4.8 Article

Population analysis of Legionella pneumophila reveals a basis for resistance to complement-mediated killing

NATURE COMMUNICATIONS (2021)

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Journal

NATURE COMMUNICATIONS
Volume 12, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41467-021-27478-z

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Categories

Multidisciplinary Sciences

Funding

  1. Chief Scientists Office Scotland [ETM/421]
  2. Wellcome Trust Collaborative award [201531/Z/16/Z]
  3. Medical Research Council (UK) [MR/N02995X/1]
  4. Biotechnology and Biological Sciences Research Council institute strategic grant funding (ISP2) [BB/P013740/1]
  5. MRC CLIMB [MR/L015080/1]
  6. International Max-Planck Research School (IMPRS-IDI)
  7. German Research Foundation [OP 86/12-1, SFB-TR84A1/A5]
  8. MRC [MR/L015080/1] Funding Source: UKRI

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The authors analyzed the genomes of 902 clinical and environmental isolates of Legionella pneumophila, and identified a bacterial gene strongly associated with human infection and resistance to complement-mediated killing.
Legionella pneumophila is the most common cause of the severe respiratory infection known as Legionnaires' disease. However, the microorganism is typically a symbiont of free-living amoeba, and our understanding of the bacterial factors that determine human pathogenicity is limited. Here we carried out a population genomic study of 902 L. pneumophila isolates from human clinical and environmental samples to examine their genetic diversity, global distribution and the basis for human pathogenicity. We find that the capacity for human disease is representative of the breadth of species diversity although some clones are more commonly associated with clinical infections. We identified a single gene (lag-1) to be most strongly associated with clinical isolates. lag-1, which encodes an O-acetyltransferase for lipopolysaccharide modification, has been distributed horizontally across all major phylogenetic clades of L. pneumophila by frequent recent recombination events. The gene confers resistance to complement-mediated killing in human serum by inhibiting deposition of classical pathway molecules on the bacterial surface. Furthermore, acquisition of lag-1 inhibits complement-dependent phagocytosis by human neutrophils, and promoted survival in a mouse model of pulmonary legionellosis. Thus, our results reveal L. pneumophila genetic traits linked to disease and provide a molecular basis for resistance to complement-mediated killing. The bacterium Legionella pneumophila can cause severe respiratory infection, but is typically a symbiont of free-living amoeba. Here, the authors analyse the genomes of 902 clinical and environmental isolates, and identify a bacterial gene that is strongly associated with human infection and confers resistance to complement-mediated killing.

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