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通过化学诱变过程中引入额外的减毒突变,从部分减毒的冷传代呼吸道合胞病毒突变体衍生而来的充分减毒且具有保护性的突变体。

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.

作者信息

Crowe J E, Bui P T, London W T, Davis A R, Hung P P, Chanock R M, Murphy B R

机构信息

Respiratory Viruses Section, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892.

出版信息

Vaccine. 1994 Jun;12(8):691-9. doi: 10.1016/0264-410x(94)90218-6.

Abstract

A cold-passaged RSV mutant, designated cp-RSV, which acquired host range mutations during 52 passages at low temperature in bovine tissue culture, was completely attenuated for seropositive adults and children but retained the capacity to cause upper respiratory disease in seronegative infants. We sought to introduce additional attenuating mutations, such as temperature-sensitive (ts) and small-plaque (sp) mutations, into the cp-RSV mutant, which is a ts+ virus, in order to generate a mutant which would be satisfactorily attenuated in seronegative infants and young children. Nine mutants of cp-RSV, which had acquired either the ts or small-plaque sp phenotype, were generated by chemical mutagenesis with 5-fluorouracil. The two ts mutants with the lowest in vitro shut-off temperature, namely the cpts-248 (38 degrees C) and cpts-530 (39 degrees C) mutants, were the most restricted of the nine cp-RSV mutant progeny tested for efficiency of replication in Balb/c mice. In seronegative chimpanzees, the cpts-248 mutant replicated fourfold less efficiently in the nasopharynx and caused significantly less rhinorrhoea than its cp-RSV parent. The cpts-248 mutant virus, like its cp-RSV parent, was 1000-fold restricted in replication in the trachea compared with wild-type RSV. Previously, another candidate RSV live attenuated vaccine strain, a mutant designated ts-1, exhibited some instability of its ts phenotype following replication in susceptible humans or chimpanzees. Hence, we sought cp-RSV ts progeny that exhibited a greater degree of stability of the ts phenotype than the prototype ts-1 mutant.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

一种冷传代呼吸道合胞病毒(RSV)突变体,命名为cp-RSV,它在牛组织培养中于低温下传代52次期间获得了宿主范围突变,对血清阳性的成人和儿童完全减毒,但仍保留在血清阴性婴儿中引起上呼吸道疾病的能力。我们试图将额外的减毒突变,如温度敏感(ts)和小蚀斑(sp)突变,引入cp-RSV突变体(这是一种ts+病毒),以产生一种在血清阴性婴儿和幼儿中能充分减毒的突变体。通过用5-氟尿嘧啶进行化学诱变,产生了9种获得ts或小蚀斑sp表型的cp-RSV突变体。在测试的9种cp-RSV突变体子代中,体外关闭温度最低的两个ts突变体,即cpts-248(38℃)和cpts-530(39℃)突变体,在Balb/c小鼠中复制效率的限制最大。在血清阴性的黑猩猩中,cpts-248突变体在鼻咽部的复制效率比其cp-RSV亲本低四倍,且引起的鼻漏明显更少。与野生型RSV相比,cpts-248突变体病毒与其cp-RSV亲本一样,在气管中的复制受到1000倍的限制。此前,另一种候选的RSV减毒活疫苗株,即命名为ts-1的突变体,在易感人类或黑猩猩中复制后,其ts表型表现出一些不稳定性。因此,我们寻找比原型ts-1突变体表现出更高程度ts表型稳定性的cp-RSV ts子代。(摘要截短于250字)

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