Replication-deficient rabies virus-based vaccines are safe and immunogenic in mice and nonhuman primates.

نویسندگان

  • Jonathan Cenna
  • Meredith Hunter
  • Gene S Tan
  • Amy B Papaneri
  • Erin P Ribka
  • Matthias J Schnell
  • Preston A Marx
  • James P McGettigan
چکیده

Although current postexposure prophylaxis rabies virus (RV) vaccines are effective, approximately 40,000-70,000 rabies-related deaths are reported annually worldwide. The development of effective formulations requiring only 1-2 applications would significantly reduce mortality. We assessed in mice and nonhuman primates the efficacy of replication-deficient RV vaccine vectors that lack either the matrix (M) or phosphoprotein (P) gene. A single dose of M gene-deficient RV induced a more rapid and efficient anti-RV response than did P gene-deficient RV immunization. Furthermore, the M gene-deleted RV vaccine induced 4-fold higher virus-neutralizing antibody (VNA) levels in rhesus macaques than did a commercial vaccine within 10 days after inoculation, and at 180 days after immunization rhesus macaques remained healthy and had higher-avidity antibodies, higher VNA titers, and a more potent antibody response typical of a type 1 T helper response than did animals immunized with a commercial vaccine. The data presented in this article suggest that the M gene-deleted RV vaccine is safe and effective and holds the potential of replacing current pre- and postexposure RV vaccines.

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عنوان ژورنال:
  • The Journal of infectious diseases

دوره 200 8  شماره 

صفحات  -

تاریخ انتشار 2009