Abstract
BackgroundM. catarrhalis is a gram-negative, gamma-proteobacterium and an opportunistic human pathogen associated with otitis media (OM) and exacerbations of chronic obstructive pulmonary disease (COPD). With direct and indirect costs for treating these conditions annually exceeding $33 billion in the United States alone, and nearly ubiquitous resistance to beta-lactam antibiotics among M. catarrhalis clinical isolates, a greater understanding of this pathogen's genome and its variability among isolates is needed.ResultsThe genomic sequences of ten geographically and phenotypically diverse clinical isolates of M. catarrhalis were determined and analyzed together with two publicly available genomes. These twelve genomes were subjected to detailed comparative and predictive analyses aimed at characterizing the supragenome and understanding the metabolic and pathogenic potential of this species. A total of 2383 gene clusters were identified, of which 1755 are core with the remaining 628 clusters unevenly distributed among the twelve isolates. These findings are consistent with the distributed genome hypothesis (DGH), which posits that the species genome possesses a far greater number of genes than any single isolate. Multiple and pair-wise whole genome alignments highlight limited chromosomal re-arrangement.ConclusionsM. catarrhalis gene content and chromosomal organization data, although supportive of the DGH, show modest overall genic diversity. These findings are in stark contrast with the reported heterogeneity of the species as a whole, as wells as to other bacterial pathogens mediating OM and COPD, providing important insight into M. catarrhalis pathogenesis that will aid in the development of novel therapeutic regimens.
Highlights
M. catarrhalis is a gram-negative, gamma-proteobacterium and an opportunistic human pathogen associated with otitis media (OM) and exacerbations of chronic obstructive pulmonary disease (COPD)
The strains chosen for this analysis represent a geographically and clinically diverse collection of isolates from the middle ear, respiratory tract and blood stream collected from North America and Europe ([18,19]; this study)
Comparative analyses revealed that all twelve isolates are highly similar within the context of their virulence and metabolic potential, Clustered regularly interspaced short palindromic repeat (CRISPR) and mobile genetic element content, chromosomal synteny and gene content
Summary
M. catarrhalis is a gram-negative, gamma-proteobacterium and an opportunistic human pathogen associated with otitis media (OM) and exacerbations of chronic obstructive pulmonary disease (COPD). The gene content of these two strains demonstrated a high degree of homology, suggesting M. catarrhalis clinical isolates may possess only limited genetic diversity, in contrast to the reported heterogeneity of the species [14,15,16]. We characterized the supragenome of M. catarrhalis, determined from the sequencing and comparative genomic analysis of twelve clinical isolates. Mathematical modeling demonstrated that we have sequenced a sufficient number of M. catarrhalis genomes to have adequately characterized both the core and supragenomes of this pathogen. We provide a context-rich, detailed analysis of the M. catarrhalis supragenome and its implications towards pathogenesis
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