在颞叶癫痫大鼠模型中海马组织中即早基因c—fos的表达(2)
5 总结与展望
癫痫作为最常见的神经科疾患之一,颞叶癫痫可能是人类最常见和被研究最热的一种癫痫形式。TLE表示该疾病的总的癫痫形式的40%,并且难以治愈。虽然从患者的脑电图、成像技术、临床表现和组织学研究能得到描述性数据,癫痫的发病机制尚不清楚。癫痫不可能是单个因子或一个单一的机制导致所有与此相关的神经病这些变化。癫痫导致神经细胞死亡,神经元的损失,或神经发生改变神经回路的传导。
氯化锂-匹罗卡品致颞叶癫痫大鼠模型具有与人类癫痫相似的行为学表现、脑电图、视频脑电图表现,是理想的研究人类颞叶癫痫发病原因与机制的模型。海马组织对缺血、缺氧特别敏感,即早基因尤其是c-fos在颞叶癫痫中表达增多与颞叶癫痫的发病机制相关。研究即早基因在颞叶癫痫大鼠的表达对人类难治性癫痫尤其是颞叶癫痫的发病机制及其预防和治疗有积极的指导意义。
因此,研究颞叶癫痫后神经元变性损伤的相关机制,对癫痫发病机制、预防和治疗具有十分重要的临床意义,加强对其中环节的重点关注和干预将是未来该领域的主要研究方向之一。
, 百拇医药
[参考文献]
[1] Kwan P, Arzimanoglou A, Berg A, et al. Definition of drug resistant epilepsy: consensus proposal by the adhoc task force of the ILAE commission on therapeutic strategies[J].Epilepsia, 2010, 51(6): 1069-1077.
[2] 王玉,阮旭中,何小华,等.侧脑室注射IL-1B. IL-rA对大脑皮层、海马Fos蛋白表达的影响[J].中国神经免疫学和神经病学杂志,2000,7(1): 11.
[3] Curia G,Longo D,Biagini G,et al.The pilocarpine model of temporal lobe epilepsy[J].J Neurosci Methods,2008,172(2):143-157.
, 百拇医药
[4] 苏曼,童晓欣.锂-匹罗卡品致痫模型海马星形胶质细胞缝隙连接研究[J].南方医科大学学报,2010,30(12):2738-2741.
[5] Zhang L, Liang S, Zhang G,et al.Seizure control of current shunt on rats with temporal lobe epilepsy and neocortical epilepsy[J].PLoS One,2014 3,9(1).
[6] 王海燕,王影,聂磊,张岩,等. 左乙拉西坦对癫痫大鼠认知功能及海马组织中NPY和NCAM-mRNA表达的影响[J].黑龙江医药科学,2013,36(3):3-5.
[7] Takei H, Wilfong A, Yoshor D, et al. Evidence of increased cell proliferation in the hippocampus in children with Ammon’s horn sclerosis[J]. Pathol Int,2007,57(2):76.
, http://www.100md.com
[8] Xu W,Orr-Urtreger A,Nigro F,et al.Multiorgan autonomic dysfunction in mice lacking the beta2 and beta4 subunits of neuronal nicotinic acetylcholine receptors[J].J Neurosci,1999,19(21):9298-9305.
[9] Rumney RM, Sunters A, Reilly GC,et al. Application of multiple forms of mechanical loading to human osteoblasts reveals increased ATP release in response to fluid flow in 3D cultures and differential regulation of immediate early genes[J].J Biomech,2012,45(3):549.
, 百拇医药
[10] 邢奋丽,邓毅,王林娥,等.即早基因c-Jun在顺铂诱发豚鼠耳蜗Corti器细胞凋亡中的作用[J].听力学及言语疾病杂志,2013,21(2):151-154.
[11] 刘晓军,雷梅芳,张玉琴.即早基因c-fos与神经系统疾病的研究进展[J].天津医科大学学报,2011,17(1):137-139.
[12] Kim, D.H., Kim, J.M., Park, S.J.,et al.GABA(A) receptor blockade enhances memory consolidation by increasing hippocampal BDNF levels[J].Neuropsychopharmacology,2012,37(2):422-433.
[13] 曹红,李军,李广明,等. 姜黄素对沙土鼠脑缺血/再灌注损伤的海马CA1区细胞凋亡和即早基因c-fos、c-jun、NF-κB表达变化的关系[J].中国应用生理学杂志,2007,23(2):184-188.
, 百拇医药
[14] Gu Y, Huang S, Chang MC, Worley P, Kirkwood A, Quinlan EM. Obligatory role for the immediate early gene NARP in critical period plasticity[J].Neuron,2013,79(2).
[15] Colciaghi F, Finardi A, Nobili P, Locatelli D, Spigolon G, Battaglia GS.Progressive Brain Damage, Synaptic Reorganization and NMDA Activation in a Model of Epileptogenic Cortical Dysplasia[J].PLoS One,2014,27,9(2).
[16] Chawla MK, Penner MR, Olson KM, Sutherland VL, Mittelman-Smith MA, Barnes CA. Spatial behavior and seizure-induced changes in c-fos mRNA expression in young and old rats[J].Neurobiol Aging,2013,34(4):1184.
[17] Pereno GL, Balaszczuk V, Beltramino CA. Kainic acid-induced early genes activation and neuronal death in the medial extended amygdala of rats[J].Exp Toxicol Pathol,2011,63(3):291.
[18] 王强,刘福友,杨旭红,等.宁痫颗粒联合卡马西平对耐药性癫痫大鼠c-fos基因表达的影响[J].辽宁中医药大学学报,2013,15(7):34-37.
