Isolation And Characterization Of A Highly Attenuated Respiratory Syncytial Virus (Rsv) Vaccine Candidate By Mutagenesis Of The Incompletely Attenuated Rsv A2 Ts-1 Ng-1 Mutant Virus

VACCINE(1995)

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摘要
Ts-1, a temperature sensitive (ts) mutant of RSV was previously derived from RSV A2 virus by mutagenesis with 5-fluorouracil (5-FU). Ts-1 was attenuated for adult volunteers and seropositive children but retained a low level of virulence in seronegative infant vaccinees as indicated by the occurrence of upper respiratory tract disease. Ts-1 NG-1, a more defective derivative of ts-1, has produced by mutagenesis of ts-1 with nitrosoguanidine. However, ts-1 NG-1 still retained a low level of virulence for the upper respiratory tract and showed some genetic instability in chimpanzees. With renewed interest in the goal of developing a live, attenuated RSV vaccine, we have now attempted to further attenuate ts-1 NG-1 by mutagenesis with 5-FU and 5-azacytidine. Four mutants that are phenotypically different from the ts-1 NG-1 parental virus were identified. Each of the four mutants was more restricted in replication in BALB/c mice compared with the ts-1 NG-1 parental virus. One of the ts-1 NG-1 derivatives, termed A-20-4, which showed the lowest (35 degrees C) in vitro shutoff temperature and which was also completely restricted in replication in BALB/c mice, was selected for further evaluation in seronegative chimpanzees, A-20-4 did not cause rhinorrhea in chimpanzees but induced detectable titers of serum RSV neutralizing antibodies in 2 of 4 chimpanzees. Apparent complete protection to subsequent challenge with, wild-type RSV was observed in each of the four chimpanzees previously immunized with A-20-4, The ts-1 NG-1 A-20-4 mutant thus represents a promising live attenuated RSV vaccine candidate.
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关键词
RESPIRATORY SYNCYTIAL VIRUS, LIVE VACCINE, VIRUS ATTENUATION
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