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Of numbers and movement – understanding transcription factor pathogenesis by advanced microscopy

机译:数字与运动 - 理解高级显微镜的转录因子发病机制

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ABSTRACT Transcription factors (TFs) are life-sustaining and, therefore, the subject of intensive research. By regulating gene expression, TFs control a plethora of developmental and physiological processes, and their abnormal function commonly leads to various developmental defects and diseases in humans. Normal TF function often depends on gene dosage, which can be altered by copy-number variation or loss-of-function mutations. This explains why TF haploinsufficiency (HI) can lead to disease. Since aberrant TF numbers frequently result in pathogenic abnormalities of gene expression, quantitative analyses of TFs are a priority in the field. In vitro single-molecule methodologies have significantly aided the identification of links between TF gene dosage and transcriptional outcomes. Additionally, advances in quantitative microscopy have contributed mechanistic insights into normal and aberrant TF function. However, to understand TF biology, TF-chromatin interactions must be characterised in vivo , in a tissue-specific manner and in the context of both normal and altered TF numbers. Here, we summarise the advanced microscopy methodologies most frequently used to link TF abundance to function and dissect the molecular mechanisms underlying TF HIs. Increased application of advanced single-molecule and super-resolution microscopy modalities will improve our understanding of how TF HIs drive disease.
机译:摘要转录因子(TFS)是寿命维持,因此是密集研究的主题。通过调节基因表达,TFS控制过多的发育和生理过程,它们的异常函数通常导致人类的各种发育缺陷和疾病。正常的TF功能通常取决于基因剂量,这可以通过拷贝数变异或功能损失来改变。这解释了为什么TF HaploUnficy(HI)可以导致疾病。由于异常TF数频繁导致基因表达的致病异常,因此TFS的定量分析是该领域的优先级。体外单分子方法有显着促进了TF基因剂量和转录结果之间的链接的鉴定。另外,定量显微镜的进步已经为正常和异常的TF功能提供了贡献的机械洞察。然而,为了了解TF生物学,TF-染色质相互作用必须以组织特异性方式和在正常和改变的TF数的上下文中以体内表征。在这里,我们总结了最常用的先进显微镜方法,用于将TF丰度链接到功能,并将其解剖其底层的分子机制。提高先进的单分子和超分辨率显微镜样式的应用将改善我们对他的驱动疾病的理解。

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