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灵长类动物皮层癫痫样活动期间内在光学信号的成像。

Imaging of intrinsic optical signals in primate cortex during epileptiform activity.

作者信息

Haglund Michael M, Hochman Daryl W

机构信息

Department of Surgery (Neurosurgery), Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

Epilepsia. 2007;48 Suppl 4:65-74. doi: 10.1111/j.1528-1167.2007.01243.x.

DOI:10.1111/j.1528-1167.2007.01243.x
PMID:17767577
Abstract

Localized increases in neuronal activity are known to alter the distribution and oxygen content of blood within the surrounding brain tissue. In the neocortex, these activity-evoked hemodynamic changes are predominantly mediated through the dilation of the microscopic pial arterioles that lie on the surface of the brain, nearest to the site of activation. Since hemoglobin absorbs light throughout the visible and near-infrared spectrum, optical microscopy combined with computer imaging techniques can be used to map the patterns of hemodynamic changes associated with neuronal activity. Examples of optical imaging data are provided here to demonstrate four points. First, depending on the optical wavelength chosen for illumination of the cortex, different spatial and temporal patterns of optical changes are elicited by similar stimuli yielding distinctly different types of physiological information. Second, by selecting the appropriate wavelengths, it is possible to generate maps from optical-imaging data that represent changes predominately due to either blood volume (at 535 nm) or blood oxygenation (at 660 nm). Third, "negative" optical signals are negative only relative to a given optical wavelength, and appear to be associated with more intense types of neuronal activation. Fourth, optical imaging is a useful technique for studying neocortical seizure activity in animal models, with the caveat that species-specific differences in cortical size and vascularization patterns may be important to consider in the interpretation of optical imaging data.

摘要

已知神经元活动的局部增强会改变周围脑组织内血液的分布和含氧量。在新皮层中,这些由活动引发的血液动力学变化主要通过位于脑表面、最靠近激活部位的微小软膜小动脉的扩张来介导。由于血红蛋白在整个可见光谱和近红外光谱范围内吸收光,光学显微镜与计算机成像技术相结合可用于绘制与神经元活动相关的血液动力学变化模式。这里提供了光学成像数据的示例来说明四点。第一,根据选择用于照射皮层的光波长,相似的刺激会引发不同的光学变化空间和时间模式,从而产生截然不同类型的生理信息。第二,通过选择合适的波长,可以从光学成像数据生成主要代表由于血容量(在535纳米处)或血液氧合(在660纳米处)引起变化的图谱。第三,“负”光学信号仅相对于给定的光波长为负,并且似乎与更强烈类型的神经元激活相关。第四,光学成像对于研究动物模型中的新皮层癫痫活动是一种有用的技术,但需要注意的是,在解释光学成像数据时,皮层大小和血管化模式的物种特异性差异可能是重要的考虑因素。

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