偏头痛发作时唾液 CGRP 水平的动态波动:与临床变量和表型特征的关联

Alicia Alpuente, Victor J. Gallardo, Laila Asskour, Edoardo Caronna, Marta Torres-Ferrus, Patricia Pozo-Rosich
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引用次数: 0

摘要

偏头痛是一种复杂的神经系统疾病,其临床表现和分子机制具有显著的异质性。降钙素基因相关肽(CGRP)已成为偏头痛病理生理学中的关键因素,但将其用作生物标志物仍面临挑战。本研究旨在调查偏头痛发作时唾液中的降钙素相关肽水平,并探讨其与临床变量之间的关联。研究人员从头痛门诊招募偏头痛患者,开展了一项前瞻性纵向试点研究。在发作间期、发作开始、发作后 2 小时和发作结束时测量唾液 CGRP 水平。利用广义线性混合模型,我们探讨了在有抑郁症状(DS)、急性发作治疗以及使用艾伦单抗治疗三个月后,CGRP 在发作过程中的变化所产生的影响。最后,我们根据 CGRP 表型对患者进行了分类和比较。研究共纳入44名偏头痛患者(90.9%为女性),分析了80次偏头痛发作。偏头痛发作时唾液 CGRP 水平升高。我们观察到 DS 与线性项 (Est. [SE]: 19.4 [5.8], p = 0.001) 和时间二次项 (-19.1 [6.0], p = 0.002) 之间存在统计学意义上的显著交互作用。此外,还发现在使用急性治疗发作时存在显著的三方交互作用(线性项:-18.5 [6.2],p = 0.005;二次项:19.2 [6.8],p = 0.005)。分子表型分析显示,72.7%(32/44)的患者仅表现为CGRP依赖性发作,而27.3%(12/44)的患者表现为非CGRP依赖性偏头痛发作。仅有 CGRP 依赖性发作的患者年龄较轻、疾病演变时间较短、先兆比例较高,每月头痛天数较少(P < 0.05)。对艾伦单抗治疗效果的探索性分析并未发现偏头痛发作时CGRP水平的变化。我们的研究强调了偏头痛在分子水平上的动态性质,并强调了结合临床变量(如抑郁症状)来理解偏头痛病理生理学的重要性。根据 CGRP 依赖性确定不同的偏头痛亚型为个性化治疗方法提供了潜在的机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Dynamic fluctuations of salivary CGRP levels during migraine attacks: association with clinical variables and phenotypic characterization
Migraine is a complex neurological disorder with significant heterogeneity in its clinical presentation and molecular mechanisms. Calcitonin gene-related peptide (CGRP) has emerged as a key player in migraine pathophysiology, but challenges remain in its utilization as a biomarker. This study aimed to investigate salivary CGRP levels during migraine attacks across the frequency spectrum and explore associations with clinical variables. A prospective longitudinal pilot study was conducted, recruiting migraine patients from an outpatient headache clinic. Salivary CGRP levels were measured at interictal, onset, post-2 h of onset and end-of-attack. Using generalized linear mixed models, we explored the effect of CGRP changes over the attack in presence of depressive symptoms (DS), acute attack treatment, and after three-months of erenumab treatment. Finally, patients were classified and compared according to their CGRP phenotype. A total of 44 migraine patients were included (90.9% women), with 80 migraine attacks analyzed. Salivary CGRP levels increased at the onset of migraine attacks. We observed statistically significant interactions between DS and both the linear (Est. [SE]: 19.4 [5.8], p = 0.001) and quadratic terms of time (-19.1 [6.0], p = 0.002). Additionally, a significant three-way interaction within the use of acute treated attack (linear-term: -18.5 [6.2], p = 0.005; quadratic-term: 19.2 [6.8], p = 0.005) was also found. Molecular phenotyping revealed that 72.7% (32/44) of patients presented only CGRP-dependent attacks, while 27.3% (12/44) presented non-CGRP-dependent migraine attacks. Patients with only CGRP-dependent attacks were associated with younger age, shorter disease evolution time, a higher proportion of aura, and fewer monthly headache days (p < 0.05). Exploratory analysis of erenumab treatment effects did not result in changes in CGRP levels during migraine attacks. Our study underscores the dynamic nature of migraine at a molecular level and emphasizes the importance of integrating clinical variables, such as depressive symptoms, in understanding its pathophysiology. The identification of distinct migraine subtypes based on CGRP dependence suggests potential opportunities for personalized treatment approaches.
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