Human mixed lineage leukemia 4 (MLL4), also known as KMT2D, regulates cell type specific transcriptional programs through enhancer activation. Along with the catalytic methyltransferase domain, MLL4 contains seven less characterized plant homeodomain (PHD) fingers. Here, we report that the sixth PHD finger of MLL4 (MLL4(PHD6)) binds to the hydrophobic motif of ten-eleven translocation 3 (TET3), a dioxygenase that converts methylated cytosine into oxidized derivatives. The solution NMR structure of the TET3-MLL4(PHD6) complex and binding assays show that, like histone H4 tail, TET3 occupies the hydrophobic site of MLL4(PHD6), and that this interaction is conserved in the seventh PHD finger of homologous MLL3 (MLL3(PHD7)). Analysis of genomic localization of endogenous MLL4 and ectopically expressed TET3 in mouse embryonic stem cells reveals a high degree overlap on active enhancers and suggests a potential functional relationship of MLL4 and TET3.
MLL4 binds TET3.
MLL4 与 TET3 结合
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作者:Becht Dustin C, Mohid Sk Abdul, Lee Ji-Eun, Zandian Mohamad, Benz Caroline, Biswas Soumi, Sinha Vikrant Kumar, Ivarsson Ylva, Ge Kai, Zhang Yi, Kutateladze Tatiana G
| 期刊: | Structure | 影响因子: | 4.300 |
| 时间: | 2024 | 起止号: | 2024 Jun 6; 32(6):706-714 |
| doi: | 10.1016/j.str.2024.03.005 | ||
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