首页> 外文期刊>Stem Cells >Medial ganglionic eminence-derived neural stem cell grafts ease spontaneous seizures and restore GDNF expression in a rat model of chronic temporal lobe epilepsy.
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Medial ganglionic eminence-derived neural stem cell grafts ease spontaneous seizures and restore GDNF expression in a rat model of chronic temporal lobe epilepsy.

机译:内侧神经神经神经神经神经神经神经神经干细胞移植物缓解并恢复慢性颞叶癫痫大鼠模型中的GDNF表达。

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Nearly 30% of patients with mesial temporal lobe epilepsy (TLE) are resistant to treatment with antiepileptic drugs. Neural stem cell (NSC) grafting into the hippocampus could offer an alternative therapy to hippocampal resection in these patients. As TLE is associated with reduced numbers of inhibitory gamma-amino butyric acid (GABA)-ergic interneurons and astrocytes expressing the anticonvulsant glial-derived neurotrophic factor (GDNF) in the hippocampus, we tested the hypothesis that grafting of NSCs that are capable of adding new GABA-ergic interneurons and GDNF-expressing astrocytes into the epileptic hippocampus restrains spontaneous recurrent motor seizures (SRMS) in chronic TLE. We grafted NSCs expanded in vitro from embryonic medial ganglionic eminence (MGE) into hippocampi of adult rats exhibiting chronic TLE with cognitive impairments. NSC grafting reduced frequencies of SRMS by 43% and stage V seizures by 90%. The duration of individual SRMS and the total time spent in seizures were reduced by 51 and 74%, respectively. Grafting did not improve the cognitive function however. Graft-derived cells (equivalent to approximately 28% of injected cells) were observed in various layers of the epileptic hippocampus where they differentiated into NeuN+ neurons (13%), S-100beta+ astrocytes (57%), and NG2+ oligodendrocyte-progenitors (3%). Furthermore, among graft-derived cells, 10% expressed GABA and 50% expressed GDNF. Additionally, NSC grafting restored GDNF in a vast majority of the hippocampal astrocytes but had no effect on neurogenesis. Thus, MGE-NSC therapy is efficacious for diminishing SRMS in chronic TLE. Addition of new GABA-ergic neurons and GDNF+ cells, and restoration of GDNF in the hippocampal astrocytes may underlie the therapeutic effect of MGE-NSC grafts.
机译:近30%的患有颞叶癫痫(TLE)的患者对抗癫痫药物进行耐药性。嫁接进入海马的神经干细胞(NSC)可以为这些患者的海马切除术提供替代治疗。由于TLE与抑制性γ-氨基丁酸(GABA)-ergic interric酸(GABA)-ergic instricon和星形胶质细胞相关联,并且在海马中表达抗惊厥药物神经营养因子(GDNF),我们测试了能够加入的NSC的假设新的GABA-ERGIC Interneurons和GDNF表达的星形胶质细胞进入癫痫海马抑制了慢性电阻的自发性反复运动癫痫发作(SRMS)。我们嫁接了NSCs在胚胎内膜神经节卓越(MGE)中扩增了成年大鼠的海马,其具有认知障碍的慢性收集。 NSC接枝SRMS的频率降低43%,阶段V癫痫发作量为90%。单独的SRMS的持续时间和癫痫发作的总时间分别降低51%和74%。然而,嫁接没有改善认知功能。在癫痫海马的各层中观察到接枝衍生的细胞(相当于约28%的注射细胞),其中它们分化为Neun +神经元(13%),S-100beta +星形胶质细胞(57%)和Ng2 +少突胶质细胞 - 祖细胞(3 %)。此外,在接枝衍生的细胞中,10%表达GABA和50%表达GDNF。此外,NSC接枝在绝大多数海马星形胶质细胞中恢复了GDNF,但对神经发生没有影响。因此,MGE-NSC治疗对于慢性狭窄的慢性缩短SRMS是有效的。添加新的GABA-ERGIC神经元和GDNF +细胞,并且在海马星形胶质细胞中恢复GDNF可能使MGE-NSC移植物的治疗效果提升。

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