Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila

Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila

Helicobacter pylori strains containing the CagA protein are associated with high risk of gastric diseases including atrophic gastritis, peptic ulcers, and gastric cancer. CagA is injected into host cells via a Type IV secretion system where it activates growth factor-like signaling, disrupts cell-ce...

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Main Authors: David W. Reid, Jonathan B. Muyskens, James T. Neal, Gino W. Gaddini, Lucy Y. Cho, Anica M. Wandler, Crystal M. Botham, Karen eGuillemin
Format: Article
Language:English
Published: Frontiers Media S.A. 2012-03-01
Series:Frontiers in Cellular and Infection Microbiology
Subjects:
Drosophila
Eye
Helicobacter pylori
Epithelia
CagA
coracle
Online Access:http://journal.frontiersin.org/Journal/10.3389/fcimb.2012.00024/full
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spelling doaj-fb98ab2db6a9482584079e25b4b7bf7b2020-11-24T21:26:45ZengFrontiers Media S.A.Frontiers in Cellular and Infection Microbiology2235-29882012-03-01210.3389/fcimb.2012.0002421074Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in DrosophilaDavid W. Reid0Jonathan B. Muyskens1James T. Neal2Gino W. Gaddini3Lucy Y. Cho4Anica M. Wandler5Crystal M. Botham6Karen eGuillemin7University of OregonUniversity of OregonUniversity of OregonUniversity of OregonUniversity of OregonUniversity of OregonUniversity of OregonUniversity of OregonHelicobacter pylori strains containing the CagA protein are associated with high risk of gastric diseases including atrophic gastritis, peptic ulcers, and gastric cancer. CagA is injected into host cells via a Type IV secretion system where it activates growth factor-like signaling, disrupts cell-cell junctions, and perturbs host cell polarity. Using a transgenic Drosophila model, we have shown that CagA expression disrupts the morphogenesis of epithelial tissues such as the adult eye. Here we describe a genetic screen to identify modifiers of CagA-induced eye defects. We determined that reducing the copy number of genes encoding components of signaling pathways known to be targeted by CagA, such as the epidermal growth factor receptor, modified the CagA-induced eye phenotypes. In our screen of just over half the Drosophila genome, we discovered 12 genes that either suppressed or enhanced CagA’s disruption of the eye epithelium. Included in this list are genes involved in epithelial integrity, intracellular trafficking, and signal transduction. We investigated the mechanism of one suppressor, encoding the epithelial polarity determinant and junction protein Coracle, which is homologous to the mammalian Protein 4.1. We found that loss of a single copy of coracle improved the organization and integrity of larval retinal epithelia expressing CagA, but did not alter CagA’s localization to cell junctions. Loss of a single copy of the coracle antagonist crumbs enhanced CagA-associated disruption of the larval retinal epithelium, whereas overexpression of crumbs suppressed this phenotype. Collectively, these results point to new cellular pathways whose disruption by CagA are likely to contribute to H. pylori-associated disease pathology.http://journal.frontiersin.org/Journal/10.3389/fcimb.2012.00024/fullDrosophilaEyeHelicobacter pyloriEpitheliaCagAcoracle
collection DOAJ
language English
format Article
sources DOAJ
author David W. Reid
Jonathan B. Muyskens
James T. Neal
Gino W. Gaddini
Lucy Y. Cho
Anica M. Wandler
Crystal M. Botham
Karen eGuillemin
spellingShingle David W. Reid
Jonathan B. Muyskens
James T. Neal
Gino W. Gaddini
Lucy Y. Cho
Anica M. Wandler
Crystal M. Botham
Karen eGuillemin
Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila
Frontiers in Cellular and Infection Microbiology
Drosophila
Eye
Helicobacter pylori
Epithelia
CagA
coracle
author_facet David W. Reid
Jonathan B. Muyskens
James T. Neal
Gino W. Gaddini
Lucy Y. Cho
Anica M. Wandler
Crystal M. Botham
Karen eGuillemin
author_sort David W. Reid
title Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila
title_short Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila
title_full Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila
title_fullStr Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila
title_full_unstemmed Identification of Genetic Modifiers of CagA-Induced Epithelial Disruption in Drosophila
title_sort identification of genetic modifiers of caga-induced epithelial disruption in drosophila
publisher Frontiers Media S.A.
series Frontiers in Cellular and Infection Microbiology
issn 2235-2988
publishDate 2012-03-01
description Helicobacter pylori strains containing the CagA protein are associated with high risk of gastric diseases including atrophic gastritis, peptic ulcers, and gastric cancer. CagA is injected into host cells via a Type IV secretion system where it activates growth factor-like signaling, disrupts cell-cell junctions, and perturbs host cell polarity. Using a transgenic Drosophila model, we have shown that CagA expression disrupts the morphogenesis of epithelial tissues such as the adult eye. Here we describe a genetic screen to identify modifiers of CagA-induced eye defects. We determined that reducing the copy number of genes encoding components of signaling pathways known to be targeted by CagA, such as the epidermal growth factor receptor, modified the CagA-induced eye phenotypes. In our screen of just over half the Drosophila genome, we discovered 12 genes that either suppressed or enhanced CagA’s disruption of the eye epithelium. Included in this list are genes involved in epithelial integrity, intracellular trafficking, and signal transduction. We investigated the mechanism of one suppressor, encoding the epithelial polarity determinant and junction protein Coracle, which is homologous to the mammalian Protein 4.1. We found that loss of a single copy of coracle improved the organization and integrity of larval retinal epithelia expressing CagA, but did not alter CagA’s localization to cell junctions. Loss of a single copy of the coracle antagonist crumbs enhanced CagA-associated disruption of the larval retinal epithelium, whereas overexpression of crumbs suppressed this phenotype. Collectively, these results point to new cellular pathways whose disruption by CagA are likely to contribute to H. pylori-associated disease pathology.
topic Drosophila
Eye
Helicobacter pylori
Epithelia
CagA
coracle
url http://journal.frontiersin.org/Journal/10.3389/fcimb.2012.00024/full
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