Zhi-Cheng Zhu, Xue-Jing Han, Zhen He, Meng-Yang Liu, Ning Wu, Xiang-Min Tong, Fei Li
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In rodent models, exogenous NPS reduces anxiety- and fear-like behaviours, speeds fear-memory extinction, stabilises the hypothalamic-pituitary-adrenal axis, enhances dopaminergic tone and elevates hippocampal brain-derived neurotrophic factor (BDNF)-changes concordant with symptom relief. Additional work shows that NPS lessens pain affect, dampens alcohol and opioid intake, eases withdrawal-induced anxiety and lowers food consumption, hinting at a multimodal therapeutic profile. These effects converge on limbic and mid-brain circuits (amygdala, ventral tegmental area, locus coeruleus, paraventricular nucleus) and engage oxytocinergic, adenosinergic and endocannabinoid pathways. Translation remains limited by NPS's rapid degradation, poor blood-brain-barrier penetration and scarcity of brain-penetrant NPSR ligands, but advances in intranasal delivery, lipid-acylated analogues, biased NPSR agonists and \"humanised\" NPSR-variant models offer promising solutions. 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引用次数: 0
摘要
创伤后应激障碍(PTSD)是一种很少单独发生的多维疾病:大约80%的患者还符合焦虑、抑郁、慢性疼痛、药物使用、饮食或认知障碍的标准。遗传、神经化学和行为方面的研究结果表明,神经肽S (NPS)系统通过其g蛋白偶联的NPS受体(NPSR)发挥作用,是这些不同表型的共同调节剂。这篇叙述性综述调查了2000-2024年发表在PubMed、Embase和Web of Science上的研究,研究了NPS/NPSR与核心PTSD特征和典型合并症的关系。功能rs324981 A/T多态性,促进NPSR表面表达和信号传导,始终与更高的PTSD风险和症状严重程度相关。在啮齿动物模型中,外源性NPS减少焦虑和恐惧样行为,加速恐惧记忆消退,稳定下丘脑-垂体-肾上腺轴,增强多巴胺能张力,提高海马脑源性神经营养因子(BDNF)-与症状缓解一致的变化。进一步的研究表明,NPS减轻了疼痛影响,抑制了酒精和阿片类药物的摄入,缓解了戒断引起的焦虑,降低了食物消耗,这暗示了一种多模式的治疗方式。这些作用集中在边缘和中脑回路(杏仁核、腹侧被盖区、蓝斑核、室旁核),并参与催产素、腺苷能和内源性大麻素途径。翻译仍然受到NPS快速降解,血脑屏障穿透性差和脑渗透NPSR配体缺乏的限制,但鼻内递送,脂酰化类似物,偏倚NPSR激动剂和“人源化”NPSR变体模型的进展提供了有希望的解决方案。总的来说,目前的临床前和遗传证据将NPS-NPSR轴定位为核心PTSD症状及其致残合并症的多功能治疗靶点,需要严格的转化研究来完善机制,优化药物样特性和测试临床疗效。
Neuropeptide S pathway in PTSD and neuropsychiatric disorders: A review.
Post-traumatic stress disorder (PTSD) is a multidimensional illness that seldom occurs alone: roughly 80 % of patients also meet criteria for anxiety, depression, chronic pain, substance-use, eating or cognitive disorders. Converging genetic, neurochemical and behavioural findings implicate the neuropeptide S (NPS) system-acting through its G-protein-coupled NPS receptor (NPSR)-as a common regulator of these diverse phenotypes. This narrative review surveys studies published 2000-2024 in PubMed, Embase and Web of Science that examine NPS/NPSR involvement in core PTSD features and typical comorbidities. The functional rs324981 A/T polymorphism, which boosts NPSR surface expression and signalling, consistently associates with greater PTSD risk and symptom severity. In rodent models, exogenous NPS reduces anxiety- and fear-like behaviours, speeds fear-memory extinction, stabilises the hypothalamic-pituitary-adrenal axis, enhances dopaminergic tone and elevates hippocampal brain-derived neurotrophic factor (BDNF)-changes concordant with symptom relief. Additional work shows that NPS lessens pain affect, dampens alcohol and opioid intake, eases withdrawal-induced anxiety and lowers food consumption, hinting at a multimodal therapeutic profile. These effects converge on limbic and mid-brain circuits (amygdala, ventral tegmental area, locus coeruleus, paraventricular nucleus) and engage oxytocinergic, adenosinergic and endocannabinoid pathways. Translation remains limited by NPS's rapid degradation, poor blood-brain-barrier penetration and scarcity of brain-penetrant NPSR ligands, but advances in intranasal delivery, lipid-acylated analogues, biased NPSR agonists and "humanised" NPSR-variant models offer promising solutions. Collectively, current pre-clinical and genetic evidence positions the NPS-NPSR axis as a versatile therapeutic target for both core PTSD symptoms and their disabling comorbidities, warranting rigorous translational studies to refine mechanism, optimise drug-like properties and test clinical efficacy.
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