Live subgroup B respiratory syncytial virus vaccines that are attenuated, genetically stable, and immunogenic in rodents and nonhuman primates

被引:48
作者
Crowe, JE [1 ]
Bui, PT [1 ]
Firestone, CY [1 ]
Connors, M [1 ]
Elkins, WR [1 ]
Chanock, RM [1 ]
Murphy, BR [1 ]
机构
[1] NIAID,NIH,INFECT DIS LAB,RESP VIRUSES SECT,BETHESDA,MD 20892
来源
JOURNAL OF INFECTIOUS DISEASES | 1996年 / 173卷 / 04期
关键词
D O I
10.1093/infdis/173.4.829
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Optimal immunization of neonates against disease caused by respiratory syncytial virus (RSV) probably will require multiple doses of a vaccine containing viruses of both subgroups A and B, Live subgroup B RSV mutants were generated containing multiple attenuating mutations, ts (temperature-sensitive) and non-ts (host range), that were introduced by prolonged passage in cell culture or by chemical mutagenesis, The cold-passaged (cp)-52 mutant was restricted in replication compared to wild type virus in rodents and nonhuman primates, In addition, the attenuation phenotype of cp-52 was stable after prolonged replication in immunosuppressed rodents, One or two ts mutations were then introduced into the cp-52 mutant to generate additional candidate vaccine strains that were more attenuated in vivo than the cp-52 parental virus, Tests in humans are being done to determine if one or more of the RSV B-1 mutants exhibit a satisfactory balance between attenuation and immunogenicity.
引用
收藏
页码:829 / 839
页数:11
相关论文
共 31 条
[1]   MOLECULAR EPIDEMIOLOGY OF RESPIRATORY SYNCYTIAL VIRUS - RAPID IDENTIFICATION OF SUBGROUP-A LINEAGES [J].
CANE, PA ;
PRINGLE, CR .
JOURNAL OF VIROLOGICAL METHODS, 1992, 40 (03) :297-306
[2]  
CANE PA, 1994, J CLIN MICROBIOL, V32, P1
[3]  
CHANOCK RM, 1991, ANIMAL MODELS RESP S, P35
[4]   AN ANTIGENIC ANALYSIS OF RESPIRATORY SYNCYTIAL VIRUS ISOLATES BY A PLAQUE REDUCTION NEUTRALIZATION TEST [J].
COATES, HV ;
ALLING, DW ;
CHANOCK, RM .
AMERICAN JOURNAL OF EPIDEMIOLOGY, 1966, 83 (02) :299-&
[5]   SATISFACTORILY ATTENUATED AND PROTECTIVE MUTANTS DERIVED FROM A PARTIALLY ATTENUATED COLD-PASSAGED RESPIRATORY SYNCYTIAL VIRUS MUTANT BY INTRODUCTION OF ADDITIONAL ATTENUATING MUTATIONS DURING CHEMICAL MUTAGENESIS [J].
CROWE, JE ;
BUI, PT ;
LONDON, WT ;
DAVIS, AR ;
HUNG, PP ;
CHANOCK, RM ;
MURPHY, BR .
VACCINE, 1994, 12 (08) :691-699
[6]   COLD PASSAGED, TEMPERATURE-SENSITIVE MUTANTS OF HUMAN RESPIRATORY SYNCYTIAL VIRUS (RSV) ARE HIGHLY ATTENUATED, IMMUNOGENIC, AND PROTECTIVE IN SERONEGATIVE CHIMPANZEES, EVEN WHEN RSV ANTIBODIES ARE INFUSED SHORTLY BEFORE IMMUNIZATION [J].
CROWE, JE ;
BUI, PT ;
SIBER, GR ;
ELKINS, WR ;
CHANOCK, RM ;
MURPHY, BR .
VACCINE, 1995, 13 (09) :847-855
[7]   A COMPARISON IN CHIMPANZEES OF THE IMMUNOGENICITY AND EFFICACY OF LIVE ATTENUATED RESPIRATORY SYNCYTIAL VIRUS (RSV) TEMPERATURE-SENSITIVE MUTANT VACCINES AND VACCINIA VIRUS RECOMBINANTS THAT EXPRESS THE SURFACE GLYCOPROTEINS OF RSV [J].
CROWE, JE ;
COLLINS, PL ;
LONDON, WT ;
CHANOCK, RM ;
MURPHY, BR .
VACCINE, 1993, 11 (14) :1395-1404
[8]   A FURTHER ATTENUATED DERIVATIVE OF A COLD-PASSAGED TEMPERATURE-SENSITIVE MUTANT OF HUMAN RESPIRATORY SYNCYTIAL VIRUS RETAINS IMMUNOGENICITY AND PROTECTIVE EFFICACY AGAINST WILD-TYPE CHALLENGE IN SERONEGATIVE CHIMPANZEES [J].
CROWE, JE ;
BUI, PT ;
DAVIS, AR ;
CHANOCK, RM ;
MURPHY, BR .
VACCINE, 1994, 12 (09) :783-790
[9]  
Erwin J, 1992, CHIMPANZEE CONSERVAT, P65
[10]   COLD-PASSAGED HUMAN PARAINFLUENZA TYPE-3 VIRUSES CONTAIN TS AND NON-TS MUTATIONS LEADING TO ATTENUATION IN RHESUS-MONKEYS [J].
HALL, SL ;
STOKES, A ;
TIERNEY, EL ;
LONDON, WT ;
BELSHE, RB ;
NEWMAN, FC ;
MURPHY, BR .
VIRUS RESEARCH, 1992, 22 (03) :173-184
1234