Distinct Genomic Features Characterize Two Clades of <i>Corynebacterium diphtheriae</i>: Proposal of <i>Corynebacterium diphtheriae</i> Subsp. <i>diphtheriae</i> Subsp. nov. and <i>Corynebacterium diphtheriae</i> Subsp. <i>lausannense</i> Subsp. nov.

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Title
Distinct Genomic Features Characterize Two Clades of <i>Corynebacterium diphtheriae</i>: Proposal of <i>Corynebacterium diphtheriae</i> Subsp. <i>diphtheriae</i> Subsp. nov. and <i>Corynebacterium diphtheriae</i> Subsp. <i>lausannense</i> Subsp. nov.
Journal
Frontiers in microbiology
Author(s)
Tagini F., Pillonel T., Croxatto A., Bertelli C., Koutsokera A., Lovis A., Greub G.
ISSN
1664-302X (Print)
ISSN-L
1664-302X
Publication state
Published
Issued date
2018
Peer-reviewed
Oui
Volume
9
Pages
1743
Language
english
Notes
Publication types: Journal Article
Publication Status: epublish
Abstract
<i>Corynebacterium diphtheriae</i> is the etiological agent of diphtheria, a disease caused by the presence of the diphtheria toxin. However, an increasing number of records report non-toxigenic <i>C. diphtheriae</i> infections. Here, a <i>C. diphtheriae</i> strain was recovered from a patient with a past history of bronchiectasis who developed a severe tracheo-bronchitis with multiple whitish lesions of the distal trachea and the mainstem bronchi. Whole-genome sequencing (WGS), performed in parallel with PCR targeting the toxin gene and the Elek test, provided clinically relevant results in a short turnaround time, showing that the isolate was non-toxigenic. A comparative genomic analysis of the new strain (CHUV2995) with 56 other publicly available genomes of <i>C. diphtheriae</i> revealed that the strains CHUV2995, CCUG 5865 and CMCNS703 share a lower average nucleotide identity (ANI) (95.24 to 95.39%) with the <i>C. diphtheriae</i> NCTC 11397 <sup>T</sup> reference genome than all other <i>C. diphtheriae</i> genomes (>98.15%). Core genome phylogeny confirmed the presence of two monophyletic clades. Based on these findings, we propose here two new <i>C. diphtheriae</i> subspecies to replace the lineage denomination used in previous multilocus sequence typing studies: <i>C. diphtheriae</i> subsp. <i>lausannense</i> subsp. nov. (instead of lineage-2), regrouping strains CHUV2995, CCUG 5865, and CMCNS703, and <i>C. diphtheriae</i> subsp. <i>diphtheriae</i> subsp. nov, regrouping all other <i>C. diphtheriae</i> in the dataset (instead of lineage-1). Interestingly, members of subspecies <i>lausannense</i> displayed a larger genome size than subspecies <i>diphtheriae</i> and were enriched in COG categories related to transport and metabolism of lipids (I) and inorganic ion (P). Conversely, they lacked all genes involved in the synthesis of pili (SpaA-type, SpaD-type and SpaH-type), molybdenum cofactor and of the nitrate reductase. Finally, the CHUV2995 genome is particularly enriched in mobility genes and harbors several prophages. The genome encodes a type II-C CRISPR-Cas locus with 2 spacers that lacks <i>csn2</i> or <i>cas4</i> , which could hamper the acquisition of new spacers and render strain CHUV2995 more susceptible to bacteriophage infections and gene acquisition through various mechanisms of horizontal gene transfer.
Keywords
CRISPR, comparative genomics, mobile genetic elements, non-toxigenic diphtheria, pili, sortase, virulence
Pubmed
Web of science
Open Access
Yes
Create date
11/09/2018 8:27
Last modification date
20/08/2019 13:32
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