双相情感障碍的特定情节和共同内在功能网络模式

X. Liu, Z.-Q. Liu, B. Wan, X. Zhang, L. Liu, J. Xiao, Y. Meng, S. Wang, C. Weng, Y. Gao
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引用次数: 0

摘要

了解双相情感障碍(BD)不同发作期(包括躁狂(BipM)、抑郁(BipD)和缓解状态(rBD))的大脑功能变化是一项重大挑战。在横断面研究中,我们收集了 117 名双相情感障碍患者(BipM:38 人;BipD:42 人;rBD:37 人)和 35 名健康对照者的静息态功能磁共振成像数据。我们的目的是确定与发作动态相关的功能连接,划分常见和特殊模式,将其验证为生物标记物,并阐明其生物学基础。最初,我们在腹侧注意网络的子区域内发现了一种常见的改变模式,同时还在默认模式网络(BipM)、前额叶网络(BipD)和边缘网络(rBD)中观察到了特定模式。利用人类连接组计划(Human Connectome Project)的大样本数据,我们进一步确定了这些连接模式具有相对较高的可靠性和遗传性。此外,这些独特的模式准确地描述了 BD 不同发作的特征,并有效地预测了与每种发作类型相关的临床症状。重要的是,通过使用样本外数据来解码这些模式背后可能的神经生物学机制,我们发现特别感兴趣的区域富含多种受体,包括特定改变的 MOR、NMDA 和 H3,以及常见改变的 A4B2、5HTT 和 5HT1a。此外,发作特异性和共同模式都显示出 L5ET、Micro/PVM、少突胶质细胞和 Chandelier 等细胞类型的高度富集。我们的研究提供了有关 BD 病程动态的新见解,为针对不同病程的个性化医疗方法铺平了道路。
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Episode-specific and common intrinsic functional network patterns in bipolar
Understanding the alterations in brain function across different episodes of bipolar disorder (BD), including manic (BipM), depressive (BipD), and remission states (rBD), poses a significant challenge. In our cross-sectional study, we collected resting-state functional magnetic resonance imaging data from 117 BD patients (BipM: 38, BipD: 42, rBD: 37) and 35 healthy controls. Our aim was to delineate functional connections associated with episode dynamics, delineate common and specific patterns, validate them as biomarkers, and elucidate their biological underpinnings. Initially, we identified a common altered pattern within the sub-regions of the ventral-attention network, alongside specific patterns observed in the default mode network for BipM, the prefrontal network for BipD, and the limbic network for rBD. Using large-sample data from the Human Connectome Project, we further identified that these connectivity patterns exhibit relatively high reliability and heritability. Also, these distinct patterns accurately characterized the diverse episodes of BD and effectively predicted the cor responding clinical symptoms linked with each episode type. Importantly, using out of sample data to decode possible neurobiological mechanisms underlying these patterns, we found that regions of particular interest were enriched in multiple receptors, including MOR, NMDA, and H3 for specific alterations, and A4B2, 5HTT, and 5HT1a for common alterations. Moreover, both episode-specific and common patterns demonstrated a high enrichment for cell types such as L5ET, Micro/PVM,oligodendrites and Chandelier. Our study offers novel insights concerning episode dynamics in BD, paving the way for personalized medicine approaches tailored to address the various episodes.
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