The FIP-HRC lipid conjugate demonstrated high antiviral potency in vitro and effectively prevented measles virus infection in cotton rats by stabilizing the prefusion F protein structure.
Does FIP-HRC lipid conjugate prevent Measles virus infection in vitro and in cotton rat models?
A novel FIP-HRC lipid conjugate demonstrates potent antiviral activity against Measles virus by targeting and stabilizing the prefusion fusion protein structure in vitro and in vivo.
Measles virus (MeV) infection remains a significant public health threat despite ongoing global efforts to increase vaccine coverage. As eradication of MeV stalls, and vulnerable populations expand, effective antivirals against MeV are in high demand. Here, we describe the development of an antiviral peptide that targets the MeV fusion (F) protein. This antiviral peptide construct is composed of a carbobenzoxy-d-Phe-l-Phe-Gly (fusion inhibitor peptide; FIP) conjugated to a lipidated MeV F C-terminal heptad repeat (HRC) domain derivative. Initial in vitro testing showed high antiviral potency and specific targeting of MeV F-associated cell plasma membranes, with minimal cytotoxicity. The FIP and HRC-derived peptide conjugates showed synergistic antiviral activities when administered individually. However, their chemical conjugation resulted in markedly increased antiviral potency. In vitro mechanistic experiments revealed that the FIP–HRC lipid conjugate exerted its antiviral activity predominantly through stabilization of the prefusion F, while HRC-derived peptides alone act predominantly on the F protein after its activation. Coupled with in vivo experiments showing effective prevention of MeV infection in cotton rats, FIP–HRC lipid conjugates show promise as potential MeV antivirals via specific targeting and stabilization of the prefusion MeV F structure.
Bovier et al. (Thu,) conducted a other in Measles virus (MeV) infection. FIP-HRC lipid conjugate vs. Individual FIP and HRC-derived peptides was evaluated on Antiviral activity and prevention of MeV infection. The FIP-HRC lipid conjugate demonstrated high antiviral potency in vitro and effectively prevented measles virus infection in cotton rats by stabilizing the prefusion F protein structure.