低温电子断层扫描中多体的自动检测

Luis Kuhn Cuellar, Stefan Pfeffer, Yuxiang Chen, Friedrich Forster
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引用次数: 1

摘要

在蛋白质合成过程中,核糖体和信使RNA组装成多体。低温电子断层扫描能够在生理条件下检测和鉴定大分子复合物,使该方法特别适合研究控制mRNA转化为蛋白质的超复合物。在这里,我们描述了一种在低温电子断层扫描中自动分配多体的方法,使用核糖体的位置和方向,通过对断层扫描数据的模板匹配进行定位,作为输入。在低温电子断层图中专家策划的多体训练数据集的基础上,我们定义了多体中邻近核糖体的相对3D排列。该先验分布用于多体分配的概率框架:来自断层图的局部核糖体表示为一个图,其边缘权重由先验分布定义。在图结构上嵌入马尔可夫随机场,并使用消息传递算法为每个核糖体推断一个多体标签,即将核糖体聚类成多体。基于模拟层析图和实验层析图对该方法的性能进行了评估,表明对于典型的低温电子层析图信噪比,多体检测是可靠的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Automated detection of polysomes in cryoelectron tomography
Ribosomes and messenger RNA assemble to polysomes during protein synthesis. Cryoelectron tomography enables detection and identification of large macromolecular complexes under physiological conditions making the method uniquely suitable to study the supercomplexes that govern translation of mRNA into proteins. Here, we describe a method for automated assignment of polysomes in cryoelectron tomograms using the positions and orientations of ribosomes, as localized by template matching on tomographic data, as input. On the basis of a training dataset of expert-curated polysomes in cryoelectron tomograms, we define the relative 3D arrangements of neighboring ribosomes in polysomes. This prior distribution is used in a probabilistic framework for polysome assignment: the localized ribosomes from a tomogram are represented as a graph of which the edge weights are defined by the prior distribution. A Markov Random Field is embedded on the graph structure, and a message-passing algorithm is used to infer a polysome-label for each ribosome, i.e., to cluster ribosomes into polysomes. The performance of the method is assessed based on simulated tomograms and experimental tomograms indicating that polysome detection is reliable for typical signal-to-noise ratios of cryoelectron tomograms.
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