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对胚胎干细胞和体干细胞中的基因组进行编程。

Programming the genome in embryonic and somatic stem cells.

作者信息

Collas Philippe, Noer Agate, Timoskainen Sanna

机构信息

Institute of Basic Medical Sciences, Department of Biochemistry, Faculty of Medicine, University of Oslo, 0317 Oslo, Norway.

出版信息

J Cell Mol Med. 2007 Jul-Aug;11(4):602-20. doi: 10.1111/j.1582-4934.2007.00079.x.

Abstract

In opposition to terminally differentiated cells, stem cells can self-renew and give rise to multiple cell types. Embryonic stem cells retain the ability of the inner cell mass of blastocysts to differentiate into all cell types of the body and have acquired in culture unlimited self-renewal capacity. Somatic stem cells are found in many adult tissues, have an extensive but finite lifespan and can differentiate into a more restricted array of cell types. A growing body of evidence indicates that multi-lineage differentiation ability of stem cells can be defined by the potential for expression of lineage-specification genes. Gene expression, or as emphasized here, potential for gene expression, is largely controlled by epigenetic modifications of DNA and chromatin on genomic regulatory and coding regions. These modifications modulate chromatin organization not only on specific genes but also at the level of the whole nucleus; they can also affect timing of DNA replication. This review highlights how mechanisms by which genes are poised for transcription in undifferentiated stem cells are being uncovered through primarily the mapping of DNA methylation, histone modifications and transcription factor binding throughout the genome. The combinatorial association of epigenetic marks on developmentally regulated and lineage-specifying genes in undifferentiated cells seems to define a pluripotent state.

摘要

与终末分化细胞不同,干细胞能够自我更新并产生多种细胞类型。胚胎干细胞保留了囊胚内细胞团分化为身体所有细胞类型的能力,并在培养中获得了无限的自我更新能力。成体干细胞存在于许多成体组织中,具有广泛但有限的寿命,并且能够分化为一系列更为受限的细胞类型。越来越多的证据表明,干细胞的多谱系分化能力可由谱系特异性基因的表达潜力来定义。基因表达,或者如本文所强调的基因表达潜力,在很大程度上受基因组调控和编码区域上DNA和染色质的表观遗传修饰控制。这些修饰不仅调节特定基因上的染色质组织,还在整个细胞核水平上进行调节;它们还可以影响DNA复制的时间。本综述重点介绍了通过对全基因组DNA甲基化、组蛋白修饰和转录因子结合进行图谱绘制,如何揭示未分化干细胞中基因准备转录的机制。未分化细胞中发育调控基因和谱系特异性基因上表观遗传标记的组合关联似乎定义了一种多能状态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/975b/3823245/a4a8a69c45d7/jcmm0011-0602-f1.jpg

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