Efficient inhibition of human papillomavirus infection by l2 minor capsid-derived lipopeptide

Huan Yan, Suan Sin Foo, Weiqiang Chen, Ji Seung Yoo, Woo Jin Shin, Christine Wu, Jae U. Jung

Research output: Contribution to journalArticlepeer-review

13 Scopus citations

Abstract

The amino (N)-terminal region of human papillomavirus (HPV) minor capsid protein (L2) is a highly conserved region which is essential for establishing viral infection. Despite its importance in viral infectivity, the role of the HPV N-terminal domain has yet to be fully characterized. Using fine mapping analysis, we identified a 36-amino-acid (aa) peptide sequence of the L2 N terminus, termed L2N, that is critical for HPV infection. Ectopic expression of L2N with the transmembrane sequence on the target cell surface conferred resistance to HPV infection. Additionally, L2N peptide with chemical or enzymatic lipidation at the carboxyl (C) terminus efficiently abrogated HPV infection in target cells. Among the synthetic L2N lipopeptides, a stearoylated lipopeptide spanning aa 13 to 46 (13-46st) exhibited the most potent anti-HPV activity, with a half-maximal inhibitory concentration (IC50) of ~200 pM. Furthermore, we demonstrated that the 13-46st lipopeptide inhibited HPV entry by blocking trans-Golgi network retrograde trafficking of virion particles, leading to rapid degradation. Fundamentally, the inhibitory effect of L2N lipopeptides appeared to be evolutionarily conserved, as they showed cross-type inhibition among various papillomaviruses. In conclusion, our findings provide new insights into the critical role of the L2N sequence in the HPV entry mechanism and identify the therapeutic potential of L2N lipopeptide as an effective anti-HPV agent.

Original languageEnglish
Article numbere01834-19
JournalmBio
Volume10
Issue number4
DOIs
StatePublished - 2019

Keywords

  • Entry inhibitor
  • Human papillomavirus
  • L2N lipopeptide
  • Minor capsid protein

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