| Literature DB >> 34592151 |
Jie Gao1, Bao-Rui Zhao1, Hui Zhang1, Yan-Lin You2, Fang Li3, Xian-Wei Wang4.
Abstract
Drosophila Vago is a small antiviral peptide. Its ortholog in Culex mosquito was found to be an interferon-like cytokine that limits virus replication through activating Jak/Stat signaling. However, this activation is independent of Domeless, the sole homolog of vertebrate type I cytokine receptor. How Vago activates the Jak/Stat pathway remains unknown. Herein, we report this process is dependent on integrin in kuruma shrimp (Marsupenaeus japonicus). Shrimp Vago-like (MjVago-L) plays an antiviral role by activating the Jak/Stat pathway and inducing Stat-regulated Ficolin. Blocking integrin abrogates the role of MjVago-L. The interaction between MjVago-L and integrin β3 is confirmed. An Asp residue in MjVago-L is found critical for the interaction and MjVago-L's antiviral role. Moreover, Fak, a key adaptor of integrin signaling, mediates MjVago-L-induced Jak/Stat activation. Therefore, this study reveals that integrin, as the receptor of MjVago-L, mediates Jak/Stat activation. The establishment of the MjVago-L/integrin/Fak/Jak/Stat/Ficolin axis provides insights into antiviral cytokine signaling in invertebrates.Entities:
Keywords: Jak/Stat; arthropod; cytokine; ficolin; integrin; invertebrate; vago; white spot syndrome virus
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Year: 2021 PMID: 34592151 DOI: 10.1016/j.celrep.2021.109761
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423