Journal ArticleOpen Access
A highly potent, stable, and safe dePEGylated lipopeptide against Nipah virus and related henipaviruses
Authors
Abstract
Nipah virus (NiV) poses a significant threat owing to its high mortality and the lack of approved therapeutics. Targeting the conserved heptad repeat 1 (HR1) domain of the viral fusion (F) protein constitutes a promising antiviral strategy. Also, lipopeptides derived from the human parainfluenza virus 3 (HPIV3) heptad repeat 2 (HR2) regions inhibit NiV fusion by blocking formation of the critical six-helix bundle (6-HB); however, their efficacy has been impeded by the controversial use of PEGylation. To resolve these limitations, we employed our proprietary heptad repeat 2 C-terminal fragment (HR2-CF) peptide displacement strategy that eliminates PEG and overcomes the resultant steric hindrance. The lead dePEGylated lipopeptide, VQ-P1-C16, exhibited antiviral activity comparable to that of PEGylated lipopeptide, VIKI-PEG4-C16. Further introducing Glu…
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