Abstract

The microbial pathogen Yersinia pestis, was the causal agent for the devastating plagues killing millions of people in Europe, India, China and even the United States. The pathogen persists in flea/rodent ecosystems on almost every continent and can cause a short but extremely painful death in untreated victims. This pathogen is a potential weapon that may be used for Biowarfare and therefore it is important to understand how this toxin works. Yersinia's modus operandi includes evading phagocytosis, destroying the host defense system and inducing programmed cell death in the target host cell. Only six proteins called Yersinia outer proteins (Yops) encoded on a virulence plasmid efficiently carry out these activities; one of them, YopJ, both blocks cytokine production and promotes apoptosis in target host cells. YopJ, a 32kD protein, blocks all major signaling pathways involved in cytokine production including all the MAPK signaling pathways and the NFKappaB pathway. The family of YopJ proteins, composed of effectors from plant and animal pathogens, has structural homology to a clan of cysteine proteases that includes adenoviral proteases and the ubiquitin-like protein proteases. Consistent with the proposal that YopJ is a hydrolase, an intact catalytic site is required for YopJ to block the activation of the evolutionarily conserved super family of MAPK kinases (MKK). Based on these observations, we propose that YopJ uses a novel mechanism to disrupt a component of the signaling machinery that is required for the activity of all of the aforementioned kinase-driven signaling cascades. We propose three Specific Aims to investigate our hypothesis: (i) To characterize the target(s) of the Yersinia effector YopJ in the mammalian MAPK signaling pathway. (ii) To characterize the target(s) of the Yersinia effector YopJ in the NFkappaB signaling pathway. (iii) To characterize the hydrolytic activity of YopJ in vitro. Results from these studies will identify the targets of YopJ and characterize the inhibitory activity of YopJ that will lead to the understanding of an evolutionarily conserved mechanism of regulation that is necessary for intracellular transmission of signals. Discovery of this mechanism is essential for understanding how signaling pathways are regulated in both plants and animals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
1R01AI056404-01
Application #
6681211
Study Section
Cell Development and Function Integrated Review Group (CDF)
Program Officer
Schaefer, Michael R
Project Start
2003-09-30
Project End
2008-01-31
Budget Start
2003-09-30
Budget End
2004-01-31
Support Year
1
Fiscal Year
2003
Total Cost
$90,999
Indirect Cost

  Institution

Name
University of Texas Sw Medical Center Dallas
Department
Biochemistry
Type
Schools of Medicine
DUNS #
800771545
City
Dallas
State
TX
Country
United States
Zip Code
75390

  Publications

Li, Peng; Kinch, Lisa N; Ray, Ann et al. (2017) Acute Hepatopancreatic Necrosis Disease-Causing Vibrio parahaemolyticus Strains Maintain an Antibacterial Type VI Secretion System with Versatile Effector Repertoires. Appl Environ Microbiol 83:
De Nisco, Nicole J; Kanchwala, Mohammed; Li, Peng et al. (2017) The cytotoxic type 3 secretion system 1 of Vibrio rewires host gene expression to subvert cell death and activate cell survival pathways. Sci Signal 10:
Ray, Ann; Kinch, Lisa N; de Souza Santos, Marcela et al. (2016) Proteomics Analysis Reveals Previously Uncharacterized Virulence Factors in Vibrio proteolyticus. MBio 7:
Sreelatha, Anju; Bennett, Terry L; Carpinone, Emily M et al. (2015) Vibrio effector protein VopQ inhibits fusion of V-ATPase-containing membranes. Proc Natl Acad Sci U S A 112:100-5
Salomon, Dor; Klimko, John A; Trudgian, David C et al. (2015) Type VI Secretion System Toxins Horizontally Shared between Marine Bacteria. PLoS Pathog 11:e1005128
Yu, Xiaobo; Woolery, Andrew R; Luong, Phi et al. (2014) Copper-catalyzed azide-alkyne cycloaddition (click chemistry)-based detection of global pathogen-host AMPylation on self-assembled human protein microarrays. Mol Cell Proteomics 13:3164-76
Salomon, Dor; Klimko, John A; Orth, Kim (2014) H-NS regulates the Vibrio parahaemolyticus type VI secretion system 1. Microbiology 160:1867-73
Salomon, Dor; Kinch, Lisa N; Trudgian, David C et al. (2014) Marker for type VI secretion system effectors. Proc Natl Acad Sci U S A 111:9271-6
Lewallen, Daniel M; Sreelatha, Anju; Dharmarajan, Venkatasubramanian et al. (2014) Inhibiting AMPylation: a novel screen to identify the first small molecule inhibitors of protein AMPylation. ACS Chem Biol 9:433-42
de Souza Santos, Marcela; Orth, Kim (2014) Intracellular Vibrio parahaemolyticus escapes the vacuole and establishes a replicative niche in the cytosol of epithelial cells. MBio 5:e01506-14

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