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基于微纳传感调控技术的细胞胞内电子学的研究进展
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作者 徐冬馨 方佳如 胡宁 《生命科学仪器》 2022年第4期4-12,共9页
建立可靠的电生理记录平台对于心脏病学和神经科学的研究至关重要。近十年来,基于微纳传感调控技术的器件被开发用于电生理平台的搭建,其独特的形貌优势和新颖的加工方式,使得高通量、高保真的电信号记录有望被实现。本综述分别从微纳... 建立可靠的电生理记录平台对于心脏病学和神经科学的研究至关重要。近十年来,基于微纳传感调控技术的器件被开发用于电生理平台的搭建,其独特的形貌优势和新颖的加工方式,使得高通量、高保真的电信号记录有望被实现。本综述分别从微纳传感调控器件的材料、结构、加工和穿膜策略等方面进行了总结,并对其在心肌细胞和神经细胞电生理检测上的应用进行了分析。在微纳传感调控技术所面临的机遇挑战下,对其广阔的发展前景进行了展望,希望借助其快速发展来推动更高层次的电生理平台搭建,以满足实验研究以及临床应用的需求。 展开更多
关键词 微纳传感调控技术 细胞生理 电兴奋细胞 纳米生物界面
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δ-opioid Receptor Induced Inhibition of Sodium Channel Function
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作者 康学智 顾全保 +5 位作者 丁光宏 晁东满 王英伟 G Balboni LH Lazarus 夏萤 《Journal of Acupuncture and Tuina Science》 2008年第5期276-278,共3页
Objective: To study the precise role of DOR in the regulation of sodium channels at present. Methods: With Xenopus oocytes co-expressing sodium channel subtype 2 (Nav1.2) and DOR. Results: 1) Nav1.2 expression i... Objective: To study the precise role of DOR in the regulation of sodium channels at present. Methods: With Xenopus oocytes co-expressing sodium channel subtype 2 (Nav1.2) and DOR. Results: 1) Nav1.2 expression induced tetrodotoxin-sensitive inward currents; 2) DOR expression reduced the inward currents; 3) activation of DOR reduced the amplitude of the current and rightly shifted the activation curve of the current in the oocytes with both Nav1.2 and DOR, but not in ones with Nav1.2 alone; 4) the DOR agonist-induced inhibition of Nay 1.2 currents was in a dose-dependent manner and saturable; 5) the DOR agonist had no effect on naive oocytes. Conclusion: These data represent the first demonstration that activation of DOR inhibits Na^+ channel function by decreasing the amplitude of sodium currents and increasing its threshold of activation. This novel finding has far-reaching impacts on novel solutions of certain neurological disorders such as hypoxic/ischemic injury, epilepsy and pain. Also, our data may improve the understanding of the mechanisms underlying acupuncture since acupuncture is known to activate the brain opioid system. 展开更多
关键词 δ-opioid Receptors Na^+ Channels Na^+ Currents UFP-512 Xenopus Oocytes EXCITABILITY
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