Streptococcus pneumoniae Cell Wall-Localized Trigger Factor Elicits a Protective Immune Response and Contributes to Bacterial Adhesion to the Host

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作者
Aviad Cohen
Shani Troib
Shahar Dotan
Hastyar Najmuldeen
Hasan Yesilkaya
Tatyana Kushnir
Marilou Shagan
Maxim Portnoi
Hannie Nachmani
Rachel Benisty
Michael Tal
Ronald Ellis
Vered Chalifa-Caspi
Ron Dagan
Yaffa Mizrachi Nebenzahl
机构
[1] Ben-Gurion University of the Negev,The Shraga Segal Department of Microbiology, Immunology and Genetics, Faculty of Health Sciences
[2] NasVax Ltd.,Department of Infection, Immunity and Inflammation to Department of Respiratory Sciences
[3] University of Leicester,Department of Biology
[4] College of Science,Bioinformatics Core Facility
[5] University of Sulaimani,The Faculty of Health Sciences
[6] National Institute for Biotechnology in the Negev (NIBN),undefined
[7] Ben-Gurion University of the Negev,undefined
[8] Ben-Gurion University of the Negev,undefined
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Trigger factor (TF) has a known cytoplasmic function as a chaperone. In a previous study we showed that pneumococcal TF is also cell-wall localized and this finding combined with the immunogenic characteristic of TF, has led us to determine the vaccine potential of TF and decipher its involvement in pneumococcal pathogenesis. Bioinformatic analysis revealed that TF is conserved among pneumococci and has no human homologue. Immunization of mice with recombinant (r)TF elicited a protective immune response against a pneumococcal challenge, suggesting that TF contributes to pneumococcal pathogenesis. Indeed, rTF and an anti-rTF antiserum inhibited bacterial adhesion to human lung derived epithelial cells, indicating that TF contributes to the bacterial adhesion to the host. Moreover, bacteria lacking TF demonstrated reduced adhesion, in vitro, to lung-derived epithelial cells, neural cells and glial cells. The reduced adhesion could be restored by chromosomal complementation. Furthermore, bacteria lacking TF demonstrated significantly reduced virulence in a mouse model. Taken together, the ability of rTF to elicit a protective immune response, involvement of TF in bacterial adhesion, conservation of the protein among pneumococcal strains and the lack of human homologue, all suggest that rTF can be considered as a future candidate vaccine with a much broader coverage as compared to the currently available pneumococcal vaccines.
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