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RECOMBINANT PRODUCTION AND PRE-CLINICAL ANALYSIS OF FIMBRIAE SUBUNITS AS VACCINE CANDIDATES AGAINST Klebsiella pneumoniae

Grant number: 24/08321-5
Support Opportunities:Scholarships in Brazil - Post-Doctoral
Start date: February 01, 2025
End date: January 31, 2027
Field of knowledge:Biological Sciences - Microbiology - Applied Microbiology
Principal Investigator:Michelle Darrieux Sampaio Bertoncini
Grantee:Rito Santo Pereira
Host Institution: Universidade São Francisco (USF). Campus Bragança Paulista. Bragança Paulista , SP, Brazil
Associated research grant:23/10579-8 - EVALUATION OF TYPE I AND TYPE III FRIMBRIAE COMPONENTS AS VACCINE CANDIDATES AGAINST Klebsiella pneumoniae INFECTIONS, AP.R

Abstract

Klebsiella pneumoniae is a Gram-negative bacterium that commonly colonizes human mucosae, from where it can spread and cause serious infections. The high morbidity and mortality rates associated with K. pneumoniae, coupled with the alarming increase in antimicrobial resistance, encourage the development of strategies to prevent these infections. In that sense, vaccines based on surface proteins are a promising approach since these antigens are usually conserved among clinical strains and accessible to the host immune system. Fimbriae are macromolecular structures exposed at the bacterial surface that play a role in adhesion and biofilm formation. K. pneumoniae expresses two types of fimbriae, I and III, that are important for its virulence. The present work aims to investigate the vaccine potential of K. pneumoniae fimbriae subunits in mouse infection models. The antigens will be produced as recombinant proteins in E. coli, purified, and used to immunize mice. The immune responses will be characterized, and protection will be assessed against urinary and respiratory infections, as well as sepsis. The induced antibodies will be evaluated in functional assays to test their ability to bind to the native fimbriae on the bacterial surface and promote complement deposition and phagocytic killing. The effect of antibodies on biofilm formation and bacterial adhesion to respiratory and urinary epithelial cells will also be investigated. The results of this study should contribute to the development of prophylactic measures against K. pneumoniae and help understand the role of fimbriae in bacterial virulence.

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