4.7 Article

Genomic Diversity of Hospital-Acquired Infections Revealed through Prospective Whole-Genome Sequencing-Based Surveillance

Journal

MSYSTEMS
Volume 7, Issue 3, Pages -

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/msystems.01384-21

Keywords

whole-genome sequencing; hospital-acquired infections; pangenome; antimicrobial resistance; horizontal gene transfer; bacterial evolution

Categories

Funding

  1. NIAID [R21Al109459, R01AI127472, U01AI124302]
  2. Department of Medicine at the University of Pittsburgh School of Medicine
  3. [KL2-TR001856]

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Healthcare-associated infections (HAIs) can lead to mortality, morbidity, and wastage of healthcare resources. This study used whole-genome sequencing to analyze the diversity of bacteria sampled from hospitalized patients at a single center. The study identified nearly 100 different bacterial species and revealed different rates of evolution among species. Antibiotic resistance genes and mobile genetic elements were also frequently observed. This study provides valuable insights into the population structure and evolution of bacteria in healthcare settings and can inform efforts in outbreak detection and prevention.
Healthcare-associated infections (HAIs) cause mortality, morbidity, and waste of health care resources. HAIs are also an important driver of antimicrobial resistance, which is increasing around the world. Beginning in November 2016, we instituted an initiative to detect outbreaks of HAIs using prospective whole-genome sequencing-based surveillance of bacterial pathogens collected from hospitalized patients. Here, we describe the diversity of bacteria sampled from hospitalized patients at a single center, as revealed through systematic analysis of bacterial isolate genomes. We sequenced the genomes of 3,004 bacterial isolates from hospitalized patients collected over a 25-month period. We identified bacteria belonging to 97 distinct species, which were distributed among 14 groups of related species. Within these groups, isolates could be distinguished from one another by both average nucleotide identity (ANI) and principal-component analysis of accessory genes (PCA-A). Core genome genetic distances and rates of evolution varied among species, which has practical implications for defining shared ancestry during outbreaks and for our broader understanding of the origins of bacterial strains and species. Finally, antimicrobial resistance genes and putative mobile genetic elements were frequently observed, and our systematic analysis revealed patterns of occurrence across the different species sampled from our hospital. Overall, this study shows how understanding the population structure of diverse pathogens circulating in a single health care setting can improve the discriminatory power of genomic epidemiology studies and can help define the processes leading to strain and species differentiation. IMPORTANCE Hospitalized patients are at increased risk of becoming infected with antibiotic-resistant organisms. We used whole-genome sequencing to survey and compare over 3,000 clinical bacterial isolates collected from hospitalized patients at a large medical center over a 2-year period. We identified nearly 100 different bacterial species, which we divided into 14 different groups of related species. When we examined how genetic relatedness differed between species, we found that different species were likely evolving at different rates within our hospital. This is significant because the identification of bacterial outbreaks in the hospital currently relies on genetic similarity cutoffs, which are often applied uniformly across organisms. Finally, we found that antibiotic resistance genes and mobile genetic elements were abundant and were shared among the bacterial isolates we sampled. Overall, this study provides an in-depth view of the genomic diversity and evolutionary processes of bacteria sampled from hospitalized patients, as well as genetic similarity estimates that can inform hospital outbreak detection and prevention efforts.

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