Mechanistic study of broadly neutralizing human monoclonal antibodies against dengue virus that target the fusion loop.

نویسندگان

  • Joshua M Costin
  • Elena Zaitseva
  • Kristen M Kahle
  • Cindo O Nicholson
  • Dawne K Rowe
  • Amanda S Graham
  • Lindsey E Bazzone
  • Greg Hogancamp
  • Marielys Figueroa Sierra
  • Rachel H Fong
  • Sung-Tae Yang
  • Li Lin
  • James E Robinson
  • Benjamin J Doranz
  • Leonid V Chernomordik
  • Scott F Michael
  • John S Schieffelin
  • Sharon Isern
چکیده

There are no available vaccines for dengue, the most important mosquito-transmitted viral disease. Mechanistic studies with anti-dengue virus (DENV) human monoclonal antibodies (hMAbs) provide a rational approach to identify and characterize neutralizing epitopes on DENV structural proteins that can serve to inform vaccine strategies. Here, we report a class of hMAbs that is likely to be an important determinant in the human humoral response to DENV infection. In this study, we identified and characterized three broadly neutralizing anti-DENV hMAbs: 4.8A, D11C, and 1.6D. These antibodies were isolated from three different convalescent patients with distinct histories of DENV infection yet demonstrated remarkable similarities. All three hMAbs recognized the E glycoprotein with high affinity, neutralized all four serotypes of DENV, and mediated antibody-dependent enhancement of infection in Fc receptor-bearing cells at subneutralizing concentrations. The neutralization activities of these hMAbs correlated with a strong inhibition of virus-liposome and intracellular fusion, not virus-cell binding. We mapped epitopes of these antibodies to the highly conserved fusion loop region of E domain II. Mutations at fusion loop residues W101, L107, and/or G109 significantly reduced the binding of the hMAbs to E protein. The results show that hMAbs directed against the highly conserved E protein fusion loop block viral entry downstream of virus-cell binding by inhibiting E protein-mediated fusion. Characterization of hMAbs targeting this region may provide new insights into DENV vaccine and therapeutic strategies.

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عنوان ژورنال:
  • Journal of virology

دوره 87 1  شماره 

صفحات  -

تاریخ انتشار 2013