Selective TLR ligand stimulation enhances in vivo mosquito-borne flavivirus pathogenicity

Tatsuya Suzuki(Juntendo University), Yuka Miyata(The University of Osaka), Saori Haga(The University of Osaka), Yumi Itoh(Juntendo University), Tsukika Tanaka(Juntendo University), Tomomi Hishinuma(Juntendo University), Yasuko Orba(Sapporo International University), Yuki Eshita(Hokkaido University), Yusuke Sakai(National Institute of Infectious Diseases), Takeshi Kurosu(National Institute of Infectious Diseases), Shigeru Tajima(National Institute of Infectious Diseases), Chang‐Kweng Lim(National Institute of Infectious Diseases), Masayuki Saijo(National Institute of Infectious Diseases), Atsushi Yamanaka(The University of Osaka), Thipruethai Phanitchat(Mahidol University), Ronald Enrique Morales Vargas(Mahidol University), Daisuke Okuzaki(The University of Osaka), Hirofumi Sawa(Sapporo International University), Takashi Satoh(Tokyo Medical and Dental University), Shizuo Akira(The University of Osaka), Yoshiharu Matsuura(The University of Osaka), Toru Okamoto(Juntendo University)
Cell Reports
August 29, 2025
Cited by 5Open Access
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Abstract

Mosquito saliva facilitates pathogen transmission and enhances the severity of diseases caused by mosquito-borne viruses; however, the underlying mechanisms are unknown. Here, we demonstrate that mosquito salivary gland extracts (SGEs) enhance flaviviral pathogenicity in vivo by activating innate immune responses following the accumulation of immune cells at the infection site. Among the innate immune signaling pathways, the TLR2 pathway enhances flaviviral pathogenicity in a manner similar to that of SGEs. TLR2 ligands and SGEs induce neutrophils to secrete chemokines that recruit virus-permissive monocytes and macrophages to infection sites. SGEs activate TLR2, and inhibition of TLR2 signaling markedly reduces mosquito-saliva-enhanced viral pathogenicity. Overall, this study provides important insights into vector-host interactions and suggests that TLR2 is a potential target for preventing mosquito-borne flaviviral infection.


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