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首页> 外文期刊>Biological psychiatry >Assessment of the neuropeptide S system in anxiety disorders.
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Assessment of the neuropeptide S system in anxiety disorders.

机译:焦虑症中神经肽S系统的评估。

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摘要

BACKGROUND: The G protein-coupled receptor neuropeptide S receptor 1 (NPSR1) and its ligand neuropeptide S (NPS) form a signaling system mainly implicated in susceptibility to asthma and inflammatory disorders in humans and regulation of anxiety and arousal in rodents. We addressed here the role of NPS and NPSR1 as susceptibility genes for human anxiety disorders. METHODS: We performed comprehensive association analysis of genetic variants in NPS and NPSR1 in three independent study samples. We first studied a population-based sample (Health 2000, Finland) of 321 anxiety disorder patients and 1317 control subjects and subsequently a Spanish clinical panic disorder sample consisting of 188 cases and 315 control subjects. In addition, we examined a birth cohort of 2020 children (Barn Allergi Miljo Stockholm Epidemiologi [BAMSE], Sweden). We then tested whether alleles of the most significantly associated single nucleotide polymorphisms alter DNA-protein complex formation in electrophoretic mobility shift assays. Finally, we compared acute stress responses on the gene expression level in wild-type and Npsr1(-/-) mice. RESULTS: We confirmed previously observed epidemiological association between anxiety and asthma in two population-based cohorts. Single nucleotide polymorphisms within NPS and NPSR1 associated with panic disorder diagnosis in the Finnish and Spanish samples and with parent-reported anxiety/depression in the BAMSE sample. Moreover, some of the implicated single nucleotide polymorphisms potentially affect transcription factor binding. Expression of neurotrophin-3, a neurotrophic factor connected to stress and panic reaction, was significantly downregulated in brain regions of stressed Npsr1(-/-) mice, whereas interleukin-1 beta, an active stress-related immunotransmitter, was upregulated. CONCLUSIONS: Our results suggest that NPS-NPSR1 signaling is likely involved in anxiety.
机译:背景:G蛋白偶联受体神经肽S受体1(NPSR1)及其配体神经肽S(NPS)形成信号系统,主要涉及人类对哮喘和炎性疾病的易感性以及啮齿动物焦虑和唤醒的调节。我们在这里讨论了NPS和NPSR1作为人类焦虑症易感基因的作用。方法:我们在三个独立的研究样本中对NPS和NPSR1的遗传变异进行了全面的关联分析。我们首先研究了以人群为基础的样本(2000年,芬兰健康),研究了321名焦虑症患者和1317名对照受试者,然后研究了由188名病例和315名对照受试者组成的西班牙临床恐慌症样本。此外,我们检查了2020名儿童的出生队列(瑞典的Barn Allergi Miljo Stockholm Epidemiologi [BAMSE])。然后,我们在电泳迁移率迁移分析中测试了最显着相关的单核苷酸多态性的等位基因是否改变了DNA-蛋白质复合物的形成。最后,我们比较了野生型和Npsr1(-/-)小鼠中基因表达水平的急性应激反应。结果:我们证实了先前在两个基于人群的队列中观察到的焦虑与哮喘之间的流行病学关联。 NPS和NPSR1中的单核苷酸多态性与芬兰和西班牙样本中的恐慌症诊断以及BAMSE样本中父母报告的焦虑/抑郁症有关。而且,一些牵连的单核苷酸多态性潜在地影响转录因子结合。在应激的Npsr1(-/-)小鼠的大脑区域中,neurotrophin-3(一种与压力和惊恐反应相关的神经营养因子)的表达显着下调,而白细胞介素1β(一种与应激相关的主动免疫递质)被上调。结论:我们的结果表明,NPS-NPSR1信号可能与焦虑有关。

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