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Global and Hox-specific roles for the MLL1 methyltransferase

机译:MLL1甲基转移酶的全局和Hox特定作用

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The mixed-lineage leukemia (MLL1/ALL-1/HRX) histone methyltransferase is involved in the epigenetic maintenance of transcriptional memory and the pathogenesis of human leukemias. To understand its role in cell type specification, we determined the human genomic binding sites of MLL1. We found that MLL1! functions as a human equivalent of yeast Set1. Like Set1, MLL1 localizes with RNA polymerase II (Pol II) to the 5' end of actively transcribed genes, where histone H3 lysine 4 trimethylation occurs. Consistent with this global role in transcription, MLL1 also localizes to microRNA (miRNA) loci that are involved in leukemia and hematopoiesis. In contrast to the 5' proximal binding behavior at most protein-coding genes, MLL1 occupies an extensive domain within a transcriptionally active region of the HoxA cluster. The ability of MLL1 to serve as a start site-specific global transcriptional regulator and to participate in larger chromatin domains at the Hox genes reveals dual roles for MLL1 in maintenance of cellular identity.
机译:混合谱系白血病(MLL1 / ALL-1 / HRX)组蛋白甲基转移酶参与转录记忆的表观遗传维持和人类白血病的发病机理。为了了解其在细胞类型规范中的作用,我们确定了MLL1的人类基因组结合位点。我们发现了MLL1!相当于酵母Set1的人类等同物。像Set1一样,MLL1用RNA聚合酶II(Pol II)定位到活跃转录的基因的5'末端,在此处发生组蛋白H3赖氨酸4三甲基化。与这种在转录中的整体作用一致,MLL1还定位于涉及白血病和造血功能的microRNA(miRNA)基因座。与大多数蛋白质编码基因的5'近端结合行为相反,MLL1在HoxA簇的转录活性区内占据一个广泛的域。 MLL1充当起始位点特异性全球转录调节因子并参与Hox基因上较大的染色质结构域的能力揭示了MLL1在维持细胞身份方面的双重作用。

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