Labastida-Ramirez Alejandro, Codadu Neela K, Agan Kagan, Wykes Robert C
Division of Neuroscience & Centre for Nanotechnology in Medicine, Faculty of Biology, Medicine, and Health, University of Manchester, Manchester, M13 9LT, UK.
Geoffrey Jefferson Brain Research Centre, Manchester Academic Health Science Centre, Northern Care Alliance NHS Foundation Trust, University of Manchester, Manchester, UK.
J Headache Pain. 2025 Aug 29;26(1):188. doi: 10.1186/s10194-025-02121-0.
Understanding the mechanisms of pathological brain network activity and the efficacy of therapies requires testing hypothesis in vivo, where brain circuitry remains preserved. Therefore, animal models are a key tool in the study of primary neurological disorders such as migraine, stroke and epilepsy. These models not only have advanced our understanding of the underlying neurobiology of these disorders but have also provided novel pharmacological targets and insights on shared pathophysiological processes such as spreading depolarizations (SD). SD, the electrographic correlate of migraine with aura, are transient waves of near-complete neuroglial depolarization associated with transmembrane ionic and water shifts. BODY: Many studies investigating the impact of SD in preclinical models have done so in the presence of anesthesia. However, the use of anesthesia is a well-known confounding factor that not only influences SD threshold or frequency but also SD-evoked hemodynamic responses as common anesthetics affect cerebral blood flow and neurovascular coupling, limiting translation. Therefore, here we discuss research methods that have recently been developed or refined to allow the study of SD in awake rodents with a focus on migraine with aura. We discuss advantages, limitations and also efforts made to transition towards minimally-invasive procedures. Methods include optogenetic approaches to induce SD, multisite high-fidelity DC-coupled electrophysiological recordings, and measurements of neurovascular signals detected at both mesoscopic/macroscopic (e.g., fluorescent reporters, functional ultrasound system) and microscopic levels (e.g., two-photon microscopy, miniscopes). Additionally, we discuss continuous wireless telemetry recordings to detect spontaneous SD frequency over weeks to months in freely moving animals.
Implementation of these methods in awake brain will close the translational gap and improve the relevance of preclinical animal models.
要了解病理性脑网络活动的机制和治疗效果,需要在体内测试假设,因为脑回路在体内得以保留。因此,动物模型是研究偏头痛、中风和癫痫等原发性神经系统疾病的关键工具。这些模型不仅加深了我们对这些疾病潜在神经生物学的理解,还提供了新的药理学靶点,并为诸如扩散性去极化(SD)等共同的病理生理过程提供了见解。SD是偏头痛伴先兆的脑电图相关表现,是与跨膜离子和水转移相关的近乎完全的神经胶质去极化的瞬态波。
许多在临床前模型中研究SD影响的研究都是在麻醉状态下进行的。然而,使用麻醉是一个众所周知的混杂因素,它不仅会影响SD阈值或频率,还会影响SD诱发的血流动力学反应,因为常见麻醉剂会影响脑血流量和神经血管耦合,从而限制了研究结果的转化。因此,在这里我们讨论最近开发或改进的研究方法,以便在清醒的啮齿动物中研究SD,重点是偏头痛伴先兆。我们讨论了这些方法的优点、局限性以及为向微创程序转变所做的努力。方法包括采用光遗传学方法诱导SD、多部位高保真直流耦合电生理记录,以及在介观/宏观水平(如荧光报告基因、功能超声系统)和微观水平(如双光子显微镜、微型显微镜)检测神经血管信号。此外,我们还讨论了连续无线遥测记录,以检测自由活动动物在数周数月内的自发SD频率。
在清醒大脑中实施这些方法将缩小转化差距,提高临床前动物模型的相关性。
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