| Literature DB >> 35674445 |
Alan Basset1, Emma Wall2,3, Daniela M Ferreira4, Richard Malley1, Elena Mitsi4, Chloe Deshusses1, Raecliffe Daly1, Sherin Pojar4, Jesús Reiné4, Jose Afonso Guerra-Assuncao2, Brigitte Denis5, Simon P Jochems4, Robert Heyderman2, Jeremy Brown2, Ying-Jie Lu1.
Abstract
The advent of pneumococcal conjugate vaccines led to the near disappearance of most of the included serotypes in high-income settings but also the rise of nonvaccine-type colonization and disease. Alternative strategies, using genetically conserved proteins as antigens, have been evaluated preclinically and clinically for years, so far unsuccessfully. One possible explanation for the failure of these efforts is that the choice of antigens may not have been sufficiently guided by an understanding of the gene expression pattern in the context of infection. Here, we present a targeted transcriptomic analysis of 160 pneumococcal genes encoding bacterial surface-exposed proteins in mouse models, human colonization, and human meningitis. We present the overlap of these different transcriptomic profiles. We identify two bacterial genes that are highly expressed in the context of mouse and human infection: SP_0282, an IID component of a mannose phosphotransferase system (PTS), and SP_1739, encoding RNase Y. We show that these two proteins can confer protection against pneumococcal nasopharyngeal colonization and intraperitoneal challenge in a murine model and generate opsonophagocytic antibodies. This study emphasizes and confirms the importance of studies of pneumococcal gene expression of bacterial surface proteins during human infection and colonization and may pave the way for the selection of a protein-based vaccine candidate.Entities:
Keywords: colonization; invasive disease; pneumococcus; transcriptome
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Year: 2022 PMID: 35674445 PMCID: PMC9302103 DOI: 10.1128/iai.00175-22
Source DB: PubMed Journal: Infect Immun ISSN: 0019-9567 Impact factor: 3.609