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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >New techniques for imaging, digitization and analysis of three-dimensional neural morphology on multiple scales.
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New techniques for imaging, digitization and analysis of three-dimensional neural morphology on multiple scales.

机译:用于在多个尺度上对三维神经形态进行成像,数字化和分析的新技术。

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摘要

Cognitive impairment in normal aging and neurodegenerative diseases is accompanied by altered morphologies on multiple scales. Understanding of the role of these structural changes in producing functional deficits in brain aging and neuropsychiatric disorders requires accurate three-dimensional representations of neuronal morphology, and realistic biophysical modeling that can directly relate structural changes to altered neuronal firing patterns. To date however, tools capable of resolving, digitizing and analyzing neuronal morphology on both local and global scales, and with sufficient throughput and automation, have been lacking. The precision of existing image analysis-based morphometric tools is restricted at the finest scales, where resolution of fine dendritic features and spine geometry is limited by the skeletonization methods used, and by quantization errors arising from insufficient imaging resolution. We are developing techniques for imaging, reconstruction and analysis of neuronal morphology that capture both local and global structural variation. To minimize quantization error and evaluate more precisely the fine geometry of dendrites and spines, we introduce a new shape analysis technique, the Rayburst sampling algorithm that uses the original grayscale data rather than the segmented images for precise, continuous radius estimation, and multidirectional radius sampling to represent non-circular branch cross-sections and anisotropic structures such as dendritic spine heads, with greater accuracy. We apply the Rayburst technique to 3D neuronal shape analysis at different scales. We reconstruct and digitize entire neurons from stacks of laser-scanning microscopy images, as well as globally complex structures such as multineuron networks and microvascular networks. We also introduce imaging techniques necessary to recover detailed information on three-dimensional mass distribution and surface roughness of amyloid beta plaques from human Alzheimer's disease patients and from the Tg2576 mouse that expresses the Swedish three-dimensional morphometry of complex histologic structures on multiple scales, the tools described in this report will enable multiscale biophysical modeling studies capable of testing potential mechanisms by which altered dendritic structure, spine geometry and network branching patterns that occur in normal aging and in many brain disorders, determine deficits of functions such as working memory and cognition.
机译:正常衰老和神经退行性疾病中的认知障碍伴随着多种尺度形态的改变。要了解这些结构变化在脑衰老和神经精神疾病中产生功能缺陷的作用,就需要对神经元形态进行精确的三维表征,并且需要能够将结构变化与改变的神经元放电模式直接相关的现实生物物理模型。然而,迄今为止,仍缺乏能够在本地和全球范围内解析,数字化和分析神经元形态,并且具有足够的吞吐量和自动化的工具。现有的基于图像分析的形态计量学工具的精度受到最严格的限制,其中精细的树突状特征和脊柱几何形状的分辨率受到所使用的骨架化方法以及成像分辨率不足引起的量化误差的限制。我们正在开发用于捕获,捕获和捕获局部和全局结构变化的神经元形态的成像,重建和分析技术。为了最小化量化误差并更精确地评​​估树突和刺的精细几何形状,我们引入了一种新的形状分析技术,即Rayburst采样算法,该算法使用原始灰度数据而不是分割图像来进行精确的连续半径估计和多方向半径采样以更高的精度表示非圆形分支横截面和各向异性结构,例如树突状脊柱头部。我们将Rayburst技术应用于不同规模的3D神经元形状分析。我们从堆栈的激光扫描显微镜图像以及全局复杂的结构(如多神经元网络和微血管网络)重建并数字化整个神经元。我们还将介绍必要的成像技术,以从人类阿尔茨海默氏病患者和Tg2576小鼠中恢复有关淀粉样蛋白β斑块的三维质量分布和表面粗糙度的详细信息,该小鼠在多个尺度上表达复杂组织学结构的瑞典三维形态,本报告中描述的工具将能够进行多尺度生物物理建模研究,从而能够测试潜在的机制,通过这些机制,改变正常衰老和许多脑部疾病中发生的树突结构,脊柱几何形状和网络分支模式,可以确定诸如工作记忆和认知功能的缺陷。

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