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Combining Confocal Laser Scanning Microscopy with Serial Section Reconstruction in the Study of Adult Neurogenesis

机译:共焦激光扫描显微镜与连续切片重建相结合在成人神经发生研究中的应用

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摘要

Current advances in imaging techniques have extended the possibility of visualizing small structures within large volumes of both fixed and live specimens without sectioning. These techniques have contributed valuable information to study neuronal plasticity in the adult brain. However, technical limits still hamper the use of these approaches to investigate neurogenic regions located far from the ventricular surface such as parenchymal neurogenic niches, or the scattered neuroblasts induced by brain lesions. Here, we present a method to combine confocal laser scanning microscopy (CLSM) and serial section reconstruction in order to reconstruct large volumes of brain tissue at cellular resolution. In this method a series of thick sections are imaged with CLSM and the resulting stacks of images are registered and 3D reconstructed. This approach is based on existing freeware software and can be performed on ordinary laboratory personal computers. By using this technique we have investigated the morphology and spatial organization of a group of doublecortin (DCX)+ neuroblasts located in the lateral striatum of the late post-natal guinea pig. The 3D study unraveled a complex network of long and poorly ramified cell processes, often fascicled and mostly oriented along the internal capsule fiber bundles. These data support CLSM serial section reconstruction as a reliable alternative to the whole mount approaches to analyze cyto-architectural features of adult germinative niches.
机译:成像技术的最新进展已经扩展了可视化固定和活动标本中的小结构而无需切片的可能性。这些技术为研究成年大脑中的神经元可塑性提供了有价值的信息。但是,技术限制仍然妨碍了使用这些方法来研究远离心室表面的神经源性区域,例如实质性神经源性壁ni或由脑损伤引起的散在的成神经细胞。在这里,我们提出了一种共焦激光扫描显微镜(CLSM)和连续切片重建相结合的方法,以便以细胞分辨率重建大量的脑组织。在这种方法中,用CLSM对一系列厚截面进行成像,然后对所得的图像堆栈进行配准并进行3D重建。这种方法基于现有的免费软件,可以在普通的实验室个人计算机上执行。通过使用此技术,我们研究了位于出生后后期豚鼠外侧纹状体中的一组双皮质素(DCX)+成神经细胞的形态和空间组织。 3D研究揭示了一个复杂的网络,该网络由漫长且分枝不佳的细胞过程组成,通常呈簇状,且大多沿内部囊状纤维束取向。这些数据支持CLSM序列切片重建,作为分析成年生殖生境的细胞结构特征的完整方法的可靠替代方案。

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