将显著性信号与精神病临床高危人群的早期逆境和情感困扰联系起来:一项事件相关 fMRI 研究的结果。

Schizophrenia Bulletin Open Pub Date : 2022-06-17 eCollection Date: 2022-01-01 DOI:10.1093/schizbullopen/sgac039
Zachary B Millman, Jason Schiffman, James M Gold, LeeAnn Akouri-Shan, Caroline Demro, John Fitzgerald, Pamela J Rakhshan Rouhakhtar, Mallory Klaunig, Laura M Rowland, James A Waltz
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引用次数: 0

摘要

有证据表明,精神病患者的显著性网络出现了失调,但很少有研究对临床高危(CHR)青少年的压力暴露和情感困扰与预测错误(PE)信号的交叉点进行了研究。在此,26 名临床高危人群和 19 名健康志愿者(HVs)在完成货币激励延迟任务的同时进行了 fMRI 研究。我们比较了这两组人对出人意料的结果--不考虑其价值的出人意料的结果--的神经反应幅度,这些反应遍及整个大脑和两个感兴趣的区域,即前脑岛和杏仁核。然后,我们研究了这些信号与 CHR 组抑郁、焦虑和创伤史严重程度的关系。与 HV 相比,CHR 青少年颞顶叶交界处的 PE 诱发激活异常,而中央前回、岛叶后部和联想纹状体的失活较弱。在杏仁核或岛叶前部没有观察到组间差异。在CHR的青少年中,创伤史越多,PE诱发的杏仁核激活越强。情感症状与 PE 神经反应之间没有关联。我们的研究结果表明,未经证实的PE信号可能会提供有关CHR综合征神经生物学的独特信息,而早期的逆境暴露可能会导致这一群体的神经生物学异质性。我们需要对患有各种风险综合征的青少年进行纵向研究,以进一步厘清显著性信号的不同方面对精神病理学发展的贡献。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Linking Salience Signaling With Early Adversity and Affective Distress in Individuals at Clinical High Risk for Psychosis: Results From an Event-Related fMRI Study.

Linking Salience Signaling With Early Adversity and Affective Distress in Individuals at Clinical High Risk for Psychosis: Results From an Event-Related fMRI Study.

Linking Salience Signaling With Early Adversity and Affective Distress in Individuals at Clinical High Risk for Psychosis: Results From an Event-Related fMRI Study.

Linking Salience Signaling With Early Adversity and Affective Distress in Individuals at Clinical High Risk for Psychosis: Results From an Event-Related fMRI Study.

Evidence suggests dysregulation of the salience network in individuals with psychosis, but few studies have examined the intersection of stress exposure and affective distress with prediction error (PE) signals among youth at clinical high-risk (CHR). Here, 26 individuals at CHR and 19 healthy volunteers (HVs) completed a monetary incentive delay task in conjunction with fMRI. We compared these groups on the amplitudes of neural responses to surprising outcomes-PEs without respect to their valence-across the whole brain and in two regions of interest, the anterior insula and amygdala. We then examined relations of these signals to the severity of depression, anxiety, and trauma histories in the CHR group. Relative to HV, youth at CHR presented with aberrant PE-evoked activation of the temporoparietal junction and weaker deactivation of the precentral gyrus, posterior insula, and associative striatum. No between-group differences were observed in the amygdala or anterior insula. Among youth at CHR, greater trauma histories were correlated with stronger PE-evoked amygdala activation. No associations were found between affective symptoms and the neural responses to PE. Our results suggest that unvalenced PE signals may provide unique information about the neurobiology of CHR syndromes and that early adversity exposure may contribute to neurobiological heterogeneity in this group. Longitudinal studies of young people with a range of risk syndromes are needed to further disentangle the contributions of distinct aspects of salience signaling to the development of psychopathology.

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