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使用严重急性呼吸综合征冠状病毒2(SARS-CoV-2)开放阅读框8(ORF8)的同源生成搜索模型进行晶体学分子置换。

Crystallographic molecular replacement using an -generated search model of SARS-CoV-2 ORF8.

作者信息

Flower Thomas G, Hurley James H

机构信息

Department of Molecular and Cell Biology and California Institute for Quantitative Biosciences, University of California, Berkeley, Berkeley, CA 94720.

出版信息

bioRxiv. 2021 Jan 5:2021.01.05.425441. doi: 10.1101/2021.01.05.425441.

Abstract

The majority of crystal structures are determined by the method of molecular replacement (MR). The range of application of MR is limited mainly by the need for an accurate search model. In most cases, pre-existing experimentally determined structures are used as search models. In favorable cases, predicted structures have yielded search models adequate for molecular replacement. The ORF8 protein of SARS-CoV-2 represents a challenging case for MR using an prediction because ORF8 has an all β-sheet fold and few orthologs. We previously determined experimentally the structure of ORF8 using the single anomalous dispersion (SAD) phasing method, having been unable to find an MR solution to the crystallographic phase problem. Following a report of an accurate prediction of the ORF8 structure, we assessed whether the predicted model would have succeeded as an MR search model. A phase problem solution was found, and the resulting structure was refined, yielding structural parameters equivalent to the original experimental solution.

摘要

大多数晶体结构是通过分子置换(MR)方法确定的。MR的应用范围主要受限于对精确搜索模型的需求。在大多数情况下,预先存在的实验确定的结构被用作搜索模型。在有利的情况下,预测结构产生了足以用于分子置换的搜索模型。SARS-CoV-2的ORF8蛋白对于使用预测进行MR来说是一个具有挑战性的案例,因为ORF8具有全β折叠结构且直系同源物很少。我们之前使用单波长反常散射(SAD)相位法通过实验确定了ORF8的结构,一直未能找到晶体学相位问题的MR解决方案。在一篇关于ORF8结构准确预测的报告之后,我们评估了预测模型作为MR搜索模型是否会成功。找到了相位问题的解决方案,并对所得结构进行了优化,得到了与原始实验解决方案相当的结构参数。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a8d/7805452/e31f7c696aba/nihpp-2021.01.05.425441-f0001.jpg

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