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小鼠红白血病细胞中c-myc的表达失调会阻止细胞分化。

Deregulated expression of c-myc by murine erythroleukaemia cells prevents differentiation.

作者信息

Prochownik E V, Kukowska J

出版信息

Nature. 1986;322(6082):848-50. doi: 10.1038/322848a0.

Abstract

Friend murine erythroleukaemia (F-MEL) cells are a permanent line of primitive erythroid precursors originally derived from the spleens of mice infected with the Friend strain of murine leukaemia virus. F-MEL cells differentiate in vitro in response to various chemical inducers. Concomitantly with induction, a biphasic regulation of c-myc oncogene transcripts is observed. Within one hour of the addition of dimethyl sulphoxide (DMSO) or hypoxanthine (Hyp), the levels of c-myc transcripts fall dramatically and remain virtually undetectable for the next few hours. Between 8 and 24 hours after induction, c-myc transcripts return to pre-induction levels and then decline again between 3 and 5 days as most of the cells undergo terminal differentiation. To explore the potential relationship between c-myc expression and F-MEL terminal differentiation, we have investigated here whether reversing the early fluctuations in c-myc transcript levels affects the ability of F-MEL cells to differentiate. We therefore constructed an amplifiable plasmid vector containing a full-length mouse c-myc complementary DNA and introduced it stably into recipient F-MEL cells. The exogenous c-myc sequences are transcribed in F-MEL cells and the transcript levels do not change significantly in response to inducing agents. The net result is continued c-myc expression following DMSO or Hyp induction and a complete or partial inhibition of F-MEL differentiation.

摘要

弗瑞德小鼠红白血病(F-MEL)细胞是一种永久性的原始红细胞前体细胞系,最初来源于感染了弗瑞德株小鼠白血病病毒的小鼠脾脏。F-MEL细胞在体外对各种化学诱导剂有反应而发生分化。在诱导的同时,观察到c-myc癌基因转录本的双相调节。在加入二甲基亚砜(DMSO)或次黄嘌呤(Hyp)后的一小时内,c-myc转录本水平急剧下降,在接下来的几个小时内几乎检测不到。诱导后8至24小时,c-myc转录本恢复到诱导前水平,然后在3至5天内再次下降,因为大多数细胞经历终末分化。为了探索c-myc表达与F-MEL终末分化之间的潜在关系,我们在此研究了逆转c-myc转录本水平的早期波动是否会影响F-MEL细胞的分化能力。因此,我们构建了一个包含全长小鼠c-myc互补DNA的可扩增质粒载体,并将其稳定地导入受体F-MEL细胞中。外源性c-myc序列在F-MEL细胞中被转录,并且转录本水平对诱导剂没有明显变化。最终结果是在DMSO或Hyp诱导后c-myc持续表达,以及F-MEL分化的完全或部分抑制。

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