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可食用褐藻孔石莼的酶提取物及其富含间苯三酚单宁的部分对中枢神经系统的抑郁作用及潜在机制。

Depressive effects on the central nervous system and underlying mechanism of the enzymatic extract and its phlorotannin-rich fraction from Ecklonia cava edible brown seaweed.

作者信息

Cho Suengmok, Han Daeseok, Kim Seon-Bong, Yoon Minseok, Yang Hyejin, Jin Young-Ho, Jo Jinho, Yong Hyeim, Lee Sang-Hoon, Jeon You-Jin, Shimizu Makoto

机构信息

Korea Food Research Institute, Sungnam, Republic of Korea.

出版信息

Biosci Biotechnol Biochem. 2012;76(1):163-8. doi: 10.1271/bbb.110702. Epub 2012 Jan 7.

Abstract

Marine plants have been reported to possess various pharmacological properties; however, there have been few reports on their neuropharmacological effects. Terrestrial plants have depressive effects on the central nervous system (CNS) because of their polyphenols which make them effective as anticonvulsants and sleep inducers. We investigated in this study the depressive effects of the polyphenol-rich brown seaweed, Ecklonia cava (EC), on CNS. An EC enzymatic extract (ECEE) showed significant anticonvulsive (>500 mg/kg) and sleep-inducing (>500 mg/kg) effects on the respective mice seizure induced by picrotoxin and on the mice sleep induced by pentobarbital. The phlorotannin-rich fraction (PTRF) from ECEE significantly potentiated the pentobarbital-induced sleep at >50 mg/kg. PTRF had binding activity to the gamma aminobutyric acid type A (GABA(A))-benzodiazepine (BZD) receptors. The sleep-inducing effects of diazepam (DZP, a well-known GABA(A)-BZD agonist), ECEE, and PTRF were completely blocked by flumazenil, a well-known antagonist of GABA(A)-BZD receptors. These results imply that ECEE produced depressive effects on CNS by positive allosteric modulation of its phlorotannins on GABA(A)-BZD receptors like DZP. Our study proposes EC as a candidate for the effective treatment of neuropsychiatric disorders such as anxiety and insomnia.

摘要

据报道,海洋植物具有多种药理特性;然而,关于它们的神经药理作用的报道却很少。陆地植物由于其多酚类物质而对中枢神经系统(CNS)有抑制作用,这使得它们作为抗惊厥药和睡眠诱导剂很有效。在本研究中,我们调查了富含多酚的褐藻——海蕴(EC)对中枢神经系统的抑制作用。一种EC酶提取物(ECEE)对由苦味毒诱导的小鼠惊厥以及由戊巴比妥诱导的小鼠睡眠分别显示出显著的抗惊厥作用(>500毫克/千克)和睡眠诱导作用(>500毫克/千克)。ECEE中富含间苯三酚鞣质的部分(PTRF)在>50毫克/千克时能显著增强戊巴比妥诱导的睡眠。PTRF对γ-氨基丁酸A型(GABA(A))-苯二氮䓬(BZD)受体具有结合活性。地西泮(DZP,一种著名的GABA(A)-BZD激动剂)、ECEE和PTRF的睡眠诱导作用被氟马西尼完全阻断,氟马西尼是一种著名的GABA(A)-BZD受体拮抗剂。这些结果表明,ECEE通过其间苯三酚鞣质对GABA(A)-BZD受体的正变构调节,像DZP一样对中枢神经系统产生抑制作用。我们的研究提出,海蕴可作为有效治疗焦虑和失眠等神经精神疾病的候选药物。

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