PLoS ONE (Jan 2012)

A human PrM antibody that recognizes a novel cryptic epitope on dengue E glycoprotein.

  • Annie Hoi Yi Chan,
  • Hwee Cheng Tan,
  • Angelia Yee Chow,
  • Angeline Pei Chiew Lim,
  • Shee Mei Lok,
  • Nicole J Moreland,
  • Subhash G Vasudevan,
  • Paul A MacAry,
  • Eng Eong Ooi,
  • Brendon J Hanson

DOI
https://doi.org/10.1371/journal.pone.0033451
Journal volume & issue
Vol. 7, no. 4
p. e33451

Abstract

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Dengue virus (DENV) is a major mosquito-borne pathogen infecting up to 100 million people each year; so far no effective treatment or vaccines are available. Recently, highly cross-reactive and infection-enhancing pre-membrane (prM)-specific antibodies were found to dominate the anti-DENV immune response in humans, raising concern over vaccine candidates that contain native dengue prM sequences. In this study, we have isolated a broadly cross-reactive prM-specific antibody, D29, during a screen with a non-immunized human Fab-phage library against the four serotypes of DENV. The antibody is capable of restoring the infectivity of virtually non-infectious immature DENV (imDENV) in FcγR-bearing K562 cells. Remarkably, D29 also cross-reacted with a cryptic epitope on the envelope (E) protein located to the DI/DII junction as evidenced by site-directed mutagenesis. This cryptic epitope, while inaccessible to antibody binding in a native virus particle, may become exposed if E is not properly folded. These findings suggest that generation of anti-prM antibodies that enhance DENV infection may not be completely avoided even with immunization strategies employing E protein alone or subunits of E proteins.