PACAP38/乳腺细胞特异性受体轴介导小鼠重复性压力诱发的头痛。

IF 7.3 1区医学 Q1 CLINICAL NEUROLOGY

Journal of Headache and Pain Pub Date : 2024-05-28 DOI:10.1186/s10194-024-01786-3

Hyeonwi Son, Yan Zhang, John Shannonhouse, Ruben Gomez, Yu Shin Kim

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引用次数: 0

摘要

背景：疼痛是一种在进化过程中得到保护的预警系统，它能让我们识别威胁，并促使我们适应这些威胁。偏头痛引起的头痛影响着全球约 15%的人口。然而，由于对偏头痛的发病机理知之甚少，偏头痛或头痛警告我们要避免的任何假定威胁的身份尚不清楚。在这里，我们发现压力诱导的垂体腺苷酸环化酶激活多肽-38（PACAP38）的增加会通过肥大细胞中与mas相关的G蛋白偶联受体B2（MrgprB2）引起雄性小鼠的头痛样行为：方法：通过重复应激模型和硬脑膜注射 PACAP38 来诱导头痛行为。我们使用面部冯弗雷试验和龇牙咧嘴量表评估了野生型小鼠和MrgprB2缺陷型小鼠的头痛行为。我们使用完整三叉神经节（TG）的活体 Pirt-GCaMP Ca2+ 成像进一步检查了三叉神经节神经元的活动：结果：重复应激和硬脑膜注射PACAP38可诱导MrgprB2依赖性头痛行为。重复应激后，血液中的 PACAP38 水平升高。PACAP38/MrgprB2诱导的肥大细胞脱颗粒使硬脑膜的三叉神经血管系统变得敏感。此外，利用体内完整三叉神经管 Pirt-GCaMP Ca2+ 成像，我们发现应激或/和 PACAP38 的升高通过 MrgprB2 使三叉神经管神经元敏感。缺失 MrgprB2 的小鼠没有表现出 TG 神经元的敏化或肥大细胞的激活。我们发现，重复应激和硬脑膜注射 PACAP38 可通过 TNF-a 和 TRPV1 通路诱导头痛行为：我们的研究结果突出表明，PACAP38-MrgprB2通路是治疗应激相关偏头痛的新靶点。此外，我们关于通过MrgprB2/PACAP38轴进行应激互感的研究结果表明，偏头痛向我们发出了应激引起的体内平衡失调的警告。

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PACAP38/mast-cell-specific receptor axis mediates repetitive stress-induced headache in mice.

Background: Pain, an evolutionarily conserved warning system, lets us recognize threats and motivates us to adapt to those threats. Headache pain from migraine affects approximately 15% of the global population. However, the identity of any putative threat that migraine or headache warns us to avoid is unknown because migraine pathogenesis is poorly understood. Here, we show that a stress-induced increase in pituitary adenylate cyclase-activating polypeptide-38 (PACAP38), known as an initiator of allosteric load inducing unbalanced homeostasis, causes headache-like behaviour in male mice via mas-related G protein-coupled receptor B2 (MrgprB2) in mast cells.

Methods: The repetitive stress model and dural injection of PACAP38 were performed to induce headache behaviours. We assessed headache behaviours using the facial von Frey test and the grimace scale in wild-type and MrgprB2-deficient mice. We further examined the activities of trigeminal ganglion neurons using in vivo Pirt-GCaMP Ca²⁺ imaging of intact trigeminal ganglion (TG).

Results: Repetitive stress and dural injection of PACAP38 induced MrgprB2-dependent headache behaviours. Blood levels of PACAP38 were increased after repetitive stress. PACAP38/MrgprB2-induced mast cell degranulation sensitizes the trigeminovascular system in dura mater. Moreover, using in vivo intact TG Pirt-GCaMP Ca²⁺ imaging, we show that stress or/and elevation of PACAP38 sensitized the TG neurons via MrgprB2. MrgprB2-deficient mice showed no sensitization of TG neurons or mast cell activation. We found that repetitive stress and dural injection of PACAP38 induced headache behaviour through TNF-a and TRPV1 pathways.

Conclusions: Our findings highlight the PACAP38-MrgprB2 pathway as a new target for the treatment of stress-related migraine headache. Furthermore, our results pertaining to stress interoception via the MrgprB2/PACAP38 axis suggests that migraine headache warns us of stress-induced homeostatic imbalance.

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来源期刊

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.