Glycolysis in energy metabolism during seizures

Glycolysis in energy metabolism during seizures

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摘要 Studies have shown that glycolysis increases during seizures, and that the glycolytic metabolite lactic acid can be used as an energy source. However, how lactic acid provides energy for seizures and how it can participate in the termination of seizures remains unclear. We reviewed possible mechanisms of glycolysis involved in seizure onset. Results showed that lactic acid was involved in seizure onset and provided energy at early stages. As seizures progress, lactic acid reduces the pH of tissue and induces metabolic acidosis, which terminates the seizure. The specific mechanism of lactic acid-induced acidosis involves several aspects, which include lactic acid-induced inhibition of the glycolytic enzyme 6-diphosphate kinase-1, inhibition of the N-methyl-D-aspartate receptor, activation of the acid-sensitive 1A ion channel, strengthening of the receptive mechanism of the inhibitory neurotransmitter Y-aminobutyric acid, and changes in the intra- and extracellular environment. Studies have shown that glycolysis increases during seizures, and that the glycolytic metabolite lactic acid can be used as an energy source. However, how lactic acid provides energy for seizures and how it can participate in the termination of seizures remains unclear. We reviewed possible mechanisms of glycolysis involved in seizure onset. Results showed that lactic acid was involved in seizure onset and provided energy at early stages. As seizures progress, lactic acid reduces the pH of tissue and induces metabolic acidosis, which terminates the seizure. The specific mechanism of lactic acid-induced acidosis involves several aspects, which include lactic acid-induced inhibition of the glycolytic enzyme 6-diphosphate kinase-1, inhibition of the N-methyl-D-aspartate receptor, activation of the acid-sensitive 1A ion channel, strengthening of the receptive mechanism of the inhibitory neurotransmitter Y-aminobutyric acid, and changes in the intra- and extracellular environment.

作者 Heng Yang Jiongxing Wu Ren Guo Yufen Peng Wen Zheng Ding Liu Zhi Song

机构地区 Department of Neurology Department of Pharmacy

出处《Neural Regeneration Research》 SCIE CAS CSCD 2013年第14期1316-1326,共11页 中国神经再生研究（英文版）

基金 supported by the National Natural Science Foundation of China,No.30971534 125 Project of the Third Xiangya Hospital,China

关键词 neural regeneration REVIEWS epilepsy energy metabolism GLYCOLYSIS EPILEPTOGENESIS terminationATP aerobic metabolism 6-diphosphate kinase-1 N-methyI-D-aspartate receptor acid-sensitive1A ion channel y-aminobutyric acid intra- and extracellular environment voltage-gated Na＋ andCa2＋ adenosine receptors ATP receptor grants-supported paper NEUROREGENERATION neural regeneration reviews epilepsy energy metabolism glycolysis epileptogenesis terminationATP aerobic metabolism 6-diphosphate kinase-1 N-methyI-D-aspartate receptor acid-sensitive1A ion channel y-aminobutyric acid intra- and extracellular environment voltage-gated Na＋ andCa2＋ adenosine receptors ATP receptor grants-supported paper neuroregeneration

分类号 R742.1 [医药卫生—神经病学与精神病学]

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1尹时华,龚树生,鄢开胜,李穗,陈沛,陈广理.Neuroglobin 基因体内转染对水杨酸钠给药后小鼠下丘核神经元听反应的影响(英文)[J].生理学报,2005,57(4):529-536. 被引量：6

二级参考文献3

1尹时华,龚树生,鄢开胜,李穗,陈沛,陈广理.水杨酸钠给药对小鼠下丘核NGB mRNA和蛋白表达的影响[J].第四军医大学学报,2004,25(23):2130-2132. 被引量：6
2包永德,朱辉,朱幸.鲫鱼视网膜谷氨酸受体和GABA受体在爪蟾卵母细胞中的表达[J].生理学报,1996,48(4):401-404. 被引量：1
3孙久荣,叶英模.超重状态出生大鼠转入正常重力状态后行为和Fos表达的改变[J].生理学报,2001,53(1):61-65. 被引量：16

