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细胞聚集增强胚胎癌细胞中MyoD介导的骨骼肌生成。

Cellular aggregation enhances MyoD-directed skeletal myogenesis in embryonal carcinoma cells.

作者信息

Skerjanc I S, Slack R S, McBurney M W

机构信息

Department of Medicine, University of Ottawa, Ontario, Canada.

出版信息

Mol Cell Biol. 1994 Dec;14(12):8451-9. doi: 10.1128/mcb.14.12.8451-8459.1994.

Abstract

When introduced into P19 embryonal carcinoma cells, recombinant genes encoding MyoD converted only a small percentage (< 3%) of the transfected cells into skeletal muscle. We isolated stably transfected cells that expressed the MyoD transcript. These P19[MyoD] cells continued to express markers characteristic of undifferentiated stem cells but also expressed myf-5 and the myotonic dystrophy kinase, transcripts normally present in myoblasts but absent from P19 cells. Aggregation of P19[MyoD] cells induced the expression of myogenin, desmin, and the retinoblastoma protein and resulted in the rapid and abundant development of skeletal muscle. Both the embryonic and the slow isoforms of myosin heavy chain were present in this muscle, indicating that it resembled skeletal muscle formed from primary myoblasts. Since aggregation of P19 cells normally results in inefficient differentiation and the development of only low levels of cardiac muscle but no skeletal muscle, we conclude that MyoD imposes the skeletal muscle program on P19 cells and that the differentiation of these cells requires inductive events provided by cell aggregation.

摘要

当将编码MyoD的重组基因导入P19胚胎癌细胞时,只有一小部分(<3%)转染细胞转变为骨骼肌细胞。我们分离出稳定转染且表达MyoD转录本的细胞。这些P19[MyoD]细胞继续表达未分化干细胞的特征性标志物,但也表达myf-5和强直性肌营养不良激酶,这些转录本通常存在于成肌细胞中而P19细胞中不存在。P19[MyoD]细胞聚集诱导生肌调节因子、结蛋白和视网膜母细胞瘤蛋白的表达,并导致骨骼肌快速大量发育。肌球蛋白重链的胚胎型和慢肌型异构体都存在于这种肌肉中,表明它类似于由原代成肌细胞形成的骨骼肌。由于P19细胞聚集通常导致分化效率低下,仅发育出低水平的心肌而无骨骼肌,我们得出结论,MyoD将骨骼肌程序强加于P19细胞,并且这些细胞的分化需要细胞聚集提供的诱导事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ffb6/359384/2986c287b3ae/molcellb00012-0785-a.jpg

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