The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.

The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.

Coxiella burnetii, the causative agent of human Q fever, is an intracellular pathogen that replicates in an acidified vacuole derived from the host lysosomal network. This pathogen encodes a Dot/Icm type IV secretion system that delivers bacterial proteins called effectors to the host cytosol. To id...

Full description

Bibliographic Details
Main Authors: Kimberly L Carey, Hayley J Newton, Anja Lührmann, Craig R Roy
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-05-01
Series:PLoS Pathogens
Online Access:http://europepmc.org/articles/PMC3102713?pdf=render
id doaj-d16fc1901aff4421a1d48be9f0e8e6bc
record_format Article
spelling doaj-d16fc1901aff4421a1d48be9f0e8e6bc2020-11-25T00:11:43ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742011-05-0175e100205610.1371/journal.ppat.1002056The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.Kimberly L CareyHayley J NewtonAnja LührmannCraig R RoyCoxiella burnetii, the causative agent of human Q fever, is an intracellular pathogen that replicates in an acidified vacuole derived from the host lysosomal network. This pathogen encodes a Dot/Icm type IV secretion system that delivers bacterial proteins called effectors to the host cytosol. To identify new effector proteins, the functionally analogous Legionella pneumophila Dot/Icm system was used in a genetic screen to identify fragments of C. burnetii genomic DNA that when fused to an adenylate cyclase reporter were capable of directing Dot/Icm-dependent translocation of the fusion protein into mammalian host cells. This screen identified Dot/Icm effectors that were proteins unique to C. burnetii, having no overall sequence homology with L. pneumophila Dot/Icm effectors. A comparison of C. burnetii genome sequences from different isolates revealed diversity in the size and distribution of the genes encoding many of these effectors. Studies examining the localization and function of effectors in eukaryotic cells provided evidence that several of these proteins have an affinity for specific host organelles and can disrupt cellular functions. The identification of a transposon insertion mutation that disrupts the dot/icm locus was used to validate that this apparatus was essential for translocation of effectors. Importantly, this C. burnetii Dot/Icm-deficient mutant was found to be defective for intracellular replication. Thus, these data indicate that C. burnetii encodes a unique subset of bacterial effector proteins translocated into host cells by the Dot/Icm apparatus, and that the cumulative activities exerted by these effectors enables C. burnetii to successfully establish a niche inside mammalian cells that supports intracellular replication.http://europepmc.org/articles/PMC3102713?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Kimberly L Carey
Hayley J Newton
Anja Lührmann
Craig R Roy
spellingShingle Kimberly L Carey
Hayley J Newton
Anja Lührmann
Craig R Roy
The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.
PLoS Pathogens
author_facet Kimberly L Carey
Hayley J Newton
Anja Lührmann
Craig R Roy
author_sort Kimberly L Carey
title The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.
title_short The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.
title_full The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.
title_fullStr The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.
title_full_unstemmed The Coxiella burnetii Dot/Icm system delivers a unique repertoire of type IV effectors into host cells and is required for intracellular replication.
title_sort coxiella burnetii dot/icm system delivers a unique repertoire of type iv effectors into host cells and is required for intracellular replication.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2011-05-01
description Coxiella burnetii, the causative agent of human Q fever, is an intracellular pathogen that replicates in an acidified vacuole derived from the host lysosomal network. This pathogen encodes a Dot/Icm type IV secretion system that delivers bacterial proteins called effectors to the host cytosol. To identify new effector proteins, the functionally analogous Legionella pneumophila Dot/Icm system was used in a genetic screen to identify fragments of C. burnetii genomic DNA that when fused to an adenylate cyclase reporter were capable of directing Dot/Icm-dependent translocation of the fusion protein into mammalian host cells. This screen identified Dot/Icm effectors that were proteins unique to C. burnetii, having no overall sequence homology with L. pneumophila Dot/Icm effectors. A comparison of C. burnetii genome sequences from different isolates revealed diversity in the size and distribution of the genes encoding many of these effectors. Studies examining the localization and function of effectors in eukaryotic cells provided evidence that several of these proteins have an affinity for specific host organelles and can disrupt cellular functions. The identification of a transposon insertion mutation that disrupts the dot/icm locus was used to validate that this apparatus was essential for translocation of effectors. Importantly, this C. burnetii Dot/Icm-deficient mutant was found to be defective for intracellular replication. Thus, these data indicate that C. burnetii encodes a unique subset of bacterial effector proteins translocated into host cells by the Dot/Icm apparatus, and that the cumulative activities exerted by these effectors enables C. burnetii to successfully establish a niche inside mammalian cells that supports intracellular replication.
url http://europepmc.org/articles/PMC3102713?pdf=render
work_keys_str_mv AT kimberlylcarey thecoxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT hayleyjnewton thecoxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT anjaluhrmann thecoxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT craigrroy thecoxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT kimberlylcarey coxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT hayleyjnewton coxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT anjaluhrmann coxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
AT craigrroy coxiellaburnetiidoticmsystemdeliversauniquerepertoireoftypeiveffectorsintohostcellsandisrequiredforintracellularreplication
_version_ 1725402615134552064

Similar Items