High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis

BACKGROUND: The Enterobacteriaceae comprise a large number of clinically relevant species with several individual subspecies. Overlapping virulence-associated gene pools and the high overall genome plasticity often interferes with correct enterobacterial strain typing and risk assessment. Array tech...

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Autores principales: Friedrich, Torben, Rahmann, Sven, Weigel, Wilfried, Rabsch, Wolfgang, Fruth, Angelika, Ron, Eliora, Gunzer, Florian, Dandekar, Thomas, Hacker, Jörg, Müller, Tobias, Dobrindt, Ulrich
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3017858/
https://www.ncbi.nlm.nih.gov/pubmed/20964857
http://dx.doi.org/10.1186/1471-2164-11-591
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author Friedrich, Torben
Rahmann, Sven
Weigel, Wilfried
Rabsch, Wolfgang
Fruth, Angelika
Ron, Eliora
Gunzer, Florian
Dandekar, Thomas
Hacker, Jörg
Müller, Tobias
Dobrindt, Ulrich
author_facet Friedrich, Torben
Rahmann, Sven
Weigel, Wilfried
Rabsch, Wolfgang
Fruth, Angelika
Ron, Eliora
Gunzer, Florian
Dandekar, Thomas
Hacker, Jörg
Müller, Tobias
Dobrindt, Ulrich
author_sort Friedrich, Torben
collection PubMed
description BACKGROUND: The Enterobacteriaceae comprise a large number of clinically relevant species with several individual subspecies. Overlapping virulence-associated gene pools and the high overall genome plasticity often interferes with correct enterobacterial strain typing and risk assessment. Array technology offers a fast, reproducible and standardisable means for bacterial typing and thus provides many advantages for bacterial diagnostics, risk assessment and surveillance. The development of highly discriminative broad-range microbial diagnostic microarrays remains a challenge, because of marked genome plasticity of many bacterial pathogens. RESULTS: We developed a DNA microarray for strain typing and detection of major antimicrobial resistance genes of clinically relevant enterobacteria. For this purpose, we applied a global genome-wide probe selection strategy on 32 available complete enterobacterial genomes combined with a regression model for pathogen classification. The discriminative power of the probe set was further tested in silico on 15 additional complete enterobacterial genome sequences. DNA microarrays based on the selected probes were used to type 92 clinical enterobacterial isolates. Phenotypic tests confirmed the array-based typing results and corroborate that the selected probes allowed correct typing and prediction of major antibiotic resistances of clinically relevant Enterobacteriaceae, including the subspecies level, e.g. the reliable distinction of different E. coli pathotypes. CONCLUSIONS: Our results demonstrate that the global probe selection approach based on longest common factor statistics as well as the design of a DNA microarray with a restricted set of discriminative probes enables robust discrimination of different enterobacterial variants and represents a proof of concept that can be adopted for diagnostics of a wide range of microbial pathogens. Our approach circumvents misclassifications arising from the application of virulence markers, which are highly affected by horizontal gene transfer. Moreover, a broad range of pathogens have been covered by an efficient probe set size enabling the design of high-throughput diagnostics.
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spelling pubmed-30178582011-01-24 High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis Friedrich, Torben Rahmann, Sven Weigel, Wilfried Rabsch, Wolfgang Fruth, Angelika Ron, Eliora Gunzer, Florian Dandekar, Thomas Hacker, Jörg Müller, Tobias Dobrindt, Ulrich BMC Genomics Research Article BACKGROUND: The Enterobacteriaceae comprise a large number of clinically relevant species with several individual subspecies. Overlapping virulence-associated gene pools and the high overall genome plasticity often interferes with correct enterobacterial strain typing and risk assessment. Array technology offers a fast, reproducible and standardisable means for bacterial typing and thus provides many advantages for bacterial diagnostics, risk assessment and surveillance. The development of highly discriminative broad-range microbial diagnostic microarrays remains a challenge, because of marked genome plasticity of many bacterial pathogens. RESULTS: We developed a DNA microarray for strain typing and detection of major antimicrobial resistance genes of clinically relevant enterobacteria. For this purpose, we applied a global genome-wide probe selection strategy on 32 available complete enterobacterial genomes combined with a regression model for pathogen classification. The discriminative power of the probe set was further tested in silico on 15 additional complete enterobacterial genome sequences. DNA microarrays based on the selected probes were used to type 92 clinical enterobacterial isolates. Phenotypic tests confirmed the array-based typing results and corroborate that the selected probes allowed correct typing and prediction of major antibiotic resistances of clinically relevant Enterobacteriaceae, including the subspecies level, e.g. the reliable distinction of different E. coli pathotypes. CONCLUSIONS: Our results demonstrate that the global probe selection approach based on longest common factor statistics as well as the design of a DNA microarray with a restricted set of discriminative probes enables robust discrimination of different enterobacterial variants and represents a proof of concept that can be adopted for diagnostics of a wide range of microbial pathogens. Our approach circumvents misclassifications arising from the application of virulence markers, which are highly affected by horizontal gene transfer. Moreover, a broad range of pathogens have been covered by an efficient probe set size enabling the design of high-throughput diagnostics. BioMed Central 2010-10-21 /pmc/articles/PMC3017858/ /pubmed/20964857 http://dx.doi.org/10.1186/1471-2164-11-591 Text en Copyright ©2010 Friedrich et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Friedrich, Torben
Rahmann, Sven
Weigel, Wilfried
Rabsch, Wolfgang
Fruth, Angelika
Ron, Eliora
Gunzer, Florian
Dandekar, Thomas
Hacker, Jörg
Müller, Tobias
Dobrindt, Ulrich
High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
title High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
title_full High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
title_fullStr High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
title_full_unstemmed High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
title_short High-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
title_sort high-throughput microarray technology in diagnostics of enterobacteria based on genome-wide probe selection and regression analysis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3017858/
https://www.ncbi.nlm.nih.gov/pubmed/20964857
http://dx.doi.org/10.1186/1471-2164-11-591
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