Programmable Macrophage Vesicle Based Bionic Self‐Adjuvanting Vaccine for Immunization against Monkeypox Virus

The emergence of monkeypox has become a global health threat after the COVID‐19 pandemic. Due to the lack of available specifically treatment against MPV, developing an available vaccine is thus the most prospective and urgent strategy. Herein, a programmable macrophage vesicle based bionic self‐adj...

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Bibliographic Details
Published in:Advanced science 2025-01, Vol.12 (1), p.e2408608-n/a
Main Authors: Lin, Weiqiang, Shen, Chenguang, Li, Mengjun, Ma, Shengchao, Liu, Chenxin, Huang, Jialin, Ren, Zuning, Yang, Yuechao, Zhao, Minghai, Xie, Qiulin, Guo, Shuang, Wang, Wei, Wang, Kaiyuan, Ma, Qiang, Jiang, Yideng, Zheng, Judun, Liao, Yuhui
Format: Article
Language:English
Subjects:
Adjuvants
Adjuvants, Immunologic - administration & dosage
Adjuvants, Vaccine
Animals
Antigens
Biomarkers
bionic vaccine
Bionics - methods
Chemokines
Cytokines
Disease Models, Animal
extracellular enveloped virion
Immunity (Disease)
Immunization - methods
Infections
Infectious diseases
intracellular mature virion
macrophage vesicles
Macrophages - immunology
Mice
monkeypox virus
Mpox
Pathogens
Protein expression
Proteins
Smallpox
Vaccines
Viral Vaccines - administration & dosage
Viral Vaccines - immunology
Viruses
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Summary:The emergence of monkeypox has become a global health threat after the COVID‐19 pandemic. Due to the lack of available specifically treatment against MPV, developing an available vaccine is thus the most prospective and urgent strategy. Herein, a programmable macrophage vesicle based bionic self‐adjuvanting vaccine (AM@AEvs‐PB) is first developed for defending against monkeypox virus (MPV). Based on MPV‐related antigen‐stimulated macrophage‐derived vesicles, the nanovaccine is constructed by loading the mature virion (MV)‐related intracellular protein (A29L/M1R) and simultaneously modifying with the enveloped virion (EV) antigen (B6R), enabling them to effectively promote antigen presentation and enhance adaptive immune through self‐adjuvant strategy. Owing to the synergistic properties of bionic vaccine coloaded MV and EV protein in defensing MPV, the activation ratio of antigen‐presenting cells is nearly four times than that of single antigen in the same dose, resulting in stronger immunity in host. Notably, intramuscular injection uptake of AM@AEvs‐PB demonstrated vigorous immune‐protective effects in the mouse challenge attempt, offering a promising strategy for pre‐clinical monkeypox vaccine development. The monkeypox‐specific bionic vaccine (AM@AEvs‐PB) is consists of IMV antigens (A29L, M1R), the EEV antigen (B6R), and MPV‐preactivated macrophagederived vesicles. AM@AEvs‐PB can induce enhanced innate immune responses, promote cross‐presentation of antigens to dendritic cells (DCs), and elicit robust adaptive immune responses, realizing immunization protection against Monkeypox Virus.
ISSN:2198-3844
2198-3844
DOI:10.1002/advs.202408608