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一种蛋白质组学结构系统方法揭示了人类所有疱疹病毒家族蛋白的深入见解。

A proteome-wide structural systems approach reveals insights into protein families of all human herpesviruses.

机构信息

Hannover Medical School, Institute of Virology, Hanover, Germany.

Centre for Structural Systems Biology, Hamburg, Germany.

出版信息

Nat Commun. 2024 Nov 26;15(1):10230. doi: 10.1038/s41467-024-54668-2.

Abstract

Structure predictions have become invaluable tools, but viral proteins are absent from the EMBL/DeepMind AlphaFold database. Here, we provide proteome-wide structure predictions for all nine human herpesviruses and analyze them in depth with explicit scoring thresholds. By clustering these predictions into structural similarity groups, we identified new families, such as the HCMV UL112-113 cluster, which is conserved in alpha- and betaherpesviruses. A domain-level search found protein families consisting of subgroups with varying numbers of duplicated folds. Using large-scale structural similarity searches, we identified viral proteins with cellular folds, such as the HSV-1 US2 cluster possessing dihydrofolate reductase folds and the EBV BMRF2 cluster that might have emerged from cellular equilibrative nucleoside transporters. Our HerpesFolds database is available at https://www.herpesfolds.org/herpesfolds and displays all models and clusters through an interactive web interface. Here, we show that system-wide structure predictions can reveal homology between viral species and identify potential protein functions.

摘要

结构预测已成为非常有价值的工具,但病毒蛋白并未包含在 EMBL/DeepMind AlphaFold 数据库中。在这里,我们提供了针对所有九种人类疱疹病毒的全蛋白质组结构预测,并使用明确的评分阈值对其进行了深入分析。通过将这些预测聚类为结构相似性组,我们鉴定了新的家族,例如 HCMV UL112-113 簇,它在α和β疱疹病毒中保守。通过域级搜索,我们发现了由具有不同折叠数的亚组组成的蛋白质家族。使用大规模结构相似性搜索,我们鉴定了具有细胞折叠的病毒蛋白,例如 HSV-1 US2 簇具有二氢叶酸还原酶折叠,以及 EBV BMRF2 簇可能源自细胞平衡核苷转运体。我们的 HerpesFolds 数据库可在 https://www.herpesfolds.org/herpesfolds 上获得,并通过交互式网络界面显示所有模型和簇。在这里,我们表明系统范围的结构预测可以揭示病毒物种之间的同源性,并确定潜在的蛋白质功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d3b4/11599850/a35c1639960d/41467_2024_54668_Fig1_HTML.jpg

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