| Literature DB >> 16698998 |
Masayuki Saijo1, Yasushi Ami, Yuriko Suzaki, Noriyo Nagata, Naoko Iwata, Hideki Hasegawa, Momoko Ogata, Shuetsu Fukushi, Tetsuya Mizutani, Tetsutaro Sata, Takeshi Kurata, Ichiro Kurane, Shigeru Morikawa.
Abstract
The potential threat of smallpox as a bioweapon has led to the production and stockpiling of smallpox vaccine in some countries. Human monkeypox, a rare but important viral zoonosis endemic to central and western Africa, has recently emerged in the United States. Thus, even though smallpox has been eradicated, a vaccinia virus vaccine that can induce protective immunity against smallpox and monkeypox is still invaluable. The ability of the highly attenuated vaccinia virus vaccine strain LC16m8, with a mutation in the important immunogenic membrane protein B5R, to induce protective immunity against monkeypox in nonhuman primates was evaluated in comparison with the parental Lister strain. Monkeys were immunized with LC16m8 or Lister and then infected intranasally or subcutaneously with monkeypox virus strain Liberia or Zr-599, respectively. Immunized monkeys showed no symptoms of monkeypox in the intranasal-inoculation model, while nonimmunized controls showed typical symptoms. In the subcutaneous-inoculation model, monkeys immunized with LC16m8 showed no symptoms of monkeypox except for a mild ulcer at the site of monkeypox virus inoculation, and those immunized with Lister showed no symptoms of monkeypox, while nonimmunized controls showed lethal and typical symptoms. These results indicate that LC16m8 prevents lethal monkeypox in monkeys, and they suggest that LC16m8 may induce protective immunity against smallpox.Entities:
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Year: 2006 PMID: 16698998 PMCID: PMC1472157 DOI: 10.1128/JVI.02642-05
Source DB: PubMed Journal: J Virol ISSN: 0022-538X Impact factor: 5.103