应激后调节HPA和黑素皮质素系统减轻小鼠偏头痛样行为。

IF 4.6 2区 医学 Q1 CLINICAL NEUROLOGY
Cephalalgia Pub Date : 2025-07-01 Epub Date: 2025-07-09 DOI:10.1177/03331024251352856
Ya-Yu Hu, Hao-Ruei Mei, Shruti Sankar, Abbas Pirwani, Armen Akopian, Christa McIntyre, Gregory Dussor
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引用次数: 0

摘要

压力是偏头痛发作的主要诱因。压力激活下丘脑-垂体-肾上腺(HPA)轴,释放糖皮质激素(GCs)来维持体内平衡,偏头痛发作可能是这种反应的副作用。我们之前在小鼠模型中证明,在应激前通过给予美曲酮抑制皮质酮(CORT)合成可以防止应激诱导的偏头痛样行为。鉴于应激源的不可预测性及其开始或终止,更好地理解HPA应激反应的适应和不适应效应至关重要。在此,我们旨在评估应激结束后下丘脑轴调制的影响。方法反复应激诱导小鼠偏头痛样行为及对硝普钠(SNP)的启动。应激后给药Metyrapone(抑制CORT合成),CORT(评估外源性给药后的作用)和促肾上腺皮质激素(ACTH)(测试CORT上游激素的作用)。此外,α-促黑素细胞激素(α-MSH, ACTH切割产物)和四氢异喹啉(THIQ),一种黑素皮质素4受体(MC4R)激动剂,被给予检查黑素皮质素受体的参与。面部过敏通过von Frey测试评估,鬼脸评分用于评估非诱发性疼痛。在给药ACTH后,分别测量对照组和应激小鼠的血清CORT水平。结果观察应激后HPA轴对应激性面部超敏反应的调节作用。Metyrapone减少急性期超敏反应和SNP的启动,提示应激后持续合成CORT在偏头痛样行为的发展中起作用。令人惊讶的是,应激后1和24小时的CORT和ACTH处理均可缓解应激诱导的行为和启动。为了确定ACTH的作用是否由循环CORT升高介导,在ACTH注射前给药metyrapone。甲替拉酮可增强应激对面部超敏反应的ACTH逆转作用。此外,应激后注射ACTH可显著提高30分钟内血清CORT水平。除了ACTH对CORT水平的影响外,ACTH的影响可能由黑素皮质素系统介导。应激后给予α-MSH或MC4R激动剂THIQ,可减少偏头痛样行为。结论反复应激对偏头痛样行为的影响存在应激、下丘脑轴和黑素皮质素信号传导之间的复杂关系。在应激反应后的早期阶段,CORT和MC4R信号都参与了行为效应的维持。这些发现提示应激后靶向HPA轴和MC4R可能是应激性偏头痛发作的潜在治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Post-stress modulation of the HPA and melanocortin systems alleviates migraine-like behaviors in mice.

BackgroundStress is a major trigger for migraine attacks. Stress activates the hypothalamic-pituitary-adrenal (HPA) axis, releasing glucocorticoids (GCs) to maintain homeostasis, and migraine attacks may occur as an adverse effect of this response. We previously demonstrated in a mouse model that inhibiting corticosterone (CORT) synthesis by administering metyrapone before stress prevented stress-induced migraine-like behaviors. Given the unpredictable nature of stressors and their onset or termination, it is critical to better understand the adaptive and maladaptive effects of the HPA stress response. Here, we aimed to evaluate the effects of HPA axis modulation following the end of stress exposure.MethodsRepeated stress induces migraine-like behaviors and priming to sodium nitroprusside (SNP) in mice. Metyrapone (to inhibit CORT synthesis), CORT (to evaluate its effects after exogenous administration), and adrenocorticotropic hormone (ACTH) (to test the effects of a hormone upstream to CORT) were administered post-stress. Additionally, α-melanocyte-stimulating hormone (α-MSH, an ACTH cleavage product) and tetrahydroisoquinoline (THIQ), a melanocortin 4 receptor (MC4R) agonist, were administered to examine melanocortin receptor involvement. Facial hypersensitivity was assessed via von Frey testing and grimace scoring was used to evaluate non-evoked pain. Serum CORT levels were measured in both control and stressed mice following ACTH administration.ResultsWe examined post-stress HPA axis modulation on stress-induced facial hypersensitivity. Metyrapone reduced acute-phase hypersensitivity and reduced priming to SNP, suggesting sustained synthesis of CORT after stress plays a role in development of migraine-like behavior. Surprisingly, both CORT and ACTH treatments at 1- and 24-h post-stress alleviated stress-induced behaviors and priming. To determine if ACTH effects were mediated by an elevation in circulating CORT, metyrapone was administered before the ACTH injection. Metyrapone increased the ACTH reversal of stress effects on facial hypersensitivity. Furthermore, post-stress ACTH injections significantly increased serum CORT levels within 30 min. In addition to ACTH effects on CORT levels, ACTH effects could be mediated by the melanocortin system. Post-stress administration of α-MSH or the MC4R agonist THIQ, reduced migraine-like behaviors.ConclusionsThere is a complex relationship between stress, the HPA axis, and melanocortin signaling, in the effects of repeated stress exposure on migraine-like behaviors. In the early post-stress response phase, there are contributions from both CORT and MC4R signaling in the maintenance of behavioral effects. These findings suggest that targeting the HPA axis and MC4R after stress may be a potential therapeutic approach for stress-induced migraine attacks.

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来源期刊
Cephalalgia
Cephalalgia 医学-临床神经学
CiteScore
10.10
自引率
6.10%
发文量
108
审稿时长
4-8 weeks
期刊介绍: Cephalalgia contains original peer reviewed papers on all aspects of headache. The journal provides an international forum for original research papers, review articles and short communications. Published monthly on behalf of the International Headache Society, Cephalalgia''s rapid review averages 5 ½ weeks from author submission to first decision.
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