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Thalamic contributions to psychosis susceptibility: Evidence from co‐activation patterns accounting for intra‐seed spatial variability (μCAPs)

机译:丘脑对精神病易感性的贡献:来自解释种子内空间变异性 (μCAPs) 的共激活模式的证据

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摘要

The temporal variability of the thalamus in functional networks may provide valuable insights into the pathophysiology of schizophrenia. To address the complexity of the role of the thalamic nuclei in psychosis, we introduced micro‐co‐activation patterns (μCAPs) and employed this method on the human genetic model of schizophrenia 22q11.2 deletion syndrome (22q11.2DS). Participants underwent resting‐state functional MRI and a data‐driven iterative process resulting in the identification of six whole‐brain μCAPs with specific activity patterns within the thalamus. Unlike conventional methods, μCAPs extract dynamic spatial patterns that reveal partially overlapping and non‐mutually exclusive functional subparts. Thus, the μCAPs method detects finer foci of activity within the initial seed region, retaining valuable and clinically relevant temporal and spatial information. We found that a μCAP showing co‐activation of the mediodorsal thalamus with brain‐wide cortical regions was expressed significantly less frequently in patients with 22q11.2DS, and its occurrence negatively correlated with the severity of positive psychotic symptoms. Additionally, activity within the auditory–visual cortex and their respective geniculate nuclei was expressed in two different μCAPs. One of these auditory–visual μCAPs co‐activated with salience areas, while the other co‐activated with the default mode network (DMN). A significant shift of occurrence from the salience+visuo‐auditory‐thalamus to the DMN + visuo‐auditory‐thalamus μCAP was observed in patients with 22q11.2DS. Thus, our findings support existing research on the gatekeeping role of the thalamus for sensory information in the pathophysiology of psychosis and revisit the evidence of geniculate nuclei hyperconnectivity with the audio‐visual cortex in 22q11.2DS in the context of dynamic functional connectivity, seen here as the specific hyper‐occurrence of these circuits with the task‐negative brain networks.
机译:丘脑在功能网络中的时间变异性可能为精神分裂症的病理生理学提供有价值的见解。为了解决丘脑核在精神病中作用的复杂性,我们引入了微共激活模式 (μCAP),并将这种方法用于精神分裂症 22q11.2 缺失综合征 (22q11.2DS) 的人类遗传模型。参与者接受了静息态功能 MRI 和数据驱动的迭代过程,从而确定了丘脑内具有特定活动模式的 6 个全脑 μCAP。与传统方法不同,μCAP 提取动态空间模式,揭示部分重叠和非互斥的功能子部分。因此,μCAPs 方法可以检测初始种子区域内更精细的活性焦点,保留有价值且具有临床相关性的时间和空间信息。我们发现,在 22q11.2DS 患者中,显示中背丘脑与全脑皮质区域共激活的 μCAP 的表达频率显著降低,并且其发生与阳性精神病症状的严重程度呈负相关。此外,听觉-视觉皮层及其各自的膝状核内的活动在两个不同的 μCAP 中表达。其中一个听觉-视觉 μCAP 与显著区域共激活,而另一个与默认模式网络 (DMN) 共激活。在 22q11.2DS 患者中观察到从显著性 + 视觉-听觉-丘脑到 DMN + 视觉-听觉-丘脑 μCAP 的发生率显着转变。因此,我们的研究结果支持关于丘脑在精神病病理生理学中感觉信息的把关作用的现有研究,并在动态功能连接的背景下重新审视了 22q11.2DS 中膝状核与视听皮层超连接的证据,这里被视为这些回路与任务负脑网络的特定过度发生。

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