PLoS Pathogens (Jan 2024)

Cathelicidin peptide analogues inhibit EV71 infection through blocking viral entry and uncoating.

  • Tingting Fan,
  • Bing Liu,
  • Haoyan Yao,
  • Xinrui Chen,
  • Hang Yang,
  • Shangrui Guo,
  • Bo Wu,
  • Xiaozhen Li,
  • Xinyu Li,
  • Meng Xun,
  • Hongliang Wang

DOI
https://doi.org/10.1371/journal.ppat.1011967
Journal volume & issue
Vol. 20, no. 1
p. e1011967

Abstract

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Given the serious neurological complications and deaths associated with enterovirus 71 (EV71) infection, there is an urgent need to develop effective antivirals against this viral infection. In this study, we demonstrated that two Cathelicidin-derived peptides, LL-18 and FF-18 were more potent against EV71 infection than the parent peptide LL-37, which is the mature and processed form of Cathelicidin. These peptides could directly bind to the EV71 virus particles, but not to coxsackievirus, indicative of their high specificity. The binding of peptides with the virus surface occupied the viral canyon region in a way that could block virus-receptor interactions and inhibit viral uncoating. In addition, these peptide analogues could also relieve the deleterious effect of EV71 infection in vivo. Therefore, Cathelicidin-derived peptides might be excellent candidates for further development of antivirals to treat EV71 infection.