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对曲坦类药物治疗偏头痛发作的多组学分析为分子机制提供了深入了解。

Multi-omic analyses of triptan-treated migraine attacks gives insight into molecular mechanisms.

机构信息

Department of Neurology, Danish Headache Center, Copenhagen University Hospital, Glostrup, Denmark.

Department of Congenital Disorders, Section for Clinical Mass Spectrometry, Danish Center for Neonatal Screening, Statens Serum Institut, Copenhagen, Denmark.

出版信息

Sci Rep. 2023 Jul 31;13(1):12395. doi: 10.1038/s41598-023-38904-1.

Abstract

Migraine is a common, polygenic disorder that is characterized by moderate to severe headache attacks. Migraine attacks are commonly treated with triptans, i.e. serotonin receptor agonists. However, triptans are effective in ~ 60% of the population, and the mechanisms of triptans are debated. Here, we aim to expose the mechanisms of triptan using metabolomics and transcriptomics in spontaneous migraine attacks. We collected temporal multi-omics profiles on 24 migraine patients, using samples collected at a migraine attack, 2 h after treatment with a triptan, when headache-free, and after a cold-pressor test. Differential metabolomic analysis was performed to find metabolites associated with treatment. Their effect was further investigated using correlation analysis and a machine learning approach. We found three differential metabolites: cortisol, sumatriptan and glutamine. The change in sumatriptan levels correlated with a change in GNAI1 and VIPR2 gene expression, both known to regulate cAMP levels. Furthermore, we found fatty acid oxidation to be affected, a mechanism known to be involved in migraine but not previously found in relation to triptans. In conclusion, using an integrative approach we find evidence for a role of glutamine, cAMP regulation, and fatty acid oxidation in the molecular mechanisms of migraine and/or the effect of triptans.

摘要

偏头痛是一种常见的多基因疾病,其特征是中度至重度头痛发作。偏头痛发作通常用曲坦类药物(即 5-羟色胺受体激动剂)治疗。然而,曲坦类药物在约 60%的人群中有效,其作用机制仍存在争议。在这里,我们旨在使用代谢组学和转录组学研究自发性偏头痛发作中曲坦类药物的作用机制。我们对 24 名偏头痛患者进行了时间性多组学分析,在偏头痛发作时、曲坦类药物治疗 2 小时后头痛缓解时以及冷压测试后采集样本。我们进行了差异代谢组学分析,以寻找与治疗相关的代谢物。使用相关分析和机器学习方法进一步研究它们的作用。我们发现了三种差异代谢物:皮质醇、舒马曲坦和谷氨酰胺。舒马曲坦水平的变化与 GNAI1 和 VIPR2 基因表达的变化相关,这两种基因都已知能调节 cAMP 水平。此外,我们发现脂肪酸氧化受到影响,这一机制已知与偏头痛有关,但以前与曲坦类药物无关。总之,我们采用综合方法发现谷氨酰胺、cAMP 调节和脂肪酸氧化在偏头痛的分子机制和/或曲坦类药物的作用中发挥作用的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/92a7/10390468/6336705cb455/41598_2023_38904_Fig1_HTML.jpg

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