首页> 外文OA文献 >Ictal lack of binding to brain parenchyma suggests integrity of the blood-brain barrier for 11C-dihydroergotamine during glyceryl trinitrate-induced migraine.
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Ictal lack of binding to brain parenchyma suggests integrity of the blood-brain barrier for 11C-dihydroergotamine during glyceryl trinitrate-induced migraine.

机译:局部缺乏与脑实质的结合,提示在三硝酸甘油酯诱导的偏头痛过程中11C-二氢麦角胺的血脑屏障完整性。

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摘要

SEE DREIER DOI 101093/AWW112 FOR A SCIENTIFIC COMMENTARY ON THIS ARTICLE: For many decades a breakdown of the blood-brain barrier has been postulated to occur in migraine. Hypothetically this would facilitate access of medications, such as dihydroergotamine or triptans, to the brain despite physical properties otherwise restricting their entry. We studied the permeability of the blood-brain barrier in six migraineurs and six control subjects at rest and during acute glyceryl trinitrate-induced migraine attacks using positron emission tomography with the novel radioligand (11)C-dihydroergotamine, which is chemically identical to pharmacologically active dihydroergotamine. The influx rate constant Ki, average dynamic image and time activity curve were assessed using arterial blood sampling and served as measures for receptor binding and thus blood-brain barrier penetration. At rest, there was binding of (11)C-dihydroergotamine in the choroid plexus, pituitary gland, and venous sinuses as expected from the pharmacology of dihydroergotamine. However, there was no binding to the brain parenchyma, including the hippocampus, the area with the highest density of the highest-affinity dihydroergotamine receptors, and the raphe nuclei, a postulated brainstem site of action during migraine, suggesting that dihydroergotamine is not able to cross the blood-brain barrier. This binding pattern was identical in migraineurs during glyceryl trinitrate-induced migraine attacks as well as in matched control subjects. We conclude that (11)C-dihydroergotamine is unable to cross the blood-brain barrier interictally or ictally demonstrating that the blood-brain barrier remains tight for dihydroergotamine during acute glyceryl trinitrate-induced migraine attacks.
机译:有关此文章的科学评论,请参见DREIER DOI 101093 / AWW112:几十年来,人们一直认为偏头痛会导致血脑屏障的破坏。从理论上讲,这将有助于药物(例如二氢麦角胺或曲普坦)进入大脑,尽管物理性质会限制其进入。我们使用正电子发射断层显像和新型放射性配体(11)C-二氢麦角胺,研究了六名偏头痛患者和六名对照受试者在休息时以及在急性三硝酸甘油酯诱发的偏头痛发作期间血脑屏障的通透性,其化学性质与药理活性相同二氢麦角胺。使用动脉血采样评估流入速率常数Ki,平均动态图像和时间活动曲线,并用作受体结合和血脑屏障渗透的量度。静息时,如双氢麦角胺药理学所预期的,在脉络丛,垂体和静脉窦中存在(11)C-二氢麦角胺的结合。但是,与脑实质之间没有结合,包括海马体(具有最高亲和力的二氢麦角胺受体的最高密度的区域)和沟缝核(偏头痛期间假定的脑干作用位点),表明二氢麦角胺不能穿越血脑屏障。在三硝酸甘油酯引起的偏头痛发作期间,偏头痛患者以及在相匹配的对照受试者中,这种结合模式是相同的。我们得出的结论是,(11)C-二氢麦角胺无法在肠壁或冰壁上穿过血脑屏障,这表明在三硝酸甘油酯诱发的偏头痛发作期间血脑屏障对于二氢麦角胺仍然很紧。

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