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大鼠肝癌-小鼠成纤维细胞异核体和杂种细胞中白蛋白产生的消退、重新表达和激活过程的免疫荧光分析。

Immunofluorescence analysis of the time-course of extinction, reexpression, and activation of albumin production in rat hepatoma-mouse fibroblast heterokaryons and hybrids.

作者信息

Mével-Ninio M, Weiss M C

出版信息

J Cell Biol. 1981 Aug;90(2):339-50. doi: 10.1083/jcb.90.2.339.

Abstract

We have used a combination of a sensitive immunocytochemical stain for intracellular albumin, and Hoechst 33258 dye for identification of parental nuclei to investigate the time-course of extinction, reexpression, and activation of albumin production in fusion products of 1s (hyperdiploid) or 2s (hypertetradiploid) rat hepatoma cells with mouse fibroblasts (L cells or embryonic cells). In all combinations, the initial event is extinction of albumin production. Extinction occurs immediately after fusion when the mouse fibroblast is a normal embryonic (senescent?) cell. In the case of an L cell, rat albumin is synthesized and secreted during the first 12 h after fusion; no production of mouse albumin occurs. Thereafter, albumin production ceases. 8-12 d after fusion, young hybrid colonies are found to resume the synthesis of rat albumin (reexpression), and several days later the production of mouse albumin begins (activation). The patterns of reexpression and activation indicate (a) that chromosome loss is not necessary for either event to occur and (b) that the cells active in the synthesis of mouse albumin are a subpopulation of those cells already engaged in the production of rat albumin. We conclude that (a) extinction is mediated by diffusible factor(s) from the L-cell parent that act in the hepatoma nucleus to prevent the formation of new albumin messenger RNA; (b) reexpression and activation are gene dosage-dependent but extinction is not; and (c) previously active genes are more rapidly expressed than previously silent ones.

摘要

我们采用了一种针对细胞内白蛋白的灵敏免疫细胞化学染色法,以及用于鉴定亲代细胞核的Hoechst 33258染料,来研究1s(超二倍体)或2s(超四倍体)大鼠肝癌细胞与小鼠成纤维细胞(L细胞或胚胎细胞)融合产物中白蛋白产生的消失、重新表达和激活的时间进程。在所有组合中,最初的事件是白蛋白产生的消失。当小鼠成纤维细胞是正常胚胎(衰老?)细胞时,融合后立即发生消失。在L细胞的情况下,大鼠白蛋白在融合后的最初12小时内合成并分泌;未检测到小鼠白蛋白的产生。此后,白蛋白产生停止。融合后8 - 12天,发现年轻的杂交集落恢复大鼠白蛋白的合成(重新表达),几天后小鼠白蛋白的产生开始(激活)。重新表达和激活的模式表明:(a)这两个事件的发生都不需要染色体丢失;(b)活跃合成小鼠白蛋白的细胞是已经参与大鼠白蛋白产生的细胞中的一个亚群。我们得出结论:(a)消失是由来自L细胞亲代的可扩散因子介导的,这些因子作用于肝癌细胞核以阻止新的白蛋白信使核糖核酸的形成;(b)重新表达和激活是基因剂量依赖性的,但消失不是;(c)先前活跃的基因比先前沉默的基因表达得更快。

相似文献

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Albumin extinction without methylation of its gene.白蛋白消失而其基因未发生甲基化。
Proc Natl Acad Sci U S A. 1984 Mar;81(6):1738-41. doi: 10.1073/pnas.81.6.1738.

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