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Global and local fMRI signals driven by neurons defined optogenetically by type and wiring

机译:由类型和接线以光遗传学方式定义的神经元驱动的全局和局部fMRI信号

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摘要

Despite a rapidly-growing scientific and clinical brain imaging literature based on functional magnetic resonance imaging (fMRI) using blood oxygenation level-dependent (BOLD) signals, it remains controversial whether BOLD signals in a particular region can be caused by activation of local excitatory neurons. This difficult question is central to the interpretation and utility of BOLD, with major significance for fMRI studies in basic research and clinical applications. Using a novel integrated technology unifying optogenetic control of inputs with high-field fMRI signal readouts, we show here that specific stimulation of local CaMKIIα-expressing excitatory neurons, either in the neocortex or thalamus, elicits positive BOLD signals at the stimulus location with classical kinetics. We also show that optogenetic fMRI (ofMRI) allows visualization of the causal effects of specific cell types defined not only by genetic identity and cell body location, but also by axonal projection target. Finally, we show that ofMRI within the living and intact mammalian brain reveals BOLD signals in downstream targets distant from the stimulus, indicating that this approach can be used to map the global effects of controlling a local cell population. In this respect, unlike both conventional fMRI studies based on correlations and fMRI with electrical stimulation that will also directly drive afferent and nearby axons, this ofMRI approach provides causal information about the global circuits recruited by defined local neuronal activity patterns. Together these findings provide an empirical foundation for the widely-used fMRI BOLD signal, and the features of ofMRI define a potent tool that may be suitable for functional circuit analysis as well as global phenotyping of dysfunctional circuitry.
机译:尽管基于使用血液氧合水平依赖性(BOLD)信号的功能磁共振成像(fMRI)的科学和临床脑成像文献迅速增长,但特定区域中的BOLD信号是否可能由局部兴奋性神经元的激活引起仍存在争议。这个难题是BOLD的解释和实用性的核心,对于基础研究和临床应用中的fMRI研究具有重要意义。使用一种新颖的集成技术,通过高场fMRI信号读数统一输入的光遗传学控制,我们在这里表明,新皮层或丘脑中局部表达CaMKIIα的兴奋性神经元的特异性刺激在刺激位置产生经典动力学的正BOLD信号。 。我们还表明,光遗传学功能磁共振成像(ofMRI)不仅可以通过遗传同一性和细胞体位置,还可以通过轴突投射目标来定义特定细胞类型的因果关系的可视化。最后,我们表明在活着的和完整的哺乳动物大脑中的MRI揭示了远离刺激的下游目标中的BOLD信号,表明该方法可用于绘制控制局部细胞群体的整体效应。在这方面,与传统的基于相关性的功能磁共振成像研究和具有电刺激功能的功能磁共振成像(也将直接驱动传入和附近的轴突)不同,这种磁共振成像方法提供了有关由定义的局部神经元活动模式招募的整体回路的因果信息。这些发现共同为广泛使用的fMRI BOLD信号提供了经验基础,ofMRI的特征定义了一种有效的工具,可能适用于功能电路分析以及功能异常电路的整体表型分析。

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