High-resolution microbial community reconstruction by integrating short reads from multiple 16S rRNA regions.
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Abstract | The emergence of massively parallel sequencing technology has revolutionized microbial profiling, allowing the unprecedented comparison of microbial diversity across time and space in a wide range of host-associated and environmental ecosystems. Although the high-throughput nature of such methods enables the detection of low-frequency bacteria, these advances come at the cost of sequencing read length, limiting the phylogenetic resolution possible by current methods. Here, we present a generic approach for integrating short reads from large genomic regions, thus enabling phylogenetic resolution far exceeding current methods. The approach is based on a mapping to a statistical model that is later solved as a constrained optimization problem. We demonstrate the utility of this method by analyzing human saliva and Drosophila samples, using Illumina single-end sequencing of a 750 bp amplicon of the 16S rRNA gene. Phylogenetic resolution is significantly extended while reducing the number of falsely detected bacteria, as compared with standard single-region Roche 454 Pyrosequencing. Our approach can be seamlessly applied to simultaneous sequencing of multiple genes providing a higher resolution view of the composition and activity of complex microbial communities. |
Year of Publication | 2013
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Journal | Nucleic Acids Res
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Volume | 41
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Issue | 22
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Pages | e205
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Date Published | 2013 Dec
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ISSN | 1362-4962
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DOI | 10.1093/nar/gkt1070
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PubMed ID | 24214960
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PubMed Central ID | PMC3905898
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Grant list | P50 GM068763 / GM / NIGMS NIH HHS / United States
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