Author:
Brown Connor L.,Mullet James,Hindi Fadi,Stoll James E.,Gupta Suraj,Choi Minyoung,Keenum Ishi,Vikesland Peter,Pruden Amy,Zhang Liqing
Abstract
ABSTRACTCurrently available databases of bacterial mobile genetic elements (MGEs) contain both “core” and accessory MGE functional modules, the latter of which are often only transiently associated with the element. The presence of these accessory genes, which are often close homologs to primarily immobile genes, limits the usability of these databases for MGE annotation. To overcome this limitation, we analysed 10,776,212 protein sequences derived from seven MGE databases to compile a comprehensive database of 6,140 manually curated protein families that are linked to the “life cycle” (integration, excision, replication/recombination/repair, transfer, and stability/defense) of all major classes of bacterial MGEs. We overlay experimental information where available to create a tiered annotation scheme of high-quality annotations and annotations inferred exclusively through bioinformatic evidence. We additionally provide an MGE-class label for each entry (e.g., plasmid, integrative element) derived from the source database, and assign a list of keywords to each entry to delineate different MGE functional modules and to facilitate annotation. The resulting database, mobileOG-db (for mobile orthologous groups), provides a simple and readily interpretable foundation for an array of MGE-centred analyses. mobileOG-db can be accessed at mobileogdb.flsi.cloud.vt.edu/, where users can browse and design, refine, and analyse custom subsets of the dynamic mobilome.
Publisher
Cold Spring Harbor Laboratory
Cited by
7 articles.
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