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Identification and Evaluation of Recombinant Outer Membrane Proteins as Vaccine Candidates Against Klebsiella pneumoniae.


ABSTRACT: Klebsiella pneumoniae found in the normal flora of the human oral and intestinal tract mainly causes hospital-acquired infections but can also cause community-acquired infections. To date, most clinical trials of vaccines against K. pneumoniae have ended in failure. Furthermore, no single conserved protein has been identified as an antigen candidate to accelerate vaccine development. In this study, we identified five outer membrane proteins of K. pneumoniae, namely, Kpn_Omp001, Kpn_Omp002, Kpn_Omp003, Kpn_Omp004, and Kpn_Omp005, by using reliable second-generation proteomics and bioinformatics. Mice vaccinated with these five KOMPs elicited significantly higher antigen-specific IgG, IgG1, and IgG2a. However, only Kpn_Omp001, Kpn_Omp002, and Kpn_Omp005 were able to induce a protective immune response with two K. pneumoniae infection models. These protective effects were accompanied by the involvement of different immune responses induced by KOMPs, which included KOMPs-specific IFN-γ-, IL4-, and IL17A-mediated immune responses. These findings indicate that Kpn_Omp001, Kpn_Omp002, and Kpn_Omp005 are three potential Th1, Th2, and Th17 candidate antigens, which could be developed into multivalent and serotype-independent vaccines against K. pneumoniae infection.

SUBMITTER: Zhang BZ 

PROVIDER: S-EPMC8564470 | biostudies-literature | 2021

REPOSITORIES: biostudies-literature

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Identification and Evaluation of Recombinant Outer Membrane Proteins as Vaccine Candidates Against <i>Klebsiella pneumoniae</i>.

Zhang Bao-Zhong BZ   Hu Danyu D   Dou Ying Y   Xiong Lifeng L   Wang Xiaolei X   Hu Jingchu J   Xing Shao-Zhen SZ   Li Wenjun W   Cai Jian-Piao JP   Jin Meiling M   Zhang Mengya M   Lin Qiubin Q   Li Min M   Yuen Kwok-Yung KY   Huang Jian-Dong JD  

Frontiers in immunology 20211020


<i>Klebsiella pneumoniae</i> found in the normal flora of the human oral and intestinal tract mainly causes hospital-acquired infections but can also cause community-acquired infections. To date, most clinical trials of vaccines against <i>K. pneumoniae</i> have ended in failure. Furthermore, no single conserved protein has been identified as an antigen candidate to accelerate vaccine development. In this study, we identified five outer membrane proteins of <i>K. pneumoniae</i>, namely, Kpn_Omp0  ...[more]

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