Inhibition of Influenza A Virus Infection by Fucoidan Targeting Viral Neuraminidase and Cellular EGFR Pathway

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作者
Wei Wang
Jiandong Wu
Xiaoshuang Zhang
Cui Hao
Xiaoliang Zhao
Guangling Jiao
Xindi Shan
Wenjing Tai
Guangli Yu
机构
[1] Key Laboratory of Marine Drugs,
[2] Ministry of Education,undefined
[3] Ocean University of China,undefined
[4] Shandong Provincial Key Laboratory of Glycoscience and Glycotechnology,undefined
[5] Ocean University of China,undefined
[6] Institute of Cerebrovascular Diseases,undefined
[7] Affiliated Hospital of Qingdao University Medical College,undefined
[8] Laboratory for Marine Drugs and Bioproducts of Qingdao National Laboratory for Marine Science and Technology,undefined
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Development of novel anti-influenza A virus (IAV) drugs with high efficiency and low toxicity is critical for preparedness against influenza outbreaks. Herein, we investigated the anti-IAV activities and mechanisms of fucoidan in vitro and in vivo. The results showed that a fucoidan KW derived from brown algae Kjellmaniella crassifolia effectively blocked IAV infection in vitro with low toxicity. KW possessed broad anti-IAV spectrum and low tendency of induction of viral resistance, superior to the anti-IAV drug amantadine. KW was capable of inactivating virus particles before infection and blocked some stages after adsorption. KW could bind to viral neuraminidase (NA) and inhibit the activity of NA to block the release of IAV. KW also interfered with the activation of EGFR, PKCα, NF-κB, and Akt, and inhibited both IAV endocytosis and EGFR internalization in IAV-infected cells, suggesting that KW may also inhibit cellular EGFR pathway. Moreover, intranasal administration of KW markedly improved survival and decreased viral titers in IAV-infected mice. Therefore, fucoidan KW has the potential to be developed into a novel nasal drop or spray for prevention and treatment of influenza in the future.
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