Delayed treatment of Ebola virus infection with plant-derived monoclonal antibodies provides protection in rhesus macaques.

نویسندگان

  • Gene Garrard Olinger
  • James Pettitt
  • Do Kim
  • Cara Working
  • Ognian Bohorov
  • Barry Bratcher
  • Ernie Hiatt
  • Steven D Hume
  • Ashley K Johnson
  • Josh Morton
  • Michael Pauly
  • Kevin J Whaley
  • Calli M Lear
  • Julia E Biggins
  • Corinne Scully
  • Lisa Hensley
  • Larry Zeitlin
چکیده

Filovirus infections can cause a severe and often fatal disease in humans and nonhuman primates, including great apes. Here, three anti-Ebola virus mouse/human chimeric mAbs (c13C6, h-13F6, and c6D8) were produced in Chinese hamster ovary and in whole plant (Nicotiana benthamiana) cells. In pilot experiments testing a mixture of the three mAbs (MB-003), we found that MB-003 produced in both manufacturing systems protected rhesus macaques from lethal challenge when administered 1 h postinfection. In a pivotal follow-up experiment, we found significant protection (P < 0.05) when MB-003 treatment began 24 or 48 h postinfection (four of six survived vs. zero of two controls). In all experiments, surviving animals that received MB-003 experienced little to no viremia and had few, if any, of the clinical symptoms observed in the controls. The results represent successful postexposure in vivo efficacy by a mAb mixture and suggest that this immunoprotectant should be further pursued as a postexposure and potential therapeutic for Ebola virus exposure.

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عنوان ژورنال:
  • Proceedings of the National Academy of Sciences of the United States of America

دوره 109 44  شماره 

صفحات  -

تاریخ انتشار 2012