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Genomic analysis reveals distinct mechanisms and functional classes of SOX10-regulated genes in melanocytes

机译:基因组分析揭示黑素细胞中SOX10调控基因的不同机制和功能类别

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摘要

SOX10 is required for melanocyte development and maintenance, and has been linked to melanoma initiation and progression. However, the molecular mechanisms by which SOX10 guides the appropriate gene expression programs necessary to promote the melanocyte lineage are not fully understood. Here we employ genetic and epigenomic analysis approaches to uncover novel genomic targets and previously unappreciated molecular roles of SOX10 in melanocytes. Through global analysis of SOX10-binding sites and epigenetic characteristics of chromatin states, we uncover an extensive catalog of SOX10 targets genome-wide. Our findings reveal that SOX10 predominantly engages 'open' chromatin regions and binds to distal regulatory elements, including novel and previously known melanocyte enhancers. Integrated chromatin occupancy and transcriptome analysis suggest a role for SOX10 in both transcriptional activation and repression to regulate functionally distinct classes of genes. We demonstrate that distinct epigenetic signatures and cis-regulatory sequence motifs predicted to bind putative co-regulatory transcription factors define SOX10-activated and SOX10-repressed target genes. Collectively, these findings uncover a central role of SOX10 as a global regulator of gene expression in the melanocyte lineage by targeting diverse regulatory pathways.
机译:SOX10是黑素细胞发育和维持所必需的,并且与黑素瘤的发生和发展有关。但是,尚不完全了解SOX10指导促进黑素细胞谱系必需的适当基因表达程序的分子机制。在这里,我们采用遗传和表观基因组学分析方法来发现黑色素细胞中新的基因组靶标和SOX10以前未被认识的分子作用。通过对SOX10结合位点和染色质状态的表观遗传特性的全局分析,我们发现了全基因组范围内SOX10靶标的广泛目录。我们的发现表明,SOX10主要参与“开放”染色质区域并结合至远端调控元件,包括新型和先前已知的黑素细胞增强剂。综合的染色质占有率和转录组分析表明SOX10在转录激活和抑制中调节功能不同的基因类别均起作用。我们证明了预测与假定的共调节转录因子结合的独特的表观遗传学特征和顺式调节序列基序定义了SOX10激活和SOX10抑制的靶基因。总的来说,这些发现揭示了SOX10作为黑色素细胞谱系中基因表达的整体调节剂的核心作用,其靶向多种调节途径。

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