Literature DB >> 23190732

Reducing bias in bacterial community analysis of lower respiratory infections.

Geraint B Rogers1, Leah Cuthbertson, Lucas R Hoffman, Peter A C Wing, Christopher Pope, Danny A P Hooftman, Andrew K Lilley, Anna Oliver, Mary P Carroll, Kenneth D Bruce, Christopher J van der Gast.   

Abstract

High-throughput pyrosequencing and quantitative PCR (Q-PCR) analysis offer greatly improved accuracy and depth of characterisation of lower respiratory infections. However, such approaches suffer from an inability to distinguish between DNA derived from viable and non-viable bacteria. This discrimination represents an important step in characterising microbial communities, particularly in contexts with poor clearance of material or high antimicrobial stress, as non-viable bacteria and extracellular DNA can contribute significantly to analyses. Pre-treatment of samples with propidium monoazide (PMA) is an effective approach to non-viable cell exclusion (NVCE). However, the impact of NVCE on microbial community characteristics (abundance, diversity, composition and structure) is not known. Here, adult cystic fibrosis (CF) sputum samples were used as a paradigm. The effects of PMA treatment on CF sputum bacterial community characteristics, as analysed by pyrosequencing and enumeration by species-specific (Pseudomonas aeruginosa) and total bacterial Q-PCR, were assessed. At the local community level, abundances of both total bacteria and of P. aeruginosa were significantly lower in PMA-treated sample portions. Meta-analysis indicated no overall significant differences in diversity; however, PMA treatment resulted in a significant alteration in local community membership in all cases. In contrast, at the metacommunity level, PMA treatment resulted in an increase in community evenness, driven by an increase in diversity, predominately representing rare community members. Importantly, PMA treatment facilitated the detection of both recognised and emerging CF pathogens, significantly influencing 'core' and 'satellite' taxa group membership. Our findings suggest failure to implement NVCE may result in skewed bacterial community analyses.

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Year:  2012        PMID: 23190732      PMCID: PMC3603400          DOI: 10.1038/ismej.2012.145

Source DB:  PubMed          Journal:  ISME J        ISSN: 1751-7362            Impact factor:   10.302


  34 in total

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9.  Partitioning core and satellite taxa from within cystic fibrosis lung bacterial communities.

Authors:  Christopher J van der Gast; Alan W Walker; Franziska A Stressmann; Geraint B Rogers; Paul Scott; Thomas W Daniels; Mary P Carroll; Julian Parkhill; Kenneth D Bruce
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10.  Polymicrobial nature of chronic diabetic foot ulcer biofilm infections determined using bacterial tag encoded FLX amplicon pyrosequencing (bTEFAP).

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  38 in total

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2.  Mechanical homogenization increases bacterial homogeneity in sputum.

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4.  Changes in cystic fibrosis airway microbiota at pulmonary exacerbation.

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6.  Interpreting infective microbiota: the importance of an ecological perspective.

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7.  Predominant pathogen competition and core microbiota divergence in chronic airway infection.

Authors:  Geraint B Rogers; Christopher J van der Gast; David J Serisier
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8.  Complexity, temporal stability, and clinical correlates of airway bacterial community composition in primary ciliary dyskinesia.

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9.  Three clinically distinct chronic pediatric airway infections share a common core microbiota.

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