共引文献5

1尹时华,唐安洲,仁毅,谭颂华,陈平,蔡红武,谢利红.水杨酸钠慢性给药对小鼠下丘核神经元超微结构及听反应特性的影响[J].中华耳科学杂志,2007,5(3):253-258. 被引量：3
2尹时华,唐安洲,幸小玲,谭颂华,谢利红.水杨酸钠对豚鼠螺旋神经节NGB mRNA和蛋白表达的影响[J].中国病理生理杂志,2007,23(12):2313-2316.
3尹时华,唐安洲,谭颂华,陈平,谢利红,任毅.水杨酸钠对幼年和成年豚鼠听性脑干反应阈值及螺旋神经节谷氨酸脱羧酶表达的影响[J].中华耳鼻咽喉头颈外科杂志,2008,43(5):364-368. 被引量：3
4刘超,孙善全.脑红蛋白与脑红蛋白介导的神经元保护作用[J].国际麻醉学与复苏杂志,2008,29(6):540-543.
5李琳,付子英,王丽萍,危晨雪,邹丽芳,陈其才,唐佳.普氏蹄蝠下丘谐波内外神经元处理多普勒频移补偿信息的差异[J].生物化学与生物物理进展,2014,41(12):1235-1244. 被引量：3

1LI Xia,CHEN ZhaoQin,JIANG Zheng,LI YeFei,ZHANG YunFeng.Zinc reverses glycine-dependent inactivation of NMDARs in cultured rat hippocampal neurons[J].Science China(Life Sciences),2012,55(12):1075-1081.
2Wenhai Huang,Chuansheng Li,Zhengrong Shen,Xiaoyu Zhu,Bo Xia,Chunqi Li.Development of a Zebrafish Model for Rapid Drug Screening against Alzheimer＇s Disease[J].Journal of Pharmacy and Pharmacology,2016,4(4):162-173. 被引量：3
3YAN Xu,SHI Zhong Fang,XU Li Xin,LI Jia Xin,WU Min,WANG Xiao Xuan,JIA Mei,DONG Li Ping,YANG Shao Hua,YUAN Fang.Glutamate Impairs Mitochondria Aerobic Respiration Capacity and Enhances Glycolysis in Cultured Rat Astrocytes[J].Biomedical and Environmental Sciences,2017,30(1):44-51. 被引量：6
4Long Teng,Fang Hong,Chenguang Zhang,Jiancheng He,Haiying Wang.Compound Formula Rehmannia alleviates levodopainduced dyskinesia in Parkinson's disease[J].Neural Regeneration Research,2014,9(4):407-412. 被引量：9
5Peijun Ju,Donghong Cui.The involvement of N-methyI-D-aspartate receptor （NMDAR） subunit NR1 in the pathophysiology of schizophrenia[J].Acta Biochimica et Biophysica Sinica,2016,48(3):209-219. 被引量：9
6Yi Ding Lan Xie Cun-Qing Chang Zhi-Min Chen Hua Ai.Activation of γ-aminobutyric Acid （A） Receptor Protects Hippocampus from Intense Exercise-induced Synapses Damage and Apoptosis in Rats[J].Chinese Medical Journal,2015(17):2330-2339. 被引量：3
7Xiao-Fei Wang,Tai-Yun Zhao,Rui-Bin Su,Ning Wu,Jin Li.Agmatine Prevents Adaptation of the Hippocampal Glutamate System in Chronic Morphine-Treated Rats[J].Neuroscience Bulletin,2016,32(6):523-530. 被引量：5
8Xiao-Min Zhang,Jian-Hong Luo.GluN2A versus GluN2B:twins,but quite different[J].Neuroscience Bulletin,2013,29(6):761-772. 被引量：5
9陈爱琴,陈晓春,周瑞祥,王玮.NMDAR/PKC通路介导基底外侧杏仁核的长时程增强[J].生理学报,2008,60(6):737-742. 被引量：1
10Lin Zhang,Jing Yang,Yunpeng Cao.What is the new target inhibiting the progression of Alzheimer's disease?[J].Neural Regeneration Research,2013,8(21):1938-1947.

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Glycolysis in energy metabolism during seizures

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