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马疱疹病毒引起的致癌转化。II. 富含缺陷干扰颗粒的1型马疱疹病毒制剂对仓鼠胚胎细胞持续感染的共同建立及致癌转化

Oncogenic transformation by by equine herpesviruses. II. Coestablishment of persistent infection and oncogenic transformation of hamster embryo cells by equine herpesvirus type 1 preparations enriched for defective interfering particles.

作者信息

Robinson R A, Vance R B, O'Callaghan D J

出版信息

J Virol. 1980 Oct;36(1):204-19. doi: 10.1128/JVI.36.1.204-219.1980.

Abstract

Infection of permissive hamster embryo cells with virus preparations enriched for defective interfering (DI) particles of equine herpesvirus type 1 (EHV-1) resulted in persistent infection and oncogenic transformation. Six cell lines, designated DI-5 to -10, exhibited biological properties (immortality, increased saturation density, growth in soft agar, etc.) inherent to transformed cells, but 2 to 18% of the total cells in these cell lines were shown to release virus as judged by electron microscope studies and infectious center assays. The released virus was shown to be standard EHV-1 and not to contain DI particles as determined by density measurements of the viral DNA in the analytical ultracentrifuge and by interference assays using the released virus. Tumorigenicity studies revealed that inoculation of these persistently infected cells into newborn LSH inbred hamsters resulted in a lethal, fulminating hepatitis, whereas inoculation into older immunocompetent hamsters (+4 weeks) led to the development of metastatic fibrous sarcomas. Tumor cell lines (DI-5T to -10T) established from these sarcomas were shown to be transplantable and virus nonproducers. Hybridization analyses of cellular DNAs from DI transformed and tumor cell lines using 32P-labeled genomic EHV-1 DNA as probes indicated that the whole virus genome was detectable in multiple copies (23 to 45) in the transformed cells and that DNA sequences representing only 43.5 to 56.6% of the virus genome were present in amounts of 2 to 4 copies per cell in the DI tumor cells. Expression of these viral DNA sequences as demonstrated by the detection of virus-neutralizing antibodies, 50% neutralizing dose titers ranging from 1:50 to 1:1,000, in the sera of animals inoculated with either the virus-producing transformed cells or the virus-nonproducing tumor cells. Further, EHV-1-specific proteins were detected in the membrane and the perinuclear region of bothDI transformed and tumor cells by indirect immunofluorescent assays using antisera against EHV-1 structural antigens, EHV-1 nonstructural antigens, or preparations of EHV-1 DI particles. The roles of DI particles in mediating persistent infection and cellular transformation are discussed.

摘要

用富含1型马疱疹病毒(EHV-1)缺陷干扰(DI)颗粒的病毒制剂感染允许性仓鼠胚胎细胞,导致持续感染和致癌转化。六个细胞系,命名为DI-5至-10,表现出转化细胞固有的生物学特性(永生性、饱和密度增加、在软琼脂中生长等),但通过电子显微镜研究和感染中心测定,这些细胞系中2%至18%的总细胞被证明能释放病毒。通过分析超速离心机中病毒DNA的密度测量以及使用释放的病毒进行干扰测定,表明释放的病毒是标准的EHV-1,不含有DI颗粒。致瘤性研究表明,将这些持续感染的细胞接种到新生LSH近交系仓鼠中会导致致命的暴发性肝炎,而接种到年龄较大的免疫活性仓鼠(+4周)中则会导致转移性纤维肉瘤的发生。从这些肉瘤建立的肿瘤细胞系(DI-5T至-10T)被证明是可移植的且不产生病毒。使用32P标记的EHV-1基因组DNA作为探针,对DI转化细胞系和肿瘤细胞系的细胞DNA进行杂交分析,结果表明在转化细胞中可检测到多拷贝(23至45)的完整病毒基因组,而在DI肿瘤细胞中,代表病毒基因组仅43.5%至56.6%的DNA序列以每个细胞2至4拷贝的量存在。在用产生病毒的转化细胞或不产生病毒的肿瘤细胞接种的动物血清中,通过检测病毒中和抗体证明了这些病毒DNA序列的表达,50%中和剂量效价范围为1:50至1:1000。此外,通过使用针对EHV-1结构抗原、EHV-1非结构抗原或EHV-1 DI颗粒制剂的抗血清进行间接免疫荧光测定,在DI转化细胞和肿瘤细胞的膜和核周区域检测到EHV-1特异性蛋白。讨论了DI颗粒在介导持续感染和细胞转化中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b70/353631/f1a5f5228524/jvirol00178-0218-a.jpg

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