Department of Neurology, University Medicine Greifswald, Greifswald, Germany.
Physical and Rehabilitation Medicine, Center for Orthopaedics, Trauma Surgery and Rehabilitation Medicine, University Medicine Greifswald, Greifswald, Germany.
J Headache Pain. 2024 Jun 19;25(1):101. doi: 10.1186/s10194-024-01810-6.
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.
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).
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.
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.
新发或恶化的头痛障碍极大地增加了新冠后患者的疾病负担。对其进行管理是提高患者参与专业、社交和个人活动能力的合适手段。然而,新冠后头痛的病理生理学机制仍知之甚少。本研究旨在调查(神经)炎症机制的作用,以便为抗炎治疗策略的制定提供指导。
我们纳入了在一家三级护理大学医院进行的跨学科新冠后康复研究(PoCoRe)中的患者(n=184 名患者),这些患者的 PCR 检测确诊的 SARS-CoV-2 感染时间均在他们首次就诊前至少 6 周。研究纳入了自感染以来报告有任何头痛的患者(n=93)。这些患者由头痛专家进行访谈和分类,根据国际头痛疾病分类,第三版(ICHD-3)进行分类。另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。在四个患者组(无头痛、头痛无变化、头痛恶化和新发头痛障碍)之间比较了炎症标志物。
患者报告的头痛更严重(n=17)、新发头痛(n=46)、头痛无变化(n=18),令人惊讶的是,尽管有自我报告,但有些患者否认有任何头痛(n=12)。与无头痛(n=1129 [0-5379] pg/ml)或头痛无变化(n=1478 [346-4332] pg/ml)的患者相比,头痛恶化(2145 [811-4866] pg/ml)和新发头痛(1668 [0-7357] pg/ml)患者的血清 CX3CL1 水平升高。其他标志物在组间也存在差异,但在头痛恶化(TGF-ß1:60 [0-310] pg/ml,VEGF:328 [86-842] pg/ml,ß-NGF:6 [3-38] pg/ml)的患者与头痛无变化(TGF-ß1:29 [0-77] pg/ml,VEGF:183 [72-380] pg/ml,ß-NGF:3 [2-89] pg/ml)的患者之间差异最为显著。头痛表型之间的结果没有差异。
本研究提供的证据表明,新冠后新发或恶化的头痛与促(神经)炎症特征相关。这支持在该人群中使用抗炎治疗方案,尤其是在亚急性期。
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