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  4. Conserved molecular chaperone PrsA stimulates protective immunity against group A Streptococcus
 
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Conserved molecular chaperone PrsA stimulates protective immunity against group A Streptococcus

Journal
NPJ vaccines
Journal Volume
9
Journal Issue
1
Date Issued
2024-02-26
Author(s)
Lai, Chien-Yu
Xie, Jia-Xun
Lai, Meng-Chih
Wu, Zhao-Yi
JR-SHIUAN LIN  
Chi, Chia-Yu
YU-TSUNG HUANG  
Chiang-Ni, Chuan
Walker, Mark J
YUNG-CHI CHANG  
DOI
10.1038/s41541-024-00839-7
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/641482
URL
https://api.elsevier.com/content/abstract/scopus_id/85185928985
Abstract
Group A Streptococcus (GAS) is a significant human pathogen that poses a global health concern. However, the development of a GAS vaccine has been challenging due to the multitude of diverse M-types and the risk of triggering cross-reactive immune responses. Our previous research has identified a critical role of PrsA1 and PrsA2, surface post-translational molecular chaperone proteins, in maintaining GAS proteome homeostasis and virulence traits. In this study, we aimed to further explore the potential of PrsA1 and PrsA2 as vaccine candidates for preventing GAS infection. We found that PrsA1 and PrsA2 are highly conserved among GAS isolates, demonstrating minimal amino acid variation. Antibodies specifically targeting PrsA1/A2 showed no cross-reactivity with human heart proteins and effectively enhanced neutrophil opsonophagocytic killing of various GAS serotypes. Additionally, passive transfer of PrsA1/A2-specific antibodies conferred protective immunity in infected mice. Compared to alum, immunization with CFA-adjuvanted PrsA1/A2 induced higher levels of Th1-associated IgG isotypes and complement activation and provided approximately 70% protection against invasive GAS challenge. These findings highlight the potential of PrsA1 and PrsA2 as universal vaccine candidates for the development of an effective GAS vaccine.
SDGs

[SDGs]SDG3

Publisher
Nature Research
Type
journal article

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