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首页> 美国卫生研究院文献>British Journal of Pharmacology and Chemotherapy >Voltage-dependent calcium channels are involved in neurogenic dural vasodilatation via a presynaptic transmitter release mechanism
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Voltage-dependent calcium channels are involved in neurogenic dural vasodilatation via a presynaptic transmitter release mechanism

机译:电压依赖性钙通道通过突触前递质释放机制参与神经源性硬脑膜血管舒张

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class="enumerated" style="list-style-type:decimal">A missense mutation of the CACNA1A gene that encodes the α1A subunit of the voltage-dependent P/Q-type calcium channel has been discovered in patients suffering from familial hemiplegic migraine. This suggested that calcium channelopathies may be involved in migraine more broadly, and established the importance of genetic mechanisms in migraine.Channelopathies share many clinical characteristics with migraine, and thus exploring calcium channel functions in the trigeminovascular system may give insights into migraine pathophysiology. It is also known that drugs blocking the P/Q- and N-type calcium channels have been successful in other animal models of trigeminovascular activation and head pain.In the present study, we used intravital microscopy to examine the effects of specific calcium channel blockers on neurogenic dural vasodilatation and calcitonin gene-related peptide (CGRP)-induced dilation.The L-type voltage-dependent calcium channel blocker calciseptine significantly attenuated (20 μg kg−1, n=7) the dilation brought about by electrical stimulation, but did not effect CGRP-induced dural dilation.The P/Q-type voltage-dependent calcium channel blocker ω-agatoxin-IVA (20 μg kg−1, n=7) significantly attenuated the dilation brought about by electrical stimulation, but did not effect CGRP-induced dural dilation.The N-type voltage-dependent calcium channel blocker ω-conotoxin-GVIA (20 μg kg−1, n=8 and 40 μg kg−1, n=7) significantly attenuated the dilation brought about by electrical stimulation, but did not effect CGRP-induced dural dilation.It is thought that the P/Q-, N- and L-type calcium channels all exist presynaptically on trigeminovascular neurons, and blockade of these channels prevents CGRP release, and, therefore, dural blood vessel dilation. These data suggest that the P/Q-, N- and L-type calcium channels may be involved in trigeminovascular nociception.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 在患有家族性偏瘫性偏头痛的患者中发现了编码电压依赖性P / Q型钙通道的α1A亚基的CACNA1A基因的错义突变。这提示钙离子通道病可能更广泛地参与偏头痛,并确立了偏头痛的遗传机制的重要性。 通道病与偏头痛具有许多临床特征,因此探索三叉神经血管系统中的钙通道功能可能有助于偏头痛病理生理学的见解。众所周知,阻断P / Q和N型钙通道的药物在其他三叉神经血管激活和头部疼痛的动物模型中也很成功。 在本研究中,我们使用了活体显微镜检查钙通道阻滞剂对神经源性硬脑膜血管舒张和降钙素基因相关肽(CGRP)诱导的扩张的影响。 L型电压依赖性钙通道阻滞剂钙西肽明显减弱(20μgkg -1 ,n = 7)电刺激引起的扩张,但不影响CGRP引起的硬脑膜扩张。 P / Q型电压依赖性钙通道阻滞剂ω -agatoxin-IVA(20μgkg −1 ,n = 7)显着减弱电刺激引起的扩张,但不影响CGRP引起的硬脑膜扩张。 N型电压依赖性钙通道阻滞剂ω-芋螺毒素-GVIA(20μgkg -1 ,n = 8和40μgkg -1 ,n = 7) att抑制了电刺激所引起的扩张,但并未影响CGRP引起的硬脑膜扩张。 认为三叉神经血管神经元上P / Q,N和L型钙通道均先突性存在。并阻断这些通道可防止CGRP释放,从而阻止硬脑膜血管扩张。这些数据表明,P / Q,N和L型钙通道可能参与了三叉神经血管伤害感受。

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