肾上腺素能受体刺激在离体豚鼠神经炎症致敏性抑郁样行为中的作用

IF 2.6 4区心理学 Q2 BEHAVIORAL SCIENCES

Stress-The International Journal on the Biology of Stress Pub Date : 2023-11-01 DOI:10.1080/10253890.2023.2239366

Rachel R Kessler, Patricia A Schiml, Sean M McGraw, Erin N Tomlin, Mikayla J Hoeferlin, Terrence Deak, Michael B Hennessy

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引用次数: 0

摘要

早期生活依恋中断似乎会使神经炎症信号敏感，从而增加日后患压力相关精神障碍（包括抑郁症）的脆弱性。压力是如何启动这一过程的尚不清楚，但对成年大鼠和小鼠的研究表明，早期压力期间交感神经系统的激活和/或皮质醇的升高是关键。与母亲分离的豚鼠幼崽表现出最初的活跃行为阶段，其特征是类似焦虑的发声。随后是炎症依赖性抑郁样行为和对反复隔离敏感的发烧。使用在成人研究中成功的策略，我们评估了交感神经系统活动和皮质醇是否对豚鼠幼崽的致敏过程有贡献。在实验1中，肾上腺素能激动剂麻黄碱（3或10 mg/kg），单独或与皮质醇（2.5 mg/kg），在第二天的初始隔离期间没有增加抑郁样行为或发烧，如果这种刺激足以解释致敏过程，则可能会增加。在实验2中，抑郁样行为和发烧都因反复隔离而敏感，但用普萘洛尔阻断β肾上腺素能受体（10或20 mg/kg）不影响这些反应或它们的致敏性。然而，高剂量的普萘洛尔确实减少了发声。这些结果表明，交感神经系统的激活既不必要也不足以诱导发育中豚鼠抑郁样行为或发热反应致敏的假定神经炎症信号。因此，在该模型中，介导早期生活依恋中断后基于神经炎症的抑郁样行为致敏的过程似乎与先前发现的成人神经炎症引发的过程不同。

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Examination of the role of adrenergic receptor stimulation in the sensitization of neuroinflammatory-based depressive-like behavior in isolated Guinea pig pups.

Early-life attachment disruption appears to sensitize neuroinflammatory signaling to increase later vulnerability for stress-related mental disorders, including depression. How stress initiates this process is unknown, but studies with adult rats and mice suggest sympathetic nervous system activation and/or cortisol elevations during the early stress are key. Guinea pig pups isolated from their mothers exhibit an initial active behavioral phase characterized by anxiety-like vocalizing. This is followed by inflammatory-dependent depressive-like behavior and fever that sensitize on repeated isolation. Using strategies that have been successful in adult studies, we assessed whether sympathetic nervous system activity and cortisol contributed to the sensitization process in guinea pig pups. In Experiment 1, the adrenergic agonist ephedrine (3 or 10 mg/kg), either alone or with cortisol (2.5 mg/kg), did not increase depressive-like behavior or fever during initial isolation the following day as might have been expected to if this stimulation was sufficient to account for the sensitization process. In Experiment 2, both depressive-like behavior and fever sensitized with repeated isolation, but beta-adrenergic receptor blockade with propranolol (10 or 20 mg/kg) did not affect either of these responses or their sensitization. The high dose of propranolol did, however, reduce vocalizing. These results suggest sympathetic nervous system activation is neither necessary nor sufficient to induce the presumptive neuroinflammatory signaling underlying sensitization of depressive-like behavioral or febrile responses in developing guinea pigs. Thus, processes mediating sensitization of neuroinflammatory-based depressive-like behavior following early-life attachment disruption in this model appear to differ from those previously found to underlie neuroinflammatory priming in adults.

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来源期刊

Stress-The International Journal on the Biology of Stress 医学-行为科学

CiteScore

5.60

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： The journal Stress aims to provide scientists involved in stress research with the possibility of reading a more integrated view of the field. Peer reviewed papers, invited reviews and short communications will deal with interdisciplinary aspects of stress in terms of: the mechanisms of stressful stimulation, including within and between individuals; the physiological and behavioural responses to stress, and their regulation, in both the short and long term; adaptive mechanisms, coping strategies and the pathological consequences of stress. Stress will publish the latest developments in physiology, neurobiology, molecular biology, genetics research, immunology, and behavioural studies as they impact on the understanding of stress and its adverse consequences and their amelioration. Specific approaches may include transgenic/knockout animals, developmental/programming studies, electrophysiology, histochemistry, neurochemistry, neuropharmacology, neuroanatomy, neuroimaging, endocrinology, autonomic physiology, immunology, chronic pain, ethological and other behavioural studies and clinical measures.