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Myeloid Leukemia Factor acts in a chaperone complex to regulate transcription factor stability and gene expression

机译:髓样白血病因子在伴侣复合物中起作用以调节转录因子的稳定性和基因表达

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摘要

Mutations that affect Myeloid Leukemia Factor (MLF) proteins are associated with leukemia and several other cancers. However, with no strong homology to other proteins of known function, the role of MLF proteins in the cell has remained elusive. Here we describe a proteomics approach that identifies MLF as a member of a nuclear chaperone complex containing a DnaJ protein, BAG2 and Hsc70. This complex associates with chromatin and regulates expression of target genes. The MLF complex is bound to sites of nucleosome depletion and sites containing active chromatin marks (e.g. H3K4me3 and H3K4me1). Hence, MLF binding is enriched at promoters and enhancers. Additionally, the MLF-chaperone complex functions to regulate transcription factor stability, including the RUNX transcription factor involved in hematopoiesis. Though Hsc70 and other co-chaperones have been shown to play a role in nuclear translocation of a variety of proteins including transcription factors, our findings suggest that MLF and the associated co-chaperones play a direct role in modulating gene transcription.
机译:影响髓系白血病因子(MLF)蛋白的突变与白血病和其他几种癌症有关。但是,由于与已知功能的其他蛋白质没有强同源性,因此MLF蛋白在细胞中的作用仍然难以捉摸。在这里,我们描述了一种蛋白质组学方法,该方法将MLF鉴定为包含DnaJ蛋白,BAG2和Hsc70的核伴侣蛋白复合物的成员。该复合物与染色质结合并调节靶基因的表达。 MLF复合物结合到核小体耗竭位点和含有活性染色质标记的位点(例如H3K4me3和H3K4me1)。因此,MLF结合在启动子和增强子处富集。另外,MLF-伴侣复合物具有调节转录因子稳定性的功能,包括参与造血作用的RUNX转录因子。尽管已显示Hsc70和其他伴侣伴侣在包括转录因子在内的多种蛋白质的核转运中发挥作用,但我们的发现表明MLF和相关伴侣伴侣在调节基因转录中起直接作用。

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