A Non-Nucleotide STING Agonist MSA-2 Synergized with Manganese in Enhancing STING Activation to Elicit Potent Anti-RNA Virus Activity in the Cells

Author:

Lin Hanrui1,Zhang Rui1,Xiang Hanyi1,Lin Xinqian1,Huang Xiongting1,Chen Jingsong1,Zhou Long1ORCID,Zhang Zhidong1ORCID,Li Yanmin1

Affiliation:

1. Key Laboratory of Animal Medicine of Sichuan Province, College of Animal and Veterinary Sciences, Southwest Minzu University, Chengdu 610093, China

Abstract

Both Manganese (Mn2+) and MSA-2 can activate the downstream signal pathway through stimulator of interferon genes (STING) and induce the expression of type I interferon, which is important for hosts to protect against DNA viruses. However, its effect on RNA viruses remains unknown. In this study, we used Seneca Valley virus (SVV) as a model RNA virus to investigate the inhibitory effects of Mn2+ and MSA-2 on the virus replication in the porcine cells (PK-15 cells). The results showed that both MSA-2 and Mn2+ were able to inhibit the SVV replication in PK-15 cells. The combination of MAS-2 and Mn2+ could confer better protection against SVV. Further studies showed that MSA-2 and Mn2+ could activate TBK1, IRF3 and NFκB through STING and induce the expression of IFN-β, IL-6 and TNF-α. The present study confirmed that MSA-2 synergized with Mn2+ in STING activation to generate a better antiviral effect in vitro, which would be helpful for the further development of effective antiviral drugs in the future.

Funder

Natural Science Foundation of Sichuan Province

Southwest Mizu University Double World-Class Project

Southwest Mizu University Research Startup Funds

Southwest Minzu University Innovation and entrepreneurship training program for undergraduates

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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