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平衡核苷转运体-1抑制剂通过抑制谷氨酸能传递发挥抗癫痫作用。

Equilibrative Nucleoside Transporters-1 Inhibitors Act as Anti-epileptic Agents by Inhibiting Glutamatergic Transmission.

作者信息

Ho Shih-Yin, Chen I-Chun, Chang Kai-Chieh, Lin Hsiao-Ru, Tsai Che-Wen, Lin Chun-Jung, Liou Horng-Huei

机构信息

Department of Neurology, National Taiwan University Hospital, College of Medicine, National Taiwan University, Taipei, Taiwan.

Department of Pharmacology, College of Medicine, National Taiwan University, Taipei, Taiwan.

出版信息

Front Neurosci. 2020 Dec 17;14:610898. doi: 10.3389/fnins.2020.610898. eCollection 2020.

Abstract

Adenosine dysregulation is associated with the occurrence of the epilepsy and equilibrative nucleoside transporters-1 (ENT-1) functions as an important regulator of extracellular adenosine in the brain. This study was aimed to prove the anti-epileptic effect of BBB permeable ENT-1 inhibitors, JMF1907 and J4, on animal models of various epilepsy, and the mechanisms that are involved. Maximal electroshock seizure (MES), pentylenetetrazol (PTZ)-induced seizure and kindling models were used as mouse models of generalized tonic-clonic epilepsy, generalized myoclonic epilepsy, and partial epilepsy, respectively. The epilepsy frequency, duration, and Racine score were evaluated. Whole-cell recordings were made from the hippocampal dentate granule cells by using a patch-clamp technique in the brain slice of the mice. In MES, JMF1907 at a dose of 5 mg kg was efficacious in decreasing hindlimb extension, while J4 did not decrease hindlimb extension until a higher dose (10 mg kg). Both JMF1907 and J4 were more potent in lengthening onset latency than ethosuximide (ETH) in PTZ-induced myoclonic epilepsy model, whereas ETH had better effects on the Racine score. In kindling model, JMF1907 and J4 at a dose of 1 mg kg had effects on seizure frequency and duration, and the effects of JMF1907 were comparable with those of carbamazepine. Both JMF1907 and J4 can reduce the glutamatergic spontaneous excitatory post-synaptic currents (sEPSCs) frequency. The maximal inhibition was about 50% for JMF1907 at a concentration of 1 μg L, whereas J4 only inhibited 40% of sEPSCs frequency at a dose of 10 μg L. ENT-1 inhibitors, JMF1907 and J4, showed anti-epileptic effects in different epilepsy models and the effects involved pre-synaptic neuronal modulation.

摘要

腺苷调节异常与癫痫的发生有关,而平衡核苷转运体-1(ENT-1)作为大脑细胞外腺苷的重要调节剂发挥作用。本研究旨在证明血脑屏障可通透的ENT-1抑制剂JMF1907和J4对各种癫痫动物模型的抗癫痫作用及其相关机制。最大电休克发作(MES)、戊四氮(PTZ)诱导的发作和点燃模型分别用作全身强直阵挛性癫痫、全身肌阵挛性癫痫和部分性癫痫的小鼠模型。评估癫痫发作频率、持续时间和拉辛评分。在小鼠脑片中,采用膜片钳技术对海马齿状颗粒细胞进行全细胞记录。在MES模型中,5mg/kg剂量的JMF1907可有效减少后肢伸展,而J4直到更高剂量(10mg/kg)才会减少后肢伸展。在PTZ诱导的肌阵挛性癫痫模型中,JMF1907和J4在延长发作潜伏期方面比乙琥胺(ETH)更有效,而ETH对拉辛评分的影响更好。在点燃模型中,1mg/kg剂量的JMF1907和J4对癫痫发作频率和持续时间有影响,JMF1907的效果与卡马西平相当。JMF1907和J4均可降低谷氨酸能自发兴奋性突触后电流(sEPSCs)频率。JMF1907在1μg/L浓度下的最大抑制率约为50%,而J4在10μg/L剂量下仅抑制40%的sEPSCs频率。ENT-1抑制剂JMF1907和J4在不同癫痫模型中显示出抗癫痫作用,其作用涉及突触前神经元调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a16/7773772/517d5673136e/fnins-14-610898-g001.jpg

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