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人类脑源性神经营养因子 rs6265 多态性作为情境性焦虑泛化的中介。

Human BDNF rs6265 polymorphism as a mediator for the generalization of contextual anxiety.

机构信息

Department of Psychology (Biological Psychology, Clinical Psychology and Psychotherapy), University of Würzburg, Würzburg, Germany.

Department of Psychiatry and Psychotherapy, Medical Center - Faculty of Medicine, University of Freiburg, Freiburg, Germany.

出版信息

J Neurosci Res. 2019 Mar;97(3):300-312. doi: 10.1002/jnr.24345. Epub 2018 Nov 7.

Abstract

The Met allele of the human brain-derived neurotrophic factor (BDNF) gene might be a risk factor for anxiety disorders and is associated with reduced hippocampal volume. Notably, hippocampus plays a crucial role in contextual learning and generalization. The role of the BDNF gene variation in human context-conditioning and generalization is still unknown. We investigated 33 carriers of the Met allele (18 females) and 32 homozygous carriers of the Val allele (15 females) with a virtual-reality context-conditioning paradigm. Electric stimulations (unconditioned stimulus, US) were unpredictably delivered in one virtual office (CTX+), but never in another virtual office (CTX-). During generalization, participants revisited CTX+ and CTX- and a generalization office (G-CTX), which was a mix of the other two. Rating data indicated successful conditioning (more negative valence, higher arousal, anxiety and contingency ratings for CTX+ than CTX-), and generalization of conditioned anxiety by comparable ratings for G-CTX and CTX+. The startle data indicated discriminative learning for Met allele carriers, but not for Val homozygotes. Moreover, a trend effect suggests that startle responses of only the Met carriers were slightly potentiated in G-CTX versus CTX-. In sum, the BDNF polymorphism did not affect contextual learning and its generalization on a verbal level. However, the physiological data suggest that Met carriers are characterized by fast discriminative contextual learning and a tendency to generalize anxiety responses to ambiguous contexts. We propose that such learning may be related to reduced hippocampal functionality and the basis for the risk of Met carriers to develop anxiety disorders.

摘要

人类脑源性神经营养因子(BDNF)基因的 Met 等位基因可能是焦虑障碍的风险因素,与海马体体积减小有关。值得注意的是,海马体在情景学习和泛化中起着至关重要的作用。BDNF 基因变异在人类情景条件作用和泛化中的作用尚不清楚。我们使用虚拟现实情景条件作用范式,调查了 33 名 Met 等位基因携带者(18 名女性)和 32 名 Val 等位基因纯合子携带者(15 名女性)。电刺激(非条件刺激,US)不可预测地在一个虚拟办公室(CTX+)中给予,但从未在另一个虚拟办公室(CTX-)中给予。在泛化过程中,参与者重新访问 CTX+和 CTX-以及一个泛化办公室(G-CTX),G-CTX 是其他两个办公室的混合。评分数据表明条件作用成功(CTX+的负性效价、唤醒度、焦虑和条件概率评分高于 CTX-),G-CTX 和 CTX+的焦虑评分相似,表明焦虑得到了泛化。惊跳数据表明,Met 等位基因携带者存在辨别性学习,但 Val 纯合子没有。此外,趋势效应表明,只有 Met 携带者的惊跳反应在 G-CTX 与 CTX-相比略有增强。总之,BDNF 多态性并未影响口头水平的情景学习及其泛化。然而,生理数据表明,Met 携带者的特点是快速辨别情景学习,以及将焦虑反应泛化到模糊情景的趋势。我们提出,这种学习可能与海马体功能降低有关,而 Met 携带者患焦虑障碍的风险则与之相关。

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