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对两种小鼠胚胎癌细胞系及一系列分化衍生物中Fv-1限制作用的分析。

Analysis of Fv-1 restriction in two murine embryonal carcinoma cell lines and a series of differentiated derivatives.

作者信息

Heitman C K, Innes C L, Jetten A M, Boone L R

机构信息

Cellular and Genetic Toxicology Branch, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709.

出版信息

J Gen Virol. 1991 Mar;72 ( Pt 3):609-16. doi: 10.1099/0022-1317-72-3-609.

Abstract

We have used antibiotic-resistant retrovirus vectors rescued by Fv-1-sensitive murine leukaemia viruses (MuLV) to examine the Fv-1 phenotype of two undifferentiated embryonal carcinoma (EC) cell lines derived from teratocarcinomas of mouse strain 129. In addition, a set of EC cell-derived differentiated cell lines was analysed. Restriction of both B-tropic and endogenous N-tropic virus is characteristic of the Nr-type restriction reported in mouse strain 129. However, results indicate that Fv-1 restriction is not expressed in the PCC4.aza1R EC cell line. In contrast, the F9 EC cell line showed a strong restriction of the B-tropic pseudotyped vector but failed to restrict endogenous N-tropic pseudotypes. The Fv-1 gene thus seems to be differentially expressed in two EC cell lines derived from the same mouse strain. Furthermore, the selective restriction of B-tropic but not endogenous N-tropic MuLV in F9 cells suggests that these activities function independently of each other. Analysis of PCC4.aza1R-derived differentiated cell lines revealed that three fibroblast cell lines derived by retinoic acid-induced differentiation were also phenotypically silent for Fv-1. However, a pre-adipocyte line established following simultaneous exposure to retinoic acid and 5-azacytidine showed strong restriction of both B-tropic and endogenous N-tropic MuLV. Although additional data suggest that there is no correlation between the differentiated pre-adipocyte phenotype and Fv-1 expression, our results nonetheless show that Nr restriction can be observed in some derivatives of PCC4.aza1R cells, presumably by activating expression of the Fv-1 gene.

摘要

我们使用了由Fv-1敏感型鼠白血病病毒(MuLV)拯救的抗抗生素逆转录病毒载体,来检测源自129品系小鼠畸胎瘤的两种未分化胚胎癌(EC)细胞系的Fv-1表型。此外,还分析了一组源自EC细胞的分化细胞系。对B嗜性和内源性N嗜性病毒的限制是129品系小鼠中报道的Nr型限制的特征。然而,结果表明Fv-1限制在PCC4.aza1R EC细胞系中未表达。相反,F9 EC细胞系对B嗜性假型载体表现出强烈的限制,但未能限制内源性N嗜性假型。因此,Fv-1基因似乎在源自同一品系小鼠的两种EC细胞系中存在差异表达。此外,F9细胞中对B嗜性而非内源性N嗜性MuLV的选择性限制表明,这些活性彼此独立发挥作用。对源自PCC4.aza1R的分化细胞系的分析表明,由视黄酸诱导分化产生的三种成纤维细胞系在Fv-1表型上也呈沉默状态。然而,在同时暴露于视黄酸和5-氮杂胞苷后建立的前脂肪细胞系对B嗜性和内源性N嗜性MuLV均表现出强烈的限制。尽管更多数据表明分化的前脂肪细胞表型与Fv-1表达之间没有相关性,但我们的结果仍然表明,在PCC4.aza1R细胞的一些衍生物中可以观察到Nr限制,可能是通过激活Fv-1基因的表达实现的。

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