Whole-Genome Sequencing of Three Clonal Clinical Isolates of B. cenocepacia from a Patient with Cystic Fibrosis

Ruth R Miller,Patrick Tang,Trevor J Hird,James E A Zlosnik,Annamaria Bevivino

doi:10.1371/journal.pone.0143472

Ruth R Miller, Patrick Tang + Show 3 more

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https://doi.org/10.1371/journal.pone.0143472

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Abstract

Burkholderia cepacia complex bacteria are amongst the most feared of pathogens in cystic fibrosis (CF). The BCC comprises at least 20 distinct species that can cause chronic and unpredictable lung infections in CF. Historically the species B. cenocepacia has been the most prevalent in CF infections and has been associated in some centers with high rates of mortality. Modeling chronic infection by B. cenocepacia in the laboratory is challenging and no models exist which effectively recapitulate CF disease caused by BCC bacteria. Therefore our understanding of factors that contribute towards the morbidity and mortality caused by this organism is limited. In this study we used whole-genome sequencing to examine the evolution of 3 clonal clinical isolates of B. cenocepacia from a patient with cystic fibrosis. The first isolate was from the beginning of infection, and the second two almost 10 years later during the final year of the patients’ life. These isolates also demonstrated phenotypic heterogeneity, with the first isolate displaying the mucoid phenotype (conferred by the overproduction of exopolysaccharide), while one of the later two was nonmucoid. In addition we also sequenced a nonmucoid derivative of the initial mucoid isolate, acquired in the laboratory by antibiotic pressure. Examination of sequence data revealed that the two late stage isolates shared 20 variant nucleotides in common compared to the early isolate. However, despite their isolation within 10 months of one another, there was also considerable variation between the late stage isolates, including 42 single nucleotide variants and three deletions. Additionally, no sequence differences were identified between the initial mucoid isolate and its laboratory acquired nonmucoid derivative, however transcript analysis indicated at least partial down regulation of genes involved in exopolysaccharide production. Our study examines the progression of B. cenocepacia throughout chronic infection, including establishment of sub-populations likely evolved from the original isolate, suggestive of parallel evolution. Additionally, the lack of sequence differences between two of the isolates with differing mucoid phenotypes suggests that other factors, such as gene regulation, come into play in establishing the mucoid phenotype.

Highlights

Bacteria belonging to the Burkholderia cepacia complex (BCC) are highly problematic pathogens in people with cystic fibrosis (CF)
One of the more challenging aspects of the infections caused by BCC bacteria is their chronic nature, with infections lasting years, and sometimes decades, making in-vitro modeling of virulence challenging
The data presented here are one of the first comparative analyses of B. cenocepacia longitudinal clinical isolates taken from a chronic cystic fibrosis infection

Summary

Introduction

Bacteria belonging to the Burkholderia cepacia complex (BCC) are highly problematic pathogens in people with cystic fibrosis (CF). There are at least 20 distinct species of bacteria in the BCC, and all except for B. ubonensis have been isolated from the lungs of people with CF [1,2,3]. Epidemic spread of B. cenocepacia has previously resulted in high rates of prevalence of this species in CF populations [4,5,6]. In some instances BCC bacteria can result in a rapidly invasive and typically fatal necrotizing pneumonia known as ‘cepacia syndrome’ [19]. The causes of these disparate outcomes are not understood and there are limited studies on adaptation of BCC bacteria to chronic infection in the CF lung

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