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体细胞获得的亲嗜性病毒在裸鼠移植的NIH/3T3转化细胞系免疫原性中的作用。

Involvement of somatically acquired ecotropic viruses in the immunogenicity of nude-transplanted NIH/3T3 transformed cell lines.

作者信息

Sensi M, Bergomi M, Panceri P, Castelli C, Lupetti R, Traversari C, Carbone G, Parmiani G

机构信息

Division of Experimental Oncology D, Istituto Nazionale Tumori, Milan, Italy.

出版信息

J Immunol. 1992 Jul 1;149(1):277-83.

PMID:1318902
Abstract

Immunogenic tumor variants were previously derived after transplantation in vivo into nude mice of NIH/3T3-transformed cell lines. Nude-passaged cell lines were rejected by immunocompetent H-2q NIH mice, were recognized by specific CTL clones, and expressed new retroviral Ag. The aim of the present work was to investigate whether somatically acquired proviral sequences were present in the genome of nude-passaged cells and to test directly for a causative relationship between murine leukemia virus (MuLV) expression and immunogenicity. Southern blot analysis of PstI-digested DNA indicated that in contrast to the parental NIH/3T3 transformed cell lines (pT, T12N/5a, NS-1) all the nude-passaged immunogenic variants (pT-nude, T12N/5a-nude, NS-1-nude) contained newly acquired ecotropic-related proviruses. Immediately after in vitro establishment, these tumors displayed multiple integration sites as assessed by analysis of 3' proviral-cellular junctions. Long term in vitro culture of one of the cell lines (pT-nude) resulted in a cell line (pT-nude/vitro) that was clonal or oligo-clonal with respect to viral integration. Northern blot analysis established that the new proviruses were actively transcribed in all the immunogenic variants. To assess whether the somatically acquired ecotropic proviral sequences encode for target structures recognized by specific CTL, obtained after immunization of NIH mice with pT-nude, the parental cell line pT was transfected with plasmids containing the entire AKV MuLV genome, the cloned AKV gag or env genes. Screening of transfectants for their ability to stimulate the production of TNF by anti-pT-nude effectors indicated that cells transfected with the entire ecotropic virus or with MuLV-env gene products could be recognized by an NIH anti-pT-nude CTL line and NIH anti-pT-nude Kq-restricted CTL clones as well as the immunizing target pT-nude.

摘要

免疫原性肿瘤变体先前是通过将NIH/3T3转化细胞系体内移植到裸鼠中获得的。经裸鼠传代的细胞系被具有免疫活性的H-2q NIH小鼠排斥,能被特异性CTL克隆识别,并表达新的逆转录病毒抗原。本研究的目的是调查经裸鼠传代的细胞基因组中是否存在体细胞获得的原病毒序列,并直接测试鼠白血病病毒(MuLV)表达与免疫原性之间的因果关系。对经PstI消化的DNA进行Southern印迹分析表明,与亲本NIH/3T3转化细胞系(pT、T12N/5a、NS-1)不同,所有经裸鼠传代的免疫原性变体(pT-裸鼠、T12N/5a-裸鼠、NS-1-裸鼠)都含有新获得的嗜亲性相关原病毒。在体外建立后,通过分析3'原病毒-细胞连接处评估,这些肿瘤显示出多个整合位点。其中一个细胞系(pT-裸鼠)的长期体外培养产生了一个细胞系(pT-裸鼠/体外),该细胞系在病毒整合方面是克隆性或寡克隆性的。Northern印迹分析确定新的原病毒在所有免疫原性变体中都有活跃转录。为了评估体细胞获得的嗜亲性原病毒序列是否编码NIH小鼠用pT-裸鼠免疫后获得的特异性CTL识别的靶结构,将亲本细胞系pT用含有整个AKV MuLV基因组、克隆的AKV gag或env基因的质粒转染。筛选转染体刺激抗pT-裸鼠效应细胞产生TNF的能力表明,用整个嗜亲性病毒或MuLV-env基因产物转染的细胞可被NIH抗pT-裸鼠CTL系和NIH抗pT-裸鼠Kq限制性CTL克隆以及免疫靶标pT-裸鼠识别。

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