Abstract

Rickettsia conorii, a member of the spotted fever group (SFG) rickettsia is an obligate intracellular tick borne pathogen and is the causative agent of Mediterranean spotted fever. Aerosol transmission of rickettsia can occur and therefore, represents a bioterrorist threat for the United States. The pathogenesis of R. conorii upon transmission into the host depends on the pathogen's ability to bind to and invade target host cells. Annotation of several sequenced rickettsial genomes has identified a large family of genes termed surface cell antigens (sca) that resemble autotransporter proteins and virulence factors in Gram-negative bacteria. While many genes in this family are degenerate or split, at least 4 genes, sca0 (rompA), sca1, sca2, and sca5 (rompB) are present as complete open reading frames in R. conorii and many other SFG rickettsia. Previous results have demonstrated that Sca0 (rOmpA) and Sca5 (rOmpB) are important for the adhesion to and subsequent invasion of non-phagocytic mammalian cells and in the generation of protective humoral immune responses. However, very little is known about the function of other outermembrane proteins in SFG rickettsia pathogenesis. We have identified the first rickettsial protein-host cell receptor pair (rOmpB-Ku70) that plays an important role in the establishment of a successful infection within target human cells. Interestingly, our results have also suggested that while rOmpB-Ku70 interactions are important during the invasion process, other conserved SFG rickettsia proteins, namely rOmpA, Sca1 and Sca2, likely play important roles during pathogenesis. The experiments outlined in this proposal will address the following research interests: i. The contributions of rOmpB and Ku70 to colonization will be analyzed by using recombinant E. coli, purified proteins and protein coupled latex beads. The induction of host signaling pathways involved in the uptake process will also be analyzed using a cell culture model. ii. We will determine the contribution of rOmpB and Ku70 to the initiation and progression of SFG rickettsial disease in a murine model of infection using wild-type and Ku70 knockout mice. iii. We will also determine the roles of conserved surface antigens, namely rOmpA, Sca1 and Sca2 in mediating invasion of non-phagocytic mammalian cells. The roles of these proteins in generating protective humoral immune responses will be examined in a murine model of infection. In addition, we will identify novel ligands that interact with these conserved surface proteins in the hopes of identifying new receptors that play roles in the pathogenesis of SFG rickettsia.

Public Health Relevance

Rickettsia conorii, the causative agent of Mediterranean spotted fever, is transmitted by tick bite inoculation into the skin of the human host. Damage to target endothelial cells especially in the lungs and brain can result in the most severe manifestations of disease including pulmonary edema and interstitial pneumonia. Although infections are controlled by broad-spectrum antibiotic therapies, untreated or misdiagnosed Mediterranean spotted fever can results in severe morbidity and mortality. With the threat of the potential use of Rickettsiae and other bacteria as agents for biological terrorism, understanding the complex interplay between the pathogen and host cells is vital for the future development of novel anti-microbials and therapies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI072606-02
Application #
7779402
Study Section
Host Interactions with Bacterial Pathogens Study Section (HIBP)
Program Officer
Perdue, Samuel S
Project Start
2009-03-02
Project End
2014-02-28
Budget Start
2010-03-01
Budget End
2011-02-28
Support Year
2
Fiscal Year
2010
Total Cost
$375,456
Indirect Cost

  Institution

Name
University of Chicago
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
005421136
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Riley, Sean P; Fish, Abigail I; Del Piero, Fabio et al. (2018) Immunity against the Obligate Intracellular Bacterial Pathogen Rickettsia australis Requires a Functional Complement System. Infect Immun 86:
Riley, Sean P; Pruneau, Ludovic; Martinez, Juan J (2017) Evaluation of changes to the Rickettsia rickettsii transcriptome during mammalian infection. PLoS One 12:e0182290
Fish, Abigail I; Riley, Sean P; Singh, Birendra et al. (2017) TheRickettsia conoriiAdr1 Interacts with the C-Terminus of Human Vitronectin in a Salt-Sensitive Manner. Front Cell Infect Microbiol 7:61
Garza, Daniel A; Riley, Sean P; Martinez, Juan J (2017) Expression of Rickettsia Adr2 protein in E. coli is sufficient to promote resistance to complement-mediated killing, but not adherence to mammalian cells. PLoS One 12:e0179544
McClure, Erin E; Chávez, Adela S Oliva; Shaw, Dana K et al. (2017) Engineering of obligate intracellular bacteria: progress, challenges and paradigms. Nat Rev Microbiol 15:544-558
Riley, Sean P; Fish, Abigail I; Garza, Daniel A et al. (2016) Nonselective Persistence of a Rickettsia conorii Extrachromosomal Plasmid during Mammalian Infection. Infect Immun 84:790-7
Curto, Pedro; Simões, Isaura; Riley, Sean P et al. (2016) Differences in Intracellular Fate of Two Spotted Fever Group Rickettsia in Macrophage-Like Cells. Front Cell Infect Microbiol 6:80
Riley, Sean P; Cardwell, Marissa M; Chan, Yvonne G Y et al. (2015) Failure of a heterologous recombinant Sca5/OmpB protein-based vaccine to elicit effective protective immunity against Rickettsia rickettsii infections in C3H/HeN mice. Pathog Dis 73:ftv101
Riley, Sean P; Macaluso, Kevin R; Martinez, Juan J (2015) Electrotransformation and Clonal Isolation of Rickettsia Species. Curr Protoc Microbiol 39:3A.6.1-20
Riley, Sean P; Patterson, Jennifer L; Nava, Samantha et al. (2014) Pathogenic Rickettsia species acquire vitronectin from human serum to promote resistance to complement-mediated killing. Cell Microbiol 16:849-61

Showing the most recent 10 out of 19 publications