• 主题
高级搜索  >
历史搜索 清空历史
首页> 外文期刊>Molecular pharmacology. >Analgesic (omega)-conotoxins CVIE and CVIF selectively and voltage-dependently block recombinant and native N-type calcium channels.
【24h】

Analgesic (omega)-conotoxins CVIE and CVIF selectively and voltage-dependently block recombinant and native N-type calcium channels.

机译:镇痛药(ω)-芋螺毒素CVIE和CVIF选择性地和电压依赖性地阻断重组的和天然的N型钙通道。

获取原文
获取原文并翻译 | 示例
           
页面导航
  • 摘要
  • 著录项
  • 相似文献
  • 相关主题

摘要

Neuronal (N)-type Ca(2+) channel-selective omega-conotoxins have emerged as potential new drugs for the treatment of chronic pain. In this study, two new omega-conotoxins, CVIE and CVIF, were discovered from a Conus catus cDNA library. Both conopeptides potently displaced (125)I-GVIA binding to rat brain membranes. In Xenopus laevis oocytes, CVIE and CVIF potently and selectively inhibited depolarization-activated Ba(2+) currents through recombinant N-type (alpha1(B-b)/alpha(2)delta1/beta(3)) Ca(2+) channels. Recovery from block increased with membrane hyperpolarization, indicating that CVIE and CVIF have a higher affinity for channels in the inactivated state. The link between inactivation and the reversibility of omega-conotoxin action was investigated by creating molecular diversity in beta subunits: N-type channels with beta(2a) subunits almost completely recovered from CVIE or CVIF block, whereas those with beta(3) subunits exhibited weak recovery, suggesting that reversibility of the omega-conotoxin block may depend on the type of beta-subunit isoform. In rat dorsal root ganglion sensory neurons, neither peptide had an effect on low-voltage-activated T-type channels but potently and selectively inhibited high voltage-activated N-type Ca(2+) channels in a voltage-dependent manner. In rat spinal cord slices, both peptides reversibly inhibited excitatory monosynaptic transmission between primary afferents and dorsal horn superficial lamina neurons. Homology models of CVIE and CVIF suggest that omega-conotoxin/voltage-gated Ca(2+) channel interaction is dominated by ionic/electrostatic interactions. In the rat partial sciatic nerve ligation model of neuropathic pain, CVIE and CVIF (1 nM) significantly reduced allodynic behavior. These N-type Ca(2+) channel-selective omega-conotoxins are therefore useful as neurophysiological tools and as potential therapeutic agents to inhibit nociceptive pain pathways.
机译:神经元(N)型Ca(2+)通道选择性ω-conotoxins已成为潜在的治疗慢性疼痛的新药。在这项研究中,从Conus catus cDNA文库中发现了两种新的ω-芋螺毒素CVIE和CVIF。两个conopepteptes强力取代(125)I-GVIA绑定到大鼠脑膜。在非洲爪蟾卵母细胞中,CVIE和CVIF通过重组N型(alpha1(B-b)/ alpha(2)delta1 / beta(3))Ca(2+)通道有效并选择性地抑制去极化激活的Ba(2+)电流。膜超极化使阻断恢复增加,表明CVIE和CVIF对处于灭活状态的通道具有更高的亲和力。通过在β亚基中创建分子多样性来研究灭活和ω-芋螺毒素作用的可逆性之间的联系:具有β(2a)亚基的N型通道几乎完全从CVIE或CVIF嵌段中回收,而具有β(3)亚基的N型通道表现出恢复较弱,提示ω-芋螺毒素块的可逆性可能取决于β-亚基同种型的类型。在大鼠背根神经节感觉神经元中,没有一种肽对低压激活的T型通道有影响,但以电压依赖性方式有效地和选择性地抑制了高压激活的N型Ca(2+)通道。在大鼠脊髓切片中,这两种肽可逆地抑制初级传入神经元和背角浅层椎板神经元之间的兴奋性单突触传递。 CVIE和CVIF的同源性模型表明,ω-芋螺毒素/电压门控Ca(2+)通道相互作用主要由离子/静电相互作用控制。在神经性疼痛的大鼠部分坐骨神经结扎模型中,CVIE和CVIF(1 nM)明显降低了异常性疼痛行为。因此,这些N型Ca(2+)通道选择性ω-芋螺毒素可用作神经生理学工具和抑制伤害性疼痛途径的潜在治疗剂。

著录项

相似文献

  • 外文文献
  • 中文文献
  • 专利
获取原文

客服邮箱:kefu@zhangqiaokeyan.com

京公网安备:11010802029741号 ICP备案号:京ICP备15016152号-6 六维联合信息科技 (北京) 有限公司©版权所有

  • 客服微信

  • 服务号