能提供一种有效的替代方法,因为DADLE既具有降低体温的能力,又能赋予广泛的其他神经保护和神经再生过程。本综述探讨了DADLE介导的低温治疗神经血管性脑损伤的前景,强调了其临床转化所需的转化步骤。

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