An intranasal nanoparticle STING agonist protects against respiratory viruses in animal models

Author:

Leekha Ankita,Saeedi Arash,Kumar Monish,Sefat K. M. Samiur Rahman,Martinez-Paniagua Melisa,Meng Hui,Fathi Mohsen,Kulkarni Rohan,Reichel Kate,Biswas Sujit,Tsitoura Daphne,Liu Xinli,Cooper Laurence J. N.,Sands Courtney M.,Das Vallabh E.,Sebastian Manu,Hurst Brett L.ORCID,Varadarajan NavinORCID

Abstract

AbstractRespiratory viral infections cause morbidity and mortality worldwide. Despite the success of vaccines, vaccination efficacy is weakened by the rapid emergence of viral variants with immunoevasive properties. The development of an off-the-shelf, effective, and safe therapy against respiratory viral infections is thus desirable. Here, we develop NanoSTING, a nanoparticle formulation of the endogenous STING agonist, 2′−3′ cGAMP, to function as an immune activator and demonstrate its safety in mice and rats. A single intranasal dose of NanoSTING protects against pathogenic strains of SARS-CoV-2 (alpha and delta VOC) in hamsters. In transmission experiments, NanoSTING reduces the transmission of SARS-CoV-2 Omicron VOC to naïve hamsters. NanoSTING also protects against oseltamivir-sensitive and oseltamivir-resistant strains of influenza in mice. Mechanistically, NanoSTING upregulates locoregional interferon-dependent and interferon-independent pathways in mice, hamsters, as well as non-human primates. Our results thus implicate NanoSTING as a broad-spectrum immune activator for controlling respiratory virus infection.

Publisher

Springer Science and Business Media LLC

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