• 主题
高级搜索  >
历史搜索 清空历史
首页> 外文期刊>American Journal of Physiology >Interactions between adenosine and K+ channel-related pathways in the coupling of somatosensory activation and pial arteriolar dilation.
【24h】

Interactions between adenosine and K+ channel-related pathways in the coupling of somatosensory activation and pial arteriolar dilation.

机译:体感激活与颈小动脉扩张耦合中腺苷和K +通道相关通路之间的相互作用。

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

Multiple, perhaps interactive, mechanisms participate in the linkage between increased neural activity and cerebral vasodilation. In the present study, we assessed whether neural activation-related pial arteriolar dilation (PAD) involved interactions among adenosine (Ado) A(2) receptors (A(2)Rs), large-conductance Ca(2+)-operated K(+) (BK(Ca)) channels, and inward rectifier K(+) (K(ir)) channels. In rats with closed cranial windows, we monitored sciatic nerve stimulation (SNS)-induced PAD in the absence or presence of pharmacological blockade of A(2)Rs (ZM-241385), ecto-5'-nucleotidase (alpha,beta-methylene-adenosine diphosphate), BK(Ca) channels (paxilline), and K(ir) channels (BaCl(2)). Individually, these interventions led to 53-66% reductions in SNS-induced PADs. Combined applications of these blockers led to little or no further repression of SNS-induced PADs, suggesting interactions among A(2)Rs and K(+) channels. In the absence of SNS, BaCl(2) blockade of K(ir) channels produced 52-80% reductions in Ado and NS-1619 (BK(Ca) channel activator)-induced PADs. In contrast, paxilline blockade of BK(Ca) channels was without effect on dilations elicited by KCl (K(ir) channel activator) and Ado suffusions, indicating that Ado- and NS-1619-associated PADs involved K(ir) channels. In addition, targeted ablation of the superficial glia limitans was associated with a selective 60-80% loss of NS-1619 responses, suggesting that the BK(Ca) channel participation (and paxilline sensitivity) derived largely from channels within the glia limitans. Additionally, blockade of either PKA or adenylyl cyclase caused markedly attenuated pial arteriolar responses to SNS and, in the absence of SNS, responses to Ado, KCl, and NS-1619. These findings suggested a key, possibly permissive, role for A(2)R-linked cAMP generation and PKA-induced K(+) channel phosphorylation in somatosensory activation-evoked PAD.
机译:多种可能相互作用的机制参与了神经活动增加与脑血管舒张之间的联系。在本研究中,我们评估了神经激活相关的椎小动脉扩张(PAD)是否涉及腺苷(Ado)A(2)受体(A(2)Rs),大电导Ca(2+)操作的K( +)(BK(Ca))通道,以及内向整流器K(+)(K(ir))通道。在闭合颅窗的大鼠中,我们在不存在或存在A(2)Rs(ZM-241385),ecto-5'-核苷酸酶(α,β-亚甲基)的药理阻断作用下,监测坐骨神经刺激(SNS)诱导的PAD -二磷酸腺苷),BK(Ca)通道(paxilline)和K(ir)通道(BaCl(2))。这些干预措施单独导致SNS诱导的PAD减少53-66%。这些阻滞剂的联合应用导致SNS诱导的PAD抑制得很少或没有进一步抑制,表明A(2)R和K(+)通道之间存在相互作用。在没有SNS的情况下,对K(ir)通道的BaCl(2)阻断产生Ado和NS-1619(BK(Ca)通道激活剂)诱导的PAD减少52-80%。相比之下,氨苄青霉素对BK(Ca)通道的阻滞对KCl(K(ir)通道激活剂)和Ado注入引起的扩张没有影响,这表明与Ado和NS-1619相关的PAD涉及K(ir)通道。此外,浅表神经胶质限脂蛋白的靶向消融与选择性的60-80%的NS-1619反应丧失有关,这表明BK(Ca)通道参与(和paxilline敏感性)主要源于神经胶质限脂剂内的通道。此外,对PKA或腺苷酸环化酶的阻断都会引起对SNS的小动脉运动明显减弱,在不存在SNS的情况下,对Ado,KCl和NS-1619的响应也会减弱。这些发现表明,在体感激活诱发的PAD中,A(2)R-关联的cAMP产生和PKA诱导的K(+)通道磷酸化具有关键性,可能是宽松的作用。

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