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RAZA:一种快速的 3D z-交叉算法,用于分割电子断层扫描图像并提取细胞器和大分子。

RAZA: A Rapid 3D z-crossings algorithm to segment electron tomograms and extract organelles and macromolecules.

机构信息

Institute for Molecular Bioscience, The University of Queensland, Brisbane, QLD, Australia.

Translational Research Institute, University of Queensland Diamantina Institute, Brisbane, QLD, Australia; Department of Electrical Engineering, University of Engineering and Technology, Lahore, Punjab, Pakistan.

出版信息

J Struct Biol. 2017 Nov;200(2):73-86. doi: 10.1016/j.jsb.2017.10.002. Epub 2017 Oct 13.

Abstract

Resolving the 3D architecture of cells to atomic resolution is one of the most ambitious challenges of cellular and structural biology. Central to this process is the ability to automate tomogram segmentation to identify sub-cellular components, facilitate molecular docking and annotate detected objects with associated metadata. Here we demonstrate that RAZA (Rapid 3D z-crossings algorithm) provides a robust, accurate, intuitive, fast, and generally applicable segmentation algorithm capable of detecting organelles, membranes, macromolecular assemblies and extrinsic membrane protein domains. RAZA defines each continuous contour within a tomogram as a discrete object and extracts a set of 3D structural fingerprints (major, middle and minor axes, surface area and volume), enabling selective, semi-automated segmentation and object extraction. RAZA takes advantage of the fact that the underlying algorithm is a true 3D edge detector, allowing the axes of a detected object to be defined, independent of its random orientation within a cellular tomogram. The selectivity of object segmentation and extraction can be controlled by specifying a user-defined detection tolerance threshold for each fingerprint parameter, within which segmented objects must fall and/or by altering the number of search parameters, to define morphologically similar structures. We demonstrate the capability of RAZA to selectively extract subgroups of organelles (mitochondria) and macromolecular assemblies (ribosomes) from cellular tomograms. Furthermore, the ability of RAZA to define objects and their contours, provides a basis for molecular docking and rapid tomogram annotation.

摘要

解析细胞的 3D 结构至原子分辨率是细胞和结构生物学最具挑战性的目标之一。这一过程的核心是能够自动化断层扫描图像分割以识别亚细胞成分,促进分子对接,并为检测到的对象标记相关元数据。在这里,我们展示了 RAZA(快速 3D z 交叉算法)提供了一种强大、准确、直观、快速且普遍适用的分割算法,能够检测细胞器、膜、大分子组装体和外膜蛋白结构域。RAZA 将断层扫描图像中的每个连续轮廓定义为一个离散对象,并提取一组 3D 结构指纹(主、中、小轴、表面积和体积),从而实现选择性、半自动分割和对象提取。RAZA 利用了这样一个事实,即底层算法是一个真正的 3D 边缘检测器,允许检测到的对象的轴被定义,而与该对象在细胞断层扫描图像中的随机方向无关。对象分割和提取的选择性可以通过为每个指纹参数指定用户定义的检测容差阈值来控制,分割对象必须落入该阈值内,或者通过改变搜索参数的数量来定义形态相似的结构。我们展示了 RAZA 从细胞断层扫描图像中选择性提取细胞器(线粒体)和大分子组装体(核糖体)亚群的能力。此外,RAZA 定义对象及其轮廓的能力为分子对接和快速断层扫描注释提供了基础。

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