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The Brain Network in a Model of Thalamocortical Dysrhythmia

机译:丘脑皮质心律失常模型中的脑网络

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摘要

Sensory information processing and higher cognitive functions rely on the interactions between thalamus and cortex. Many types of neurological and psychiatric disorders are accompanied or driven by alterations in the brain connectivity. In this study, putative changes in functional and effective corticocortical (CC), thalamocortical (TC), and corticothalamic (CT) connectivity during wakefulness and slow-wave sleep (SWS) in a model of thalamocortical dysrhythmia, TRIP8b−/− mice, and in control (wild-type or WT) mice are described. Coherence and nonlinear Granger causality (GC) were calculated for twenty 10 s length epochs of SWS and active wakefulness (AW) of each animal. Coherence was reduced between 4 and ca 20 Hz in the cortex and between cortex and thalamus during SWS compared with AW in WT but not in TRIP8b−/− mice. Moreover, TRIP8b−/− mice showed lower CT coherence during AW compared with WT mice; these differences were no longer present during SWS. Unconditional GC analysis also showed sleep-related reductions in TC and CT couplings in WT mice, while TRIP8b−/− mice showed diminished wake and enhanced sleep CC coupling and rather strong CT-directed coupling during wake and sleep, although smaller during sleep. Conditional GC coupling analysis confirmed the diminished CC and enhanced CT coupling in TRIP8b−/− mice. Our findings indicate that altered properties of hyperpolarization-activated cyclic nucleotide-gated cation channels, characterizing TRIP8b−/− mice, have clear effects on CC, TC, and CT networks. A more complete understanding of the function of the altered communication within these networks awaits detailed phenotyping of TRIP8b−/− mice aimed at specifics of sensory and attentional processes.
机译:感觉信息处理和更高的认知功能依赖于丘脑和皮层之间的相互作用。许多类型的神经系统疾病和精神疾病都伴随或驱动着大脑连接能力的改变。在这项研究中,在丘脑神经节律不齐模型TRIP8b -/- 小鼠,以及对照(野生型或WT)小鼠。计算了每只动物的SWS的20个10 length长时期和主动觉醒(AW)的相干性和非线性格兰杰因果关系(GC)。与野生型相比,SWS期间皮层和皮层与丘脑之间的相干性降低了约4至20 Hz,而野生型TRIP8b -/-小鼠中相干性没有降低。此外,与野生型小鼠相比,TRIP8b -/-小鼠在AW期间显示出较低的CT相干性; SWS期间不再存在这些差异。无条件GC分析还显示了WT小鼠与睡眠有关的TC和CT耦合降低,而TRIP8b -/-小鼠表现出减弱的唤醒和增强的睡眠CC耦合,以及在唤醒和睡眠期间表现出较强的CT定向耦合,尽管在睡眠时较小。条件性GC偶联分析证实了TRIP8b -/-小鼠的CC减少和CT偶联增强。我们的发现表明,表征TRIP8b -// 小鼠的超极化激活的环状核苷酸门控阳离子通道的特性改变,对CC,TC和CT网络具有明显的影响。对这些网络中通信发生改变的功能的更完整的了解,正在等待着眼于特定的感觉和注意过程的TRIP8b -/-小鼠的详细表型。

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