Dissertations and Theses (Open Access)
Author ORCID Identifier
0000-0002-1591-0264
Date of Graduation
5-2025
Document Type
Dissertation (PhD)
Program Affiliation
Molecular and Translational Biology
Degree Name
Doctor of Philosophy (PhD)
Advisor/Committee Chair
Scott Evans, MD
Committee Member
Jun-ichi Abe, MD, PhD
Committee Member
George Calin, MD, PhD
Committee Member
Shane Cunha, PhD
Committee Member
Harry Karmouty-Quintana, PhD
Committee Member
Samuel Shelburne, MD, PhD
Abstract
Pneumonia is the leading infectious cause of death worldwide and presents a continuing risk among immunocompromised patients. Our work has been focused for many years on the phenomenon of inducible epithelial resistance, where activation of the innate immune response in the airway epithelium is necessary and sufficient to produce a pathogen-killing but self-protective environment to prevent severe disease. Inducible resistance is pathogen-agnostic and has been demonstrated against an array of respiratory infections. We achieve this using a combination of pattern recognition receptor agonists – Pam2CSK4 and ODN M362 being the current formulation – which produce synergistic levels of pathogen reduction and protection in our models. Recent endeavors by members of our lab have sought to identify and characterize the mechanisms which contribute to synergy including the release of reactive oxygen species, production of antimicrobial peptides and proinflammatory cytokines, and the identification of alternative receptors and pathways for our ligands. In this work, I have developed a new model for multi-system coronavirus disease using the murine coronavirus MHV-A59 which infects the respiratory epithelium before disseminating to multiple organ systems. Pam2/ODN treatment decreased morbidity and mortality associated with MHV infection, limited lung injury and spread to other organs, and produced a unique gene expression signature in epithelial cells to diminish the impact of infection. I have also pursued describing the activation cascade of RIG-I as a newly identified receptor for ODN. I have demonstrated that the RIG-I:ODN interaction is not determined by ODN sequence, secondary structure, or CpG motifs, but is instead dependent on the phosphorothioate-modified backbone common in immunostimulatory ODNs. I have also shown that ODN leads to the activation of IRF3, a transcription factor and downstream component of RIG-I signaling, as well as the upregulation of IRF3-regulated genes. Together, the findings of this thesis expand our understanding of inducible epithelial resistance both at the level of molecular mechanisms of protection and at the translational level of characterizing new applications against novel pathogens
Recommended Citation
Longmire, Michael, "Expanding inducible epithelial resistance against pneumonia: novel virus, novel receptor" (2025). Dissertations and Theses (Open Access). 1455.
https://digitalcommons.library.tmc.edu/utgsbs_dissertations/1455
Keywords
pneumonia, pattern recognition receptors, epithelium, coronavirus, influenza, innate immunity
Included in
Biochemistry Commons, Immunity Commons, Immunology of Infectious Disease Commons, Nucleic Acids, Nucleotides, and Nucleosides Commons, Respiratory Tract Diseases Commons, Virology Commons, Virus Diseases Commons