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一种与过度解读恐惧反应有关的神经肽 S 受体变体:灾难化的潜在神经遗传学基础。

A neuropeptide S receptor variant associated with overinterpretation of fear reactions: a potential neurogenetic basis for catastrophizing.

机构信息

Institute for Systems Neuroscience, University Medical Center Hamburg-Eppendorf (UKE), Hamburg, Germany.

出版信息

Mol Psychiatry. 2010 Nov;15(11):1045, 1067-74. doi: 10.1038/mp.2010.79. Epub 2010 Jul 13.

Abstract

Neuropeptide S (NPS) is a recently discovered G protein-coupled receptor ligand that modulates fear-like behaviors in rodents. A frequent A>T single-nucleotide polymorphism in the human NPS receptor gene NPSR1 confers a 10-fold higher efficacy of NPS signaling in vitro and has been linked with panic disorder (PD). We here report data from a classical fear-conditioning paradigm in healthy normal volunteers, in which carriers of the NPSR1 T allele evaluated their fear reactions to conditioned stimuli (CSs) as more pronounced than AA homozygous participants, although they did not show elevated peripheral-physiological conditioned responses (skin conductance responses-SCRs). T carriers also exhibited stronger CS-evoked brain activity in the rostral dorsomedial prefrontal cortex (dmPFC), an area that supports the explicit, conscious appraisal of threat stimuli. By contrast, more caudally situated mid-dmPFC, which has previously been associated with the generation of SCRs, showed no elevated response. Moreover, rostral dmPFC activation was correlated with participants' fear evaluations, further strengthening the link of this activation to increased individual fear appraisal. Our data suggest a genetic and neuroanatomical substrate for catastrophizing overinterpretations of fear reactions and provide a mechanistic explanation for the association between the NPSR1 T allele and PD.

摘要

神经肽 S(NPS)是一种新发现的 G 蛋白偶联受体配体,可调节啮齿动物的类似恐惧行为。人类 NPS 受体基因 NPSR1 中的一个常见 A>T 单核苷酸多态性赋予了 NPS 信号在体外的 10 倍更高的功效,并且与惊恐障碍(PD)有关。我们在此报告了一项健康正常志愿者的经典恐惧条件反射范式的数据,其中 NPSR1 T 等位基因的携带者对条件刺激(CS)的恐惧反应评估比 AA 纯合子参与者更为明显,尽管他们没有表现出外周生理条件反应(皮肤电导反应-SCR)升高。T 携带者在额背内侧前额皮质(dmPFC)的前背侧也表现出更强的 CS 诱发脑活动,该区域支持对威胁刺激的明确,有意识的评估。相比之下,以前与 SCR 生成相关的更靠尾的 dmPFC 没有显示出升高的反应。此外,前 dmPFC 的激活与参与者的恐惧评估相关,进一步加强了这种激活与个体恐惧评估增加之间的联系。我们的数据表明,NPSR1 T 等位基因与 PD 之间的关联提供了对恐惧反应的灾难性过度解释的遗传和神经解剖学基础。

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