A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528
<p>Abstract</p> <p>Background</p> <p><it>Pseudomonas syringae </it>is a widespread bacterial pathogen that causes disease on a broad range of economically important plant species. Pathogenicity of <it>P. syringae </it>strains is dependent on the...
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doaj-7c7513324e804d91bf2a7189090a1dc42020-11-24T22:14:27ZengBMCBMC Genomics1471-21642009-08-0110139510.1186/1471-2164-10-395A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528Dangl Jeffery LMacLean DanielIbanez SelenaStudholme David JChang Jeff HRathjen John P<p>Abstract</p> <p>Background</p> <p><it>Pseudomonas syringae </it>is a widespread bacterial pathogen that causes disease on a broad range of economically important plant species. Pathogenicity of <it>P. syringae </it>strains is dependent on the type III secretion system, which secretes a suite of up to about thirty virulence 'effector' proteins into the host cytoplasm where they subvert the eukaryotic cell physiology and disrupt host defences. <it>P. syringae </it>pathovar <it>tabaci </it>naturally causes disease on wild tobacco, the model member of the Solanaceae, a family that includes many crop species as well as on soybean.</p> <p>Results</p> <p>We used the 'next-generation' Illumina sequencing platform and the Velvet short-read assembly program to generate a 145X deep 6,077,921 nucleotide draft genome sequence for <it>P. syringae </it>pathovar <it>tabaci </it>strain 11528. From our draft assembly, we predicted 5,300 potential genes encoding proteins of at least 100 amino acids long, of which 303 (5.72%) had no significant sequence similarity to those encoded by the three previously fully sequenced <it>P. syringae </it>genomes. Of the core set of Hrp Outer Proteins that are conserved in three previously fully sequenced <it>P. syringae </it>strains, most were also conserved in strain 11528, including AvrE1, HopAH2, HopAJ2, HopAK1, HopAN1, HopI, HopJ1, HopX1, HrpK1 and HrpW1. However, the <it>hrpZ1 </it>gene is partially deleted and <it>hopAF1 </it>is completely absent in 11528. The draft genome of strain 11528 also encodes close homologues of HopO1, HopT1, HopAH1, HopR1, HopV1, HopAG1, HopAS1, HopAE1, HopAR1, HopF1, and HopW1 and a degenerate HopM1'. Using a functional screen, we confirmed that <it>hopO1, hopT1, hopAH1</it>, <it>hopM1'</it>, <it>hopAE1</it>, <it>hopAR1</it>, and <it>hopAI1' </it>are part of the virulence-associated HrpL regulon, though the <it>hopAI1' </it>and <it>hopM1' </it>sequences were degenerate with premature stop codons. We also discovered two additional HrpL-regulated effector candidates and an HrpL-regulated distant homologue of <it>avrPto1</it>.</p> <p>Conclusion</p> <p>The draft genome sequence facilitates the continued development of <it>P. syringae </it>pathovar <it>tabaci </it>on wild tobacco as an attractive model system for studying bacterial disease on plants. The catalogue of effectors sheds further light on the evolution of pathogenicity and host-specificity as well as providing a set of molecular tools for the study of plant defence mechanisms. We also discovered several large genomic regions in <it>Pta </it>11528 that do not share detectable nucleotide sequence similarity with previously sequenced <it>Pseudomonas </it>genomes. These regions may include horizontally acquired islands that possibly contribute to pathogenicity or epiphytic fitness of <it>Pta </it>11528.</p> http://www.biomedcentral.com/1471-2164/10/395 |
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DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Dangl Jeffery L MacLean Daniel Ibanez Selena Studholme David J Chang Jeff H Rathjen John P |
spellingShingle |
Dangl Jeffery L MacLean Daniel Ibanez Selena Studholme David J Chang Jeff H Rathjen John P A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528 BMC Genomics |
author_facet |
Dangl Jeffery L MacLean Daniel Ibanez Selena Studholme David J Chang Jeff H Rathjen John P |
author_sort |
Dangl Jeffery L |
title |
A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528 |
title_short |
A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528 |
title_full |
A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528 |
title_fullStr |
A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528 |
title_full_unstemmed |
A draft genome sequence and functional screen reveals the repertoire of type III secreted proteins of <it>Pseudomonas syringae </it>pathovar <it>tabaci </it>11528 |
title_sort |
draft genome sequence and functional screen reveals the repertoire of type iii secreted proteins of <it>pseudomonas syringae </it>pathovar <it>tabaci </it>11528 |
publisher |
BMC |
series |
BMC Genomics |
issn |
1471-2164 |
publishDate |
2009-08-01 |
description |
<p>Abstract</p> <p>Background</p> <p><it>Pseudomonas syringae </it>is a widespread bacterial pathogen that causes disease on a broad range of economically important plant species. Pathogenicity of <it>P. syringae </it>strains is dependent on the type III secretion system, which secretes a suite of up to about thirty virulence 'effector' proteins into the host cytoplasm where they subvert the eukaryotic cell physiology and disrupt host defences. <it>P. syringae </it>pathovar <it>tabaci </it>naturally causes disease on wild tobacco, the model member of the Solanaceae, a family that includes many crop species as well as on soybean.</p> <p>Results</p> <p>We used the 'next-generation' Illumina sequencing platform and the Velvet short-read assembly program to generate a 145X deep 6,077,921 nucleotide draft genome sequence for <it>P. syringae </it>pathovar <it>tabaci </it>strain 11528. From our draft assembly, we predicted 5,300 potential genes encoding proteins of at least 100 amino acids long, of which 303 (5.72%) had no significant sequence similarity to those encoded by the three previously fully sequenced <it>P. syringae </it>genomes. Of the core set of Hrp Outer Proteins that are conserved in three previously fully sequenced <it>P. syringae </it>strains, most were also conserved in strain 11528, including AvrE1, HopAH2, HopAJ2, HopAK1, HopAN1, HopI, HopJ1, HopX1, HrpK1 and HrpW1. However, the <it>hrpZ1 </it>gene is partially deleted and <it>hopAF1 </it>is completely absent in 11528. The draft genome of strain 11528 also encodes close homologues of HopO1, HopT1, HopAH1, HopR1, HopV1, HopAG1, HopAS1, HopAE1, HopAR1, HopF1, and HopW1 and a degenerate HopM1'. Using a functional screen, we confirmed that <it>hopO1, hopT1, hopAH1</it>, <it>hopM1'</it>, <it>hopAE1</it>, <it>hopAR1</it>, and <it>hopAI1' </it>are part of the virulence-associated HrpL regulon, though the <it>hopAI1' </it>and <it>hopM1' </it>sequences were degenerate with premature stop codons. We also discovered two additional HrpL-regulated effector candidates and an HrpL-regulated distant homologue of <it>avrPto1</it>.</p> <p>Conclusion</p> <p>The draft genome sequence facilitates the continued development of <it>P. syringae </it>pathovar <it>tabaci </it>on wild tobacco as an attractive model system for studying bacterial disease on plants. The catalogue of effectors sheds further light on the evolution of pathogenicity and host-specificity as well as providing a set of molecular tools for the study of plant defence mechanisms. We also discovered several large genomic regions in <it>Pta </it>11528 that do not share detectable nucleotide sequence similarity with previously sequenced <it>Pseudomonas </it>genomes. These regions may include horizontally acquired islands that possibly contribute to pathogenicity or epiphytic fitness of <it>Pta </it>11528.</p> |
url |
http://www.biomedcentral.com/1471-2164/10/395 |
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