Occurrence of new or more severe headaches following COVID-19 is associated with markers of microglial activation and peripheral sensitization: results from a prospective cohort study.

IF 7.3 1区 医学 Q1 CLINICAL NEUROLOGY
Johanna Ruhnau, Max Blücher, Susanne Bahlmann, Almut Zieme, Antje Vogelgesang, Anke Steinmetz, Robert Fleischmann
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引用次数: 0

Abstract

Background: New onset or worsening of a headache disorder substantially contributes to the disease burden of post-COVID-19. Its management poses a suitable means to enhance patients' participation in professional, social, and personal activities. Unfortunately, the pathophysiology of post-COVID-19 headaches is poorly understood. This study aims to investigate the role of (neuro-) inflammatory mechanisms in order to guide the development of anti-inflammatory treatment strategies.

Methods: We included patients from the interdisciplinary post-COVID-19 Rehabilitation Study (PoCoRe, n = 184 patients) run at a tertiary care university hospital, comprising patients with PCR-confirmed SARS-CoV-2 infection ≥ 6 weeks prior to their initial consultation. Patients reporting any headache since their infection were considered for this study (n = 93). These were interviewed and classified according to the International Classification of Headache Disorders, Third Edition (ICHD-3) by headache specialists. Patient sera were additionally analysed for levels of VILIP-1, MCP-1 (CCL2), sTREM-2, BDNF, TGF-ß1, VEGF, IL-6, sTREM-1, ß-NGF, IL-18, TNF-alpha, sRAGE, and CX3CL1 (Fractalkine). Markers of inflammation were compared between four groups of patients (none, unchanged, worsened, or new headache disorder).

Results: Patients reported experiencing more severe headaches (n = 17), new onset headaches (n = 46), unchanged headaches (n = 18), and surprisingly, some patients denied having any headaches (n = 12) despite self-reports. Serum levels of CX3CL1 were increased in the worsened (2145 [811-4866] pg/ml) and new onset (1668 [0-7357] pg/ml) headache group as compared to patients with no (1129 [0-5379] pg/ml) or unchanged (1478 [346-4332] pg/ml) headaches. Other markers also differed between groups, but most significantly between patients with worsened (TGF-ß1: 60 [0-310] pg/ml, VEGF: 328 [86-842] pg/ml, ß-NGF: 6 [3-38] pg/ml) as compared to unchanged headaches (TGF-ß1: 29 [0-77] pg/ml, VEGF: 183 [72-380] pg/ml, ß-NGF: 3 [2-89] pg/ml). The results did not differ between headache phenotypes.

Discussion: This study provides evidence that worsened or new headaches following COVID-19 are associated with pro-(neuro-)inflammatory profiles. This supports the use of anti-inflammatory treatment options in this population, especially in the subacute phase.

COVID-19 后出现新的或更严重的头痛与小胶质细胞活化和外周敏化标志物有关:一项前瞻性队列研究的结果。
背景:头痛疾病的新发或恶化在很大程度上加重了后 COVID-19 的疾病负担。治疗头痛是提高患者参与职业、社会和个人活动能力的适当手段。遗憾的是,人们对 COVID-19 后头痛的病理生理学知之甚少。本研究旨在探讨(神经)炎症机制的作用,以指导抗炎治疗策略的开发:我们从一家三甲大学医院开展的跨学科 COVID-19 后康复研究(PoCoRe,n = 184 名患者)中纳入了患者,这些患者在初诊前 PCR 证实感染 SARS-CoV-2 ≥ 6 周。本研究考虑了自感染以来报告过任何头痛的患者(n = 93)。头痛专家根据《国际头痛疾病分类》第三版(ICHD-3)对这些患者进行了访谈和分类。此外,还分析了患者血清中 VILIP-1、MCP-1 (CCL2)、sTREM-2、BDNF、TGF-ß1、VEGF、IL-6、sTREM-1、ß-NGF、IL-18、TNF-α、sRAGE 和 CX3CL1 (Fractalkine) 的水平。对四组患者(无、无变化、恶化或新头痛病)的炎症指标进行了比较:结果:患者报告了更严重的头痛(17 例)、新发头痛(46 例)、头痛症状不变(18 例),令人惊讶的是,尽管有自我报告,但一些患者否认有任何头痛(12 例)。与没有头痛(1129 [0-5379] pg/ml)或头痛程度不变(1478 [346-4332] pg/ml)的患者相比,头痛恶化组(2145 [811-4866] pg/ml)和新发头痛组(1668 [0-7357] pg/ml)患者血清中的 CX3CL1 水平升高。其他指标在不同组间也存在差异,但最显著的是恶化组患者(TGF-ß1:60 [0-310] pg/ml,VEGF:328 [86-842] pg/ml,ß-NGF:6 [3-38] pg/ml)与无变化组患者(TGF-ß1:29 [0-77] pg/ml,VEGF:183 [72-380] pg/ml,ß-NGF:3 [2-89] pg/ml)之间的差异。不同头痛表型的结果没有差异:讨论:本研究提供的证据表明,COVID-19 导致的头痛恶化或新头痛与促(神经)炎症特征有关。这支持在这类人群中使用抗炎治疗方案,尤其是在亚急性阶段。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Headache and Pain
Journal of Headache and Pain 医学-临床神经学
CiteScore
11.80
自引率
13.50%
发文量
143
审稿时长
6-12 weeks
期刊介绍: The Journal of Headache and Pain, a peer-reviewed open-access journal published under the BMC brand, a part of Springer Nature, is dedicated to researchers engaged in all facets of headache and related pain syndromes. It encompasses epidemiology, public health, basic science, translational medicine, clinical trials, and real-world data. With a multidisciplinary approach, The Journal of Headache and Pain addresses headache medicine and related pain syndromes across all medical disciplines. It particularly encourages submissions in clinical, translational, and basic science fields, focusing on pain management, genetics, neurology, and internal medicine. The journal publishes research articles, reviews, letters to the Editor, as well as consensus articles and guidelines, aimed at promoting best practices in managing patients with headaches and related pain.
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