首页> 外文OA文献 >THE MAMMALIAN CELL-VIRUS RELATIONSHIP : VI. SUSTAINED INFECTION OF HELA CELLS BY COXSACKIE B3 VIRUS AND EFFECT ON SUPERINFECTION
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THE MAMMALIAN CELL-VIRUS RELATIONSHIP : VI. SUSTAINED INFECTION OF HELA CELLS BY COXSACKIE B3 VIRUS AND EFFECT ON SUPERINFECTION

机译:哺乳动物细胞与病毒的关系:VI。柯萨奇B3病毒持续感染HELA细胞及其对超感染的影响。

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摘要

Sustained infection of HeLa cells by Coxsackie B3 virus, dependent on presence of viral inhibitor in culture medium, was achieved. Persistent treatment of carrier cultures with anti-Coxsackie B3 hyperimmune monkey serum eventually eliminated virus from carrier cultures indicating that a lysogenic virus-cell relationship was not operative. Free virus was produced continuously by carrier cultures despite washing and neutralization with antiserum to eliminate free virus temporarily. In carrier cultures, about 1.5 to 1.9 plaque-forming units of virus per cell were cell-associated; approximately 6 per cent of this cell-associated virus was not neutralizable by antiserum. In growth medium containing anti-B3 antibody, cells from carrier cultures formed colonies as efficiently as cells from B3-cured cultures. Assays of carrier cultures for infectious centers indicated that less than 1 per cent of cells produced free infectious virus. The Coxsackie B3 virus-carrier state appeared to represent surface residence of B3 virus on the majority of carrier cells with restriction of productive infection to a small proportion of the population. Coxsackie B3 carrier HeLa cultures, unlike control cultures, were not destroyed by challenge with Coxsackie B1, B3, or B5 viruses. The B3 carrier state did not interfere with superinfection by herpes, vaccinia, and types 1 to 3 polioviruses. In contrast to parental or B3-cured lines, B3-carrier HeLa cultures superinfected with Coxsackie B1 virus produced no significant virus, and cultures superinfected with B5 viruses produced new virus to a limited extent only. Specific interference with Coxsackie virus superinfection by the B3-carrier state of HeLa cells was shown to be attributable to failure of attachment in the instance of Coxsackie B1 virus, and failure of penetration and/or eclipse in the instance of B5 virus. The interfering effect was circumvented successfully by superinfection of carrier cells with ribonucleic acid extracted from Coxsackie B1 and B5 viruses.
机译:柯萨奇B3病毒持续感染HeLa细胞,这取决于培养基中病毒抑制剂的存在。用抗Coxsackie B3超免疫猴子血清对载体培养物进行持久处理最终从载体培养物中消除了病毒,这表明溶源性病毒与细胞的关系不起作用。尽管用抗血清洗涤并中和以暂时消除游离病毒,但通过载体培养连续产生游离病毒。在载体培养中,每个细胞约有1.5至1.9个病毒斑块形成单位与细胞相关。该细胞相关病毒中约有6%无法被抗血清中和。在含有抗B3抗体的生长培养基中,来自载体培养物的细胞形成菌落的效率与来自B3固化培养物的细胞一样有效。对感染中心进行载体培养的分析表明,不到1%的细胞产生游离的感染病毒。柯萨奇B3病毒携带者的状态似乎代表B3病毒在大多数载体细胞上的表面驻留,而生产感染只限于一小部分人群。与对照培养不同,柯萨奇B3携带者的HeLa培养物并未受到柯萨奇B1,B3或B5病毒的攻击而破坏。 B3携带者状态不会干扰疱疹,牛痘和1-3型脊髓灰质炎病毒的过度感染。与亲本或B3治愈系不同,用Coxsackie B1病毒超级感染的B3载体HeLa培养物未产生明显的病毒,而用B5病毒超级感染的培养物仅在有限的程度上产生了新病毒。已证明,HeLa细胞的B3携带者状态对Coxsackie病毒的过度感染产生了特定的干扰,这归因于在Coxsackie B1病毒的情况下附着失败,在B5病毒的情况下的渗透和/或蚀失败。通过用从柯萨奇B1和B5病毒中提取的核糖核酸对感染的细胞进行超感染,成功地避免了干扰作用。

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