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A histone chaperone, DEK, transcriptionally coactivates a nuclear receptor.

机译:组蛋白伴侣DEK在转录上共激活核受体。

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摘要

Chromatin reorganization is essential for transcriptional control by sequence-specific transcription factors. However, the molecular link between transcriptional control and chromatin reconfiguration remains unclear. By colocalization of the nuclear ecdysone receptor (EcR) on the ecdysone-induced puff in the salivary gland, Drosophila DEK (dDEK) was genetically identified as a coactivator of EcR in both insect cells and intact flies. Biochemical purification and characterization of the complexes containing fly and human DEKs revealed that DEKs serve as histone chaperones via phosphorylation by forming complexes with casein kinase 2. Consistent with the preferential association of the DEK complex with histones enriched in active epigenetic marks, dDEK facilitated H3.3 assembly during puff formation. In some human myeloid leukemia patients, DEK was fused to CAN by chromosomal translocation. This mutation significantly reduced formation of the DEK complex, which is required for histone chaperone activity. Thus, the present study suggests that at least one histone chaperone can be categorized as a type of transcriptional coactivator for nuclear receptors.
机译:染色质重组对于通过序列特异性转录因子进行转录控制至关重要。然而,转录控制和染色质重构之间的分子联系仍然不清楚。通过在唾液腺中蜕皮激素诱导的粉扑上的核蜕皮激素受体(EcR)的共定位,果蝇DEK(dDEK)在遗传上被确定为昆虫细胞和完整果蝇中EcR的共激活因子。含有果蝇和人DEK的复合物的生化纯化和表征表明,DEK通过与酪蛋白激酶2形成复合物,通过磷酸化充当组蛋白伴侣。与DEK复合物与富含活性表观遗传标记的组蛋白的优先结合相一致,dDEK促进了H3。 3在粉扑形成过程中组装。在某些人类粒细胞白血病患者中,DEK通过染色体易位与CAN融合。这种突变显着减少了DEK复合物的形成,这是组蛋白伴侣活性所必需的。因此,本研究表明至少一种组蛋白分子伴侣可以归类为核受体的转录共激活因子。

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