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在缺血性中风小鼠模型中,给予α-亚麻酸进行肠内或肠外营养干预以对抗感觉运动和认知缺陷。

Alpha-linolenic acid given as enteral or parenteral nutritional intervention against sensorimotor and cognitive deficits in a mouse model of ischemic stroke.

作者信息

Bourourou Miled, Heurteaux Catherine, Blondeau Nicolas

机构信息

Université de Nice Sophia Antipolis, IPMC, Sophia Antipolis, F-06560, France; CNRS, IPMC, Sophia Antipolis, F-06560, France.

Université de Nice Sophia Antipolis, IPMC, Sophia Antipolis, F-06560, France; CNRS, IPMC, Sophia Antipolis, F-06560, France.

出版信息

Neuropharmacology. 2016 Sep;108:60-72. doi: 10.1016/j.neuropharm.2016.04.040. Epub 2016 Apr 29.

DOI:10.1016/j.neuropharm.2016.04.040
PMID:27133376
Abstract

Stroke is a leading cause of disability and death worldwide. Numerous therapeutics applied acutely after stroke have failed to improve long-term clinical outcomes. An emerging direction is nutritional intervention with omega-3 polyunsaturated fatty acids acting as disease-modifying factors and targeting post-stroke disabilities. Our previous studies demonstrated that the omega-3 precursor, alpha-linolenic acid (ALA) administrated by injections or dietary supplementation reduces stroke damage by direct neuroprotection, and triggering brain artery vasodilatation and neuroplasticity. Successful translation of putative therapies will depend on demonstration of robust efficacy on common deficits resulting from stroke like loss of motor control and memory/learning. This study evaluated the value of ALA as adjunctive therapy for stroke recovery by comparing whether oral or intravenous supplementation of ALA best support recovery from ischemia. Motor and cognitive deficits were assessed using rotarod, pole and Morris water maze tests. ALA supplementation in diet was better than intravenous treatment in improving motor coordination, but this improvement was not due to a neuroprotective effect since infarct size was not reduced. Both types of ALA supplementation improved spatial learning and memory after stroke. This cognitive improvement correlated with higher survival of hippocampal neurons. These results support clinical investigation establishing therapeutic plans using ALA supplementation.

摘要

中风是全球致残和致死的主要原因。中风后急性期应用的众多治疗方法均未能改善长期临床预后。一个新出现的方向是进行营养干预,使用ω-3多不饱和脂肪酸作为疾病修饰因子,针对中风后的残疾状况。我们之前的研究表明,通过注射或饮食补充给予ω-3前体α-亚麻酸(ALA),可通过直接神经保护、触发脑动脉血管舒张和神经可塑性来减轻中风损伤。将假定的治疗方法成功转化应用将取决于证明其对中风导致的常见缺陷(如运动控制丧失和记忆/学习障碍)具有强大疗效。本研究通过比较口服或静脉补充ALA是否最有利于从缺血中恢复,评估了ALA作为中风恢复辅助治疗的价值。使用转棒试验、爬杆试验和莫里斯水迷宫试验评估运动和认知缺陷。饮食中补充ALA在改善运动协调性方面优于静脉治疗,但这种改善并非由于神经保护作用,因为梗死灶大小并未减小。两种类型的ALA补充均改善了中风后的空间学习和记忆。这种认知改善与海马神经元较高的存活率相关。这些结果支持开展临床研究,制定使用ALA补充剂的治疗方案。

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