(收稿日期:2014-09-08), 百拇医药(邢英瀛 陈文武)
癫痫作为最常见的神经科疾患之一,颞叶癫痫可能是人类最常见和被研究最热的一种癫痫形式。TLE表示该疾病的总的癫痫形式的40%,并且难以治愈。虽然从患者的脑电图、成像技术、临床表现和组织学研究能得到描述性数据,癫痫的发病机制尚不清楚。癫痫不可能是单个因子或一个单一的机制导致所有与此相关的神经病这些变化。癫痫导致神经细胞死亡,神经元的损失,或神经发生改变神经回路的传导。
氯化锂-匹罗卡品致颞叶癫痫大鼠模型具有与人类癫痫相似的行为学表现、脑电图、视频脑电图表现,是理想的研究人类颞叶癫痫发病原因与机制的模型。海马组织对缺血、缺氧特别敏感,即早基因尤其是c-fos在颞叶癫痫中表达增多与颞叶癫痫的发病机制相关。研究即早基因在颞叶癫痫大鼠的表达对人类难治性癫痫尤其是颞叶癫痫的发病机制及其预防和治疗有积极的指导意义。
因此,研究颞叶癫痫后神经元变性损伤的相关机制,对癫痫发病机制、预防和治疗具有十分重要的临床意义,加强对其中环节的重点关注和干预将是未来该领域的主要研究方向之一。
, 百拇医药
[参考文献]
[1] Kwan P, Arzimanoglou A, Berg A, et al. Definition of drug resistant epilepsy: consensus proposal by the adhoc task force of the ILAE commission on therapeutic strategies[J].Epilepsia, 2010, 51(6): 1069-1077.
[2] 王玉,阮旭中,何小华,等.侧脑室注射IL-1B. IL-rA对大脑皮层、海马Fos蛋白表达的影响[J].中国神经免疫学和神经病学杂志,2000,7(1): 11.
[3] Curia G,Longo D,Biagini G,et al.The pilocarpine model of temporal lobe epilepsy[J].J Neurosci Methods,2008,172(2):143-157.
, 百拇医药
[4] 苏曼,童晓欣.锂-匹罗卡品致痫模型海马星形胶质细胞缝隙连接研究[J].南方医科大学学报,2010,30(12):2738-2741.
[5] Zhang L, Liang S, Zhang G,et al.Seizure control of current shunt on rats with temporal lobe epilepsy and neocortical epilepsy[J].PLoS One,2014 3,9(1).
[6] 王海燕,王影,聂磊,张岩,等. 左乙拉西坦对癫痫大鼠认知功能及海马组织中NPY和NCAM-mRNA表达的影响[J].黑龙江医药科学,2013,36(3):3-5.
[7] Takei H, Wilfong A, Yoshor D, et al. Evidence of increased cell proliferation in the hippocampus in children with Ammon’s horn sclerosis[J]. Pathol Int,2007,57(2):76.
, http://www.100md.com
[8] Xu W,Orr-Urtreger A,Nigro F,et al.Multiorgan autonomic dysfunction in mice lacking the beta2 and beta4 subunits of neuronal nicotinic acetylcholine receptors[J].J Neurosci,1999,19(21):9298-9305.
[9] Rumney RM, Sunters A, Reilly GC,et al. Application of multiple forms of mechanical loading to human osteoblasts reveals increased ATP release in response to fluid flow in 3D cultures and differential regulation of immediate early genes[J].J Biomech,2012,45(3):549.
, 百拇医药
[10] 邢奋丽,邓毅,王林娥,等.即早基因c-Jun在顺铂诱发豚鼠耳蜗Corti器细胞凋亡中的作用[J].听力学及言语疾病杂志,2013,21(2):151-154.
[11] 刘晓军,雷梅芳,张玉琴.即早基因c-fos与神经系统疾病的研究进展[J].天津医科大学学报,2011,17(1):137-139.
[12] Kim, D.H., Kim, J.M., Park, S.J.,et al.GABA(A) receptor blockade enhances memory consolidation by increasing hippocampal BDNF levels[J].Neuropsychopharmacology,2012,37(2):422-433.
[13] 曹红,李军,李广明,等. 姜黄素对沙土鼠脑缺血/再灌注损伤的海马CA1区细胞凋亡和即早基因c-fos、c-jun、NF-κB表达变化的关系[J].中国应用生理学杂志,2007,23(2):184-188.
, 百拇医药
[14] Gu Y, Huang S, Chang MC, Worley P, Kirkwood A, Quinlan EM. Obligatory role for the immediate early gene NARP in critical period plasticity[J].Neuron,2013,79(2).
[15] Colciaghi F, Finardi A, Nobili P, Locatelli D, Spigolon G, Battaglia GS.Progressive Brain Damage, Synaptic Reorganization and NMDA Activation in a Model of Epileptogenic Cortical Dysplasia[J].PLoS One,2014,27,9(2).
[16] Chawla MK, Penner MR, Olson KM, Sutherland VL, Mittelman-Smith MA, Barnes CA. Spatial behavior and seizure-induced changes in c-fos mRNA expression in young and old rats[J].Neurobiol Aging,2013,34(4):1184.
[17] Pereno GL, Balaszczuk V, Beltramino CA. Kainic acid-induced early genes activation and neuronal death in the medial extended amygdala of rats[J].Exp Toxicol Pathol,2011,63(3):291.
[18] 王强,刘福友,杨旭红,等.宁痫颗粒联合卡马西平对耐药性癫痫大鼠c-fos基因表达的影响[J].辽宁中医药大学学报,2013,15(7):34-37.
(收稿日期:2014-09-08), 百拇医药(邢英瀛 陈文武)