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组织型纤溶酶原激活剂诱导人横纹肌肉瘤细胞分化:生肌调节因子的表达

TPA-induced differentiation of human rhabdomyosarcoma cells: expression of the myogenic regulatory factors.

作者信息

Bouché M, Senni M I, Grossi A M, Zappelli F, Polimeni M, Arnold H H, Cossu G, Molinaro M

机构信息

Istituto di Istologia ed Embriologia Generale, Fac. di Medicina, Università di Roma La Sapienza, Italy.

出版信息

Exp Cell Res. 1993 Sep;208(1):209-17. doi: 10.1006/excr.1993.1239.

Abstract

RD cells (a cell line derived from a human rhabdomyosarcoma) undergo a very limited myogenic differentiation despite the fact that they express several myogenic determination genes. Since we have previously shown (Aguanno et al., Cancer Res. 50, 3377, 1990) that the tumor promoter 12-O-tetradecanoylphorbol-13-acetate (TPA) induces myogenic differentiation in these cells, in this paper we investigate the mechanism by which TPA interferes with the expression and/or function of the myogenic determination genes. Northern blot analysis revealed that RD cells express the myf3 (the human analog of MyoD) and myf4 (the human analog of myogenin) transcripts, but not myf5 or myf6 transcripts. The myf3 and the myf4 gene products are correctly translated and accumulated in the nuclei as shown by immunofluorescence analysis. The tumor promoter (TPA) does not modify the pattern of expression of the myf factors while it induces the accumulation of muscle-specific transcripts, such as alpha-actin and fast myosin light chain 1, and their corresponding proteins. On the other hand, within 1 day of treatment, TPA inhibits the expression of the Id gene, which is a negative regulator of MyoD activity. However, while the TPA-induced inhibition of Id message accumulation correlates with differentiation, cell confluence also causes a reduction in Id message accumulation, without inducing differentiation. Under our experimental conditions, overexpression of any of the myf cDNAs in RD cells does induce spontaneous differentiation but enhances the effect of TPA treatment independently from the level of the expressed message. These data suggest that differentiation of RD cells is likely to depend upon the activity of complexes containing the various members of the MyoD family, which can be regulated by proteins affecting MyoD dimerization such as Id, but also by other mechanisms induced by TPA, such as phosphorylation.

摘要

RD细胞(一种源自人横纹肌肉瘤的细胞系)尽管表达多种生肌决定基因,但经历非常有限的生肌分化。由于我们之前已经表明(阿瓜诺等人,《癌症研究》50卷,3377页,1990年)肿瘤启动子12 - O - 十四酰佛波醇 - 13 - 乙酸酯(TPA)可诱导这些细胞的生肌分化,在本文中我们研究TPA干扰生肌决定基因表达和/或功能的机制。Northern印迹分析显示RD细胞表达myf3(MyoD的人类类似物)和myf4(生肌调节因子的人类类似物)转录本,但不表达myf5或myf6转录本。免疫荧光分析表明,myf3和myf4基因产物被正确翻译并在细胞核中积累。肿瘤启动子(TPA)在诱导肌肉特异性转录本如α-肌动蛋白和快肌球蛋白轻链1及其相应蛋白质积累时,并不改变myf因子的表达模式。另一方面,在处理1天内,TPA抑制Id基因的表达,Id基因是MyoD活性的负调节因子。然而,虽然TPA诱导的Id信息积累抑制与分化相关,但细胞汇合也会导致Id信息积累减少,而不诱导分化。在我们的实验条件下,RD细胞中任何一种myf cDNA的过表达确实会诱导自发分化,但独立于表达信息的水平增强TPA处理的效果。这些数据表明,RD细胞的分化可能取决于包含MyoD家族各成员的复合物的活性,其可由影响MyoD二聚化的蛋白质(如Id)调节,也可由TPA诱导的其他机制(如磷酸化)调节。

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