Abstract

During chronic respiratory infections of cystic fibrosis (CF) patients, bacteria adaptively evolve in response to the nutritional and immune environment as well as influence other infecting microbes. The present study was designed to gain insights into the genetic mechanisms underlying adaptation and diversification by the two most prevalent pathogenic species of the Burkholderia cepacia complex (Bcc), B. cenocepacia and B. multivorans. Herein, we study the evolution of both of these species during coinfection of a CF patient for 4.4 years using genome sequences of 9 B. multivorans and 11 B. cenocepacia. This co-infection spanned at least 3 years following initial infection by B. multivorans and ultimately ended in the patient’s death by cepacia syndrome. Both species acquired several mutations with accumulation rates of 2.08 (B. cenocepacia) and 2.27 (B. multivorans) SNPs/year. Many of the mutated genes are associated with oxidative stress response, transition metal metabolism, defense mechanisms against antibiotics, and other metabolic alterations consistent with the idea that positive selection might be driven by the action of the host immune system, antibiotic therapy and low oxygen and iron concentrations. Two orthologous genes shared by B. cenocepacia and B. multivorans were found to be under strong selection and accumulated mutations associated with lineage diversification. One gene encodes a nucleotide sugar dehydratase involved in lipopolysaccharide O-antigen (OAg) biosynthesis (wbiI). The other gene encodes a putative two-component regulatory sensor kinase protein required to sense and adapt to oxidative- and heavy metal- inducing stresses. This study contributes to understanding of shared and species-specific evolutionary patterns of B. cenocepacia and B. multivorans evolving in the same CF lung environment.

Highlights

  • Chronic pulmonary infections are considered the leading cause for morbidity and premature death of patients at risk, as cystic fibrosis (CF) patients and immunocompromised individuals (Lipuma, 2010)

  • The first isolates obtained from patient J, B. cenocepacia IST439 and B. multivorans IST419, were used as the ancestor reference strains for comparative genomic analysis

  • Fourteen unique genomic islands (GIs) were predicted in B. cenocepacia IST439 genome (MLST profile ST218) and termed BcenST218_GI1 to BcenST218_GI14 (Supplementary Figure 1 – panel A and Supplementary Table 4) while 17 unique GIs were detected in B. multivorans IST419 (MLST profile ST836) and termed BmST836_GI1 to BmST836_GI17 (Supplementary Figure 1 – panel B and Supplementary Table 5)

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Summary

Introduction

Chronic pulmonary infections are considered the leading cause for morbidity and premature death of patients at risk, as cystic fibrosis (CF) patients and immunocompromised individuals (Lipuma, 2010). Several opportunistic pathogens may populate the CF airways and the heterogeneous microbial populations usually present are difficult to eradicate (Lipuma, 2010). Burkholderia cepacia complex (Bcc) species are feared by CF patients (Mahenthiralingam et al, 2005). Pulmonary infection with Bcc bacteria can involve a single species or co-infection with more than one Bcc species and, besides interpatient transmission, these bacteria can cause chronic infections and a marked decline of lung functions and decreased life expectancy. Some Bcc species can lead to a lethal uncontrolled clinical deterioration with septicemia and necrotizing pneumonia (the “cepacia syndrome”) (Mahenthiralingam et al, 2005)

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