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Cortical functional architecture and local coupling between neuronal activity and the microcirculation revealed by in vivo high-resolution optical imaging of intrinsic signals.

机译:皮质功能结构和神经元活动与微循环之间的局部耦合通过内在信号的体内高分辨率光学成像揭示。

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摘要

We have shown previously the existence of small, activity-dependent changes in intrinsic optical properties of cortex that are useful for optical imaging of cortical functional architecture. In this study we introduce a higher resolution optical imaging system that offers spatial and temporal resolution exceeding that achieved by most alternative imaging techniques for imaging cortical functional architecture or for monitoring local changes in cerebral blood volume or oxygen saturation. In addition, we investigated the mechanisms responsible for the activity-dependent intrinsic signals evoked by sensory stimuli, and studied their origins and wavelength dependence. These studies enabled high-resolution visualization of cortical functional architecture at wavelengths ranging from 480 to 940 nm. With the use of near-infrared illumination it was possible to image cortical functional architecture through the intact dura or even through a thinned skull. In addition, the same imaging technique proved useful for imaging and discriminating sensory-evoked, activity-dependent changes in local blood volume and oxygen saturation (oxygen delivery). Illumination at 570 nm allowed imaging of activity-dependent blood volume increases, whereas at 600-630 nm, the predominant signal probably originated from activity-dependent oxygen delivery from capillaries. The onset of oxygen delivery started prior to the blood volume increase. Thus, optical imaging based on intrinsic signals is a minimally invasive procedure for monitoring short- and long-term changes in cerebral activity.
机译:我们之前已经显示了皮质固有的光学特性中存在与活动有关的细微变化,这些变化可用于皮质功能结构的光学成像。在这项研究中,我们介绍了一种更高分辨率的光学成像系统,该系统提供的时空分辨率超过了大多数替代成像技术所能实现的皮质功能体系成像或监测脑血容量或血氧饱和度的局部变化。此外,我们研究了由感觉刺激引起的与活动有关的内在信号的机制,并研究了其起源和波长依赖性。这些研究实现了在480至940 nm波长范围内的皮质功能结构的高分辨率可视化。通过使用近红外照明,可以通过完整的硬脑膜甚至薄的颅骨对皮质功能结构进行成像。此外,相同的成像技术被证明可用于成像和区分局部血容量和血氧饱和度(氧气输送)的感觉诱发性,活动依赖性变化。 570 nm处的照明可以使活动相关的血容量增加,而在600-630 nm处,主要的信号可能源自毛细血管中活动相关的氧传递。氧气输送开始于血容量增加之前。因此,基于内在信号的光学成像是一种用于监测大脑活动的短期和长期变化的微创程序。

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