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运用传输电子显微镜和 3View 技术来确定胶原纤维原纤维的大小和三维结构。

Using transmission electron microscopy and 3View to determine collagen fibril size and three-dimensional organization.

机构信息

Wellcome Trust Centre for Cell-Matrix Research, Faculty of Life Sciences, University of Manchester, Manchester, UK.

出版信息

Nat Protoc. 2013;8(7):1433-48. doi: 10.1038/nprot.2013.086. Epub 2013 Jun 27.

Abstract

Collagen fibrils are the major tensile element in vertebrate tissues, in which they occur as ordered bundles in the extracellular matrix. Abnormal fibril assembly and organization results in scarring, fibrosis, poor wound healing and connective tissue diseases. Transmission electron microscopy (TEM) is used to assess the formation of the fibrils, predominantly by measuring fibril diameter. Here we describe a protocol for measuring fibril diameter as well as fibril volume fraction, mean fibril length, fibril cross-sectional shape and fibril 3D organization, all of which are major determinants of tissue function. Serial-section TEM (ssTEM) has been used to visualize fibril 3D organization in vivo. However, serial block face-scanning electron microscopy (SBF-SEM) has emerged as a time-efficient alternative to ssTEM. The protocol described below is suitable for preparing tissues for TEM and SBF-SEM (by 3View). We describe how to use 3View for studying collagen fibril organization in vivo and show how to find and track individual fibrils. The overall time scale is ~8 d from isolating the tissue to having a 3D image stack.

摘要

胶原纤维是脊椎动物组织中的主要拉伸元素,它们以有序束的形式存在于细胞外基质中。异常的纤维组装和组织导致疤痕、纤维化、伤口愈合不良和结缔组织疾病。透射电子显微镜(TEM)用于评估纤维的形成,主要通过测量纤维直径。在这里,我们描述了一种测量纤维直径以及纤维体积分数、平均纤维长度、纤维横截面形状和纤维 3D 组织的方案,所有这些都是组织功能的主要决定因素。连续切片 TEM(ssTEM)已用于可视化体内纤维的 3D 组织。然而,连续块面扫描电子显微镜(SBF-SEM)已经成为 ssTEM 的一种高效替代方法。下面描述的方案适用于准备 TEM 和 SBF-SEM(通过 3View)的组织。我们描述了如何使用 3View 研究体内胶原纤维的组织,并展示了如何找到和跟踪单个纤维。从分离组织到获得 3D 图像堆栈的总时间尺度约为 8 天。

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