Abstract

The Rickettsiae are obligate intracellular bacterial pathogens that cause serious diseases, such as spotted fever and typhus. We study the model spotted fever group (SFG) species Rickettsia parkeri, which causes an eschar-associated human rickettsiosis, is experimentally tractable, and has emerging mouse models of pathogenesis, making it ideal for revealing molecular mechanisms of SFG Rickettsia infection and virulence. During infection, SFG Rickettsia invade host cells by mobilizing the actin cytoskeleton, escape from the phagosome into the cytosol, replicate while avoiding degradation by autophagy, and harness actin polymerization to promote intracellular motility and cell-cell spread. However, there are fundamental gaps in our knowledge of the molecular mechanisms by which SFG Rickettsia exploit or disrupt host cell components to promote their infection cycle. To bridge these gaps, in the current funding period we have pioneered an innovative combination of bacterial genetics and host cell biology to identify key Rickettsia factors that manipulate host cells. In unpublished work, we discovered that outer membrane protein OmpB is crucial for both invasion and avoidance of autophagy. We also observed that patatin-like phospholipase Pat1 plays a role in phagosome escape and/or autophagy evasion. Additionally, in published work, we demonstrated that Rickettsia use two actin-polymerizing surface proteins to direct sequential phases of motility ? with RickA driving early motility and surface cell antigen Sca2 driving late motility. However, key outstanding questions remain, including: How do Rickettsia engage host receptors to promote invasion? How do Rickettsia degrade membranes during phagosome escape or inhibit membrane engulfment to avoid autophagy? And how do Rickettsia coordinate and use two actin assembly factors in distinct phases of motility? Our preliminary and published findings suggest the overall hypothesis that OmpB, Pat1, RickA, and Sca2 are multifunctional proteins that mobilize or disrupt host cell components and play a crucial role in infection in vivo. This hypothesis will be tested in three Aims focused on uncovering the mechanisms through which OmpB, Pat1, RickA, and Sca2 influence invasion, intracellular survival, and motility.
The Aims are to: (1) define the role of Rickettsia surface protein OmpB in invasion and intracellular survival; (2) investigate the role of Pat1 phospholipase in phagosome escape and intracellular survival; and (3) determine how and why Rickettsia use two distinct actin-based motility mechanisms. The proposed studies will advance the field by revealing crucial molecular mechanisms used by Rickettsia and other pathogens to manipulate host cells and the importance of these mechanisms to infectivity. Our studies may also lead to improved diagnostics and treatments for rickettsial and other infections.

Public Health Relevance

Bacterial pathogens in the genus Rickettsia cause serious human diseases, including spotted fever and typhus. The proposed work seeks to fill fundamental gaps in our knowledge of key virulence mechanisms used by Rickettsia as they mobilize or disrupt host cell components to promote cellular invasion, avoid intracellular elimination, and undergo intracellular motility and spread. These studies may reveal new mechanisms of host-pathogen interactions, and new approaches for diagnosing and treating infections.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI109044-06
Application #
9694594
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Perdue, Samuel S
Project Start
2014-09-01
Project End
2023-08-31
Budget Start
2019-09-01
Budget End
2020-08-31
Support Year
6
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
University of California Berkeley
Department
Biochemistry
Type
Schools of Arts and Sciences
DUNS #
124726725
City
Berkeley
State
CA
Country
United States
Zip Code
94710

  Publications

Lamason, Rebecca L; Kafai, Natasha M; Welch, Matthew D (2018) A streamlined method for transposon mutagenesis of Rickettsia parkeri yields numerous mutations that impact infection. PLoS One 13:e0197012
Harris, Emma K; Jirakanwisal, Krit; Verhoeve, Victoria I et al. (2018) The role of Sca2 and RickA in the dissemination of Rickettsia parkeri in Amblyomma maculatum. Infect Immun :
McFarland, Adelle P; Burke, Thomas P; Carletti, Alexie A et al. (2018) RECON-Dependent Inflammation in Hepatocytes Enhances Listeria monocytogenes Cell-to-Cell Spread. MBio 9:
Lamason, Rebecca L; Welch, Matthew D (2017) Actin-based motility and cell-to-cell spread of bacterial pathogens. Curr Opin Microbiol 35:48-57
Choe, Julie E; Welch, Matthew D (2016) Actin-based motility of bacterial pathogens: mechanistic diversity and its impact on virulence. Pathog Dis :
Lamason, Rebecca L; Bastounis, Effie; Kafai, Natasha M et al. (2016) Rickettsia Sca4 Reduces Vinculin-Mediated Intercellular Tension to Promote Spread. Cell 167:670-683.e10
Welch, Matthew D (2015) Why should cell biologists study microbial pathogens? Mol Biol Cell 26:4295-301
Benanti, Erin L; Nguyen, Catherine M; Welch, Matthew D (2015) Virulent Burkholderia species mimic host actin polymerases to drive actin-based motility. Cell 161:348-60
Engström, Patrik; Krishnan, K Syam; Ngyuen, Bidong D et al. (2014) A 2-pyridone-amide inhibitor targets the glucose metabolism pathway of Chlamydia trachomatis. MBio 6:e02304-14