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用改良的生物素化葡聚糖胺标记法解析成年大鼠大脑皮质和丘脑神经元的详细结构。

Resolving the detailed structure of cortical and thalamic neurons in the adult rat brain with refined biotinylated dextran amine labeling.

机构信息

Department of Surgery, School of Medicine and Public Health, University of Wisconsin-Madison, Madison, Wisconsin, United States of America.

出版信息

PLoS One. 2012;7(11):e45886. doi: 10.1371/journal.pone.0045886. Epub 2012 Nov 5.

Abstract

Biotinylated dextran amine (BDA) has been used frequently for both anterograde and retrograde pathway tracing in the central nervous system. Typically, BDA labels axons and cell somas in sufficient detail to identify their topographical location accurately. However, BDA labeling often has proved to be inadequate to resolve the fine structural details of axon arbors or the dendrites of neurons at a distance from the site of BDA injection. To overcome this limitation, we varied several experimental parameters associated with the BDA labeling of neurons in the adult rat brain in order to improve the sensitivity of the method. Specifically, we compared the effect on labeling sensitivity of: (a) using 3,000 or 10,000 MW BDA; (b) injecting different volumes of BDA; (c) co-injecting BDA with NMDA; and (d) employing various post-injection survival times. Following the extracellular injection of BDA into the visual cortex, labeled cells and axons were observed in both cortical and thalamic areas of all animals studied. However, the detailed morphology of axon arbors and distal dendrites was evident only under optimal conditions for BDA labeling that take into account the: molecular weight of the BDA used, concentration and volume of BDA injected, post-injection survival time, and toning of the resolved BDA with gold and silver. In these instances, anterogradely labeled axons and retrogradely labeled dendrites were resolved in fine detail, approximating that which can be achieved with intracellularly injected compounds such as biocytin or fluorescent dyes.

摘要

生物素化葡聚糖胺(Biotinylated Dextran Amine,BDA)常用于中枢神经系统的顺行和逆行示踪。通常,BDA 可以充分标记轴突和细胞体,以准确识别它们的拓扑位置。然而,BDA 标记通常不足以解析轴突树突或神经元树突在远离 BDA 注射部位的精细结构细节。为了克服这一限制,我们改变了与成年大鼠大脑中神经元 BDA 标记相关的几个实验参数,以提高该方法的灵敏度。具体来说,我们比较了以下因素对标记灵敏度的影响:(a)使用 3000 或 10000 MW BDA;(b)注射不同体积的 BDA;(c)将 BDA 与 NMDA 共注射;以及(d)采用不同的注射后存活时间。在将 BDA 经细胞外注射到视皮层后,在所有研究动物的皮质和丘脑区域都观察到了标记的细胞和轴突。然而,只有在考虑到以下因素的最佳 BDA 标记条件下,才能观察到轴突树突和远端树突的详细形态:所用 BDA 的分子量、注射的 BDA 的浓度和体积、注射后的存活时间,以及用金和银对已解析的 BDA 进行色调调整。在这些情况下,可以解析出顺行标记的轴突和逆行标记的树突,其细节程度与使用细胞内注射的化合物(如生物胞素或荧光染料)所达到的程度相近。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c24/3489877/8b0be5875357/pone.0045886.g001.jpg

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