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发育过程中视黄酸调控的靶基因:综合基因组学分析

Retinoic Acid-Regulated Target Genes During Development: Integrative Genomics Analysis.

作者信息

Rochette-Egly Cecile

机构信息

Université de Strasbourg, IGBMC (Institut de Génétique et de Biologie Moléculaire et Cellulaire), INSERM, U964, CNRS, UMR7104, 1 rue Laurent Fries, BP 10142, 67404, Illkirch Cedex, France.

出版信息

Subcell Biochem. 2020;95:57-85. doi: 10.1007/978-3-030-42282-0_3.

Abstract

Retinoic acid (RA), a major natural active metabolite of vitamin A (VA) is well known to play critical roles in embryonic development. The effects of RA are mediated by nuclear receptors (RARs), which regulate the expression of gene batteries involved in cell growth and differentiation. Since the early 1990s several laboratories have focused on understanding how RA-regulated genes and RAR binding sites operate by studying the differentiation of embryonal carcinoma cells and embryonic stem cells. The development of hybridization-based microarray technology and high performance software analysis programs has allowed the characterization of thousands of RA-regulated genes. During the two last decades, publication of the genome sequence of various organisms has allowed advances in massive parallel sequencing and bioinformatics analysis of genome-wide data sets. These new generation sequencing (NGS) technologies have revolutionized the field by providing a global integrated picture of RA-regulated gene networks and the regulatory programs involved in cell fate decisions during embryonal carcinoma and embryonic stem cells differentiation. Now the challenge is to reconstruct the RA-regulated gene networks at the single cell level during the development of specialized embryonic tissues.

摘要

视黄酸(RA)是维生素A(VA)的主要天然活性代谢产物,众所周知,它在胚胎发育中起着关键作用。RA的作用是由核受体(RARs)介导的,核受体调节参与细胞生长和分化的基因群的表达。自20世纪90年代初以来,几个实验室一直致力于通过研究胚胎癌细胞和胚胎干细胞的分化来了解RA调节基因和RAR结合位点是如何运作的。基于杂交的微阵列技术和高性能软件分析程序的发展,使得数千个RA调节基因得以表征。在过去的二十年里,各种生物体基因组序列的公布推动了大规模平行测序和全基因组数据集的生物信息学分析的进展。这些新一代测序(NGS)技术通过提供RA调节基因网络以及胚胎癌细胞和胚胎干细胞分化过程中涉及细胞命运决定的调控程序的全局综合图景,彻底改变了该领域。现在的挑战是在特殊胚胎组织发育过程中,在单细胞水平上重建RA调节的基因网络。

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