首页> 外文期刊>Journal of Neurophysiology >Novel potassium channel blocker, 4-AP-3-MeOH, inhibits fast potassium channels and restores axonal conduction in injured guinea pig spinal cord white matter.
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Novel potassium channel blocker, 4-AP-3-MeOH, inhibits fast potassium channels and restores axonal conduction in injured guinea pig spinal cord white matter.

机译:新型钾通道阻滞剂4-AP-3-MeOH可抑制快速的钾通道并恢复豚鼠脊髓白质损伤中的轴突传导。

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We have demonstrated that 4-aminopyridine-3-methanol (4-AP-3-MeOH), a 4-aminopyridine derivative, significantly restores axonal conduction in stretched spinal cord white-matter strips and shows no preference in restoring large and small axons. This compound is 10 times more potent when compared with 4-AP and other derivatives in restoring axonal conduction. Unlike 4-AP, 4-AP-3-MeOH can restore axonal conduction without changing axonal electrophysiological properties. In addition, we also have confirmed that 4-AP-3-MeOH is indeed an effective blocker of I(A) based on patch-clamp studies using guinea pig dorsal root ganglia cells. Furthermore, we have also provided the critical evidence to confirm the unmasking of potassium channels following mechanical injury. Taken together, our data further supports and implicates the role of potassium channels in conduction loss and its therapeutic value as an effective target for intervention to restore function in spinal cord trauma. Furthermore, due to its high potency and possible low side effect of impacting electrophysiological properties, 4-AP-3-MeOH is perhaps the optimal choice in reversing conduction block in spinal cord injury compared with other derivatives previously reported from this group.
机译:我们已经证明4-氨基吡啶-3-甲醇(4-AP-3-MeOH),一种4-氨基吡啶衍生物,可以显着恢复伸展的脊髓白质条带中的轴突传导,并且在恢复大小轴突方面没有任何偏好。与4-AP和其他衍生物相比,该化合物在恢复轴突传导方面的功效是其十倍。与4-AP不同,4-AP-3-MeOH可以在不改变轴突电生理特性的情况下恢复轴突传导。此外,基于使用豚鼠背根神经节细胞的膜片钳研究,我们还证实了4-AP-3-MeOH确实是I(A)的有效阻断剂。此外,我们还提供了关键证据,以确认机械损伤后钾通道的暴露。综上所述,我们的数据进一步支持并暗示了钾通道在传导丧失中的作用及其治疗价值,作为干预措施可有效恢复脊髓创伤中的功能。此外,由于它的高功效和影响电生理特性的低副作用,与先前从该组报道的其他衍生物相比,4-AP-3-MeOH可能是脊髓损伤中逆转传导阻滞的最佳选择。

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