Tepper Stewart J, Stillman Mark J
Center for Headache and Pain, Department of Neurology, Neurological Institute, Cleveland Clinic Foundation, Cleveland, OH 44195, USA.
Headache. 2008 Sep;48(8):1259-68. doi: 10.1111/j.1526-4610.2008.01214.x.
Calcitonin gene-related peptide (CGRP) is linked to migraine and other primary headache disorders. It is found in every location described in migraine genesis and processing, including meninges, trigeminal ganglion, trigeminocervical complex, brainstem nuclei, and cortex. It is released in animal models following stimulation of the CNS similar to that seen in migraine, and triptans inhibit this release. Injection of CGRP into migraineurs results in delayed headache similar to migraine. Elevation of CGRP occurs during migraine, resolving following migraine-specific treatment. Finally, and most importantly, CGRP receptor antagonists terminate migraine with efficacy similar to triptans. Both intravenous olcegepant (BIBN 4096 BS) and oral telcagepant (MK-0974) have been effective, safe, and well tolerated in phase I and II studies. Telcagepant is currently in phase III trials, and preliminary results are favorable. The potential for a migraine-specific medication without vasoconstrictive or vascular side effects is enormous. CGRP receptor blockade may also have applications in other pathologic and pain syndromes.
降钙素基因相关肽(CGRP)与偏头痛及其他原发性头痛疾病相关。在偏头痛发生和进展的各个部位均能发现它,包括脑膜、三叉神经节、三叉神经颈复合体、脑干核团及皮质。在动物模型中,类似于偏头痛发作时中枢神经系统受到刺激的情况下,它会被释放出来,而曲坦类药物可抑制这种释放。向偏头痛患者体内注射CGRP会引发类似于偏头痛的延迟性头痛。偏头痛发作时CGRP水平会升高,经偏头痛特异性治疗后恢复正常。最后,也是最重要的一点,CGRP受体拮抗剂能够终止偏头痛发作,疗效与曲坦类药物相似。静脉注射olcegepant(BIBN 4096 BS)和口服telcagepant(MK - 0974)在I期和II期研究中均显示出有效、安全且耐受性良好。Telcagepant目前正处于III期试验阶段,初步结果令人满意。研发一种无血管收缩或血管副作用的偏头痛特异性药物潜力巨大。CGRP受体阻断在其他病理和疼痛综合征中可能也有应用。
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