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Functional Targets of the Monogenic Diabetes Transcription Factors HNF-1α and HNF-4α Are Highly Conserved Between Mice and Humans

机译:单基因糖尿病转录因子HNF-1α和HNF-4α的功能靶标在小鼠和人类之间高度保守。

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摘要

OBJECTIVEThe evolutionary conservation of transcriptional mechanisms has been widely exploited to understand human biology and disease. Recent findings, however, unexpectedly showed that the transcriptional regulators hepatocyte nuclear factor (HNF)-1α and -4α rarely bind to the same genes in mice and humans, leading to the proposal that tissue-specific transcriptional regulation has undergone extensive divergence in the two species. Such observations have major implications for the use of mouse models to understand HNF-1α– and HNF-4α–deficient diabetes. However, the significance of studies that assess binding without considering regulatory function is poorly understood.
机译:目的转录机制的进化保守性已被广泛用于理解人类生物学和疾病。然而,最近的发现出乎意料地表明,转录调节子肝细胞核因子(HNF)-1α和-4α在小鼠和人类中很少与相同的基因结合,从而导致提出以下建议:组织特异性转录调节已在两者之间发生了广泛的分歧。种类。这些观察结果对使用小鼠模型了解HNF-1α和HNF-4α缺乏型糖尿病具有重要意义。但是,对评估结合而不考虑调节功能的研究的重要性了解甚少。

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