High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.

Whole-genome sequencing is a powerful technique for obtaining the reference sequence information of multiple organisms. Its use can be dramatically expanded to rapidly identify genomic variations, which can be linked with phenotypes to obtain biological insights. We explored these potential applicat...

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Main Authors: Anjana Srivatsan, Yi Han, Jianlan Peng, Ashley K Tehranchi, Richard Gibbs, Jue D Wang, Rui Chen
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-08-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC2474695?pdf=render
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spelling doaj-358053c915364332899582933e5746d82020-11-24T21:41:39ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042008-08-0148e100013910.1371/journal.pgen.1000139High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.Anjana SrivatsanYi HanJianlan PengAshley K TehranchiRichard GibbsJue D WangRui ChenWhole-genome sequencing is a powerful technique for obtaining the reference sequence information of multiple organisms. Its use can be dramatically expanded to rapidly identify genomic variations, which can be linked with phenotypes to obtain biological insights. We explored these potential applications using the emerging next-generation sequencing platform Solexa Genome Analyzer, and the well-characterized model bacterium Bacillus subtilis. Combining sequencing with experimental verification, we first improved the accuracy of the published sequence of the B. subtilis reference strain 168, then obtained sequences of multiple related laboratory strains and different isolates of each strain. This provides a framework for comparing the divergence between different laboratory strains and between their individual isolates. We also demonstrated the power of Solexa sequencing by using its results to predict a defect in the citrate signal transduction pathway of a common laboratory strain, which we verified experimentally. Finally, we examined the molecular nature of spontaneously generated mutations that suppress the growth defect caused by deletion of the stringent response mediator relA. Using whole-genome sequencing, we rapidly mapped these suppressor mutations to two small homologs of relA. Interestingly, stable suppressor strains had mutations in both genes, with each mutation alone partially relieving the relA growth defect. This supports an intriguing three-locus interaction module that is not easily identifiable through traditional suppressor mapping. We conclude that whole-genome sequencing can drastically accelerate the identification of suppressor mutations and complex genetic interactions, and it can be applied as a standard tool to investigate the genetic traits of model organisms.http://europepmc.org/articles/PMC2474695?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Anjana Srivatsan
Yi Han
Jianlan Peng
Ashley K Tehranchi
Richard Gibbs
Jue D Wang
Rui Chen
spellingShingle Anjana Srivatsan
Yi Han
Jianlan Peng
Ashley K Tehranchi
Richard Gibbs
Jue D Wang
Rui Chen
High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
PLoS Genetics
author_facet Anjana Srivatsan
Yi Han
Jianlan Peng
Ashley K Tehranchi
Richard Gibbs
Jue D Wang
Rui Chen
author_sort Anjana Srivatsan
title High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
title_short High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
title_full High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
title_fullStr High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
title_full_unstemmed High-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
title_sort high-precision, whole-genome sequencing of laboratory strains facilitates genetic studies.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2008-08-01
description Whole-genome sequencing is a powerful technique for obtaining the reference sequence information of multiple organisms. Its use can be dramatically expanded to rapidly identify genomic variations, which can be linked with phenotypes to obtain biological insights. We explored these potential applications using the emerging next-generation sequencing platform Solexa Genome Analyzer, and the well-characterized model bacterium Bacillus subtilis. Combining sequencing with experimental verification, we first improved the accuracy of the published sequence of the B. subtilis reference strain 168, then obtained sequences of multiple related laboratory strains and different isolates of each strain. This provides a framework for comparing the divergence between different laboratory strains and between their individual isolates. We also demonstrated the power of Solexa sequencing by using its results to predict a defect in the citrate signal transduction pathway of a common laboratory strain, which we verified experimentally. Finally, we examined the molecular nature of spontaneously generated mutations that suppress the growth defect caused by deletion of the stringent response mediator relA. Using whole-genome sequencing, we rapidly mapped these suppressor mutations to two small homologs of relA. Interestingly, stable suppressor strains had mutations in both genes, with each mutation alone partially relieving the relA growth defect. This supports an intriguing three-locus interaction module that is not easily identifiable through traditional suppressor mapping. We conclude that whole-genome sequencing can drastically accelerate the identification of suppressor mutations and complex genetic interactions, and it can be applied as a standard tool to investigate the genetic traits of model organisms.
url http://europepmc.org/articles/PMC2474695?pdf=render
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