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Mechanistic insights into the recognition of 5-methylcytosine oxidation derivatives by the SUVH5 SRA domain

机译:关于SUVH5 SRA域识别5-甲基胞嘧啶氧化衍生物的机理的见解

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摘要

5-Methylcytosine (5 mC) is associated with epigenetic gene silencing in mammals and plants. 5 mC is consecutively oxidized to 5-hydroxymethylcytosine (5 hmC), 5-formylcytosine (5fC) and 5-carboxylcytosine (5caC) by ten-eleven translocation enzymes. We performed binding and structural studies to investigate the molecular basis of the recognition of the 5 mC oxidation derivatives in the context of a CG sequence by the SET- and RING-associated domain (SRA) of the SUVH5 protein (SUVH5 SRA). Using calorimetric measurements, we demonstrate that the SRA domain binds to the hydroxymethylated CG (5hmCG) DNA duplex in a similar manner to methylated CG (5mCG). Interestingly, the SUVH5 SRA domain exhibits weaker affinity towards carboxylated CG (5caCG) and formylated CG (5fCG). We report the 2.6 Å resolution crystal structure of the SUVH5 SRA domain in a complex with fully hydroxymethyl-CG and demonstrate a dual flip-out mechanism, whereby the symmetrical 5hmCs are simultaneously extruded from the partner strands of the DNA duplex and are positioned within the binding pockets of individual SRA domains. The hydroxyl group of 5hmC establishes both intra- and intermolecular interactions in the binding pocket. Collectively, we show that SUVH5 SRA recognizes 5hmC in a similar manner to 5 mC, but exhibits weaker affinity towards 5 hmC oxidation derivatives.
机译:5-甲基胞嘧啶(5 mC)与哺乳动物和植物中的表观遗传基因沉默有关。 5 mC被十一个11易位酶连续氧化为5-羟甲基胞嘧啶(5 hmC),5-甲酰基胞嘧啶(5fC)和5-羧基胞嘧啶(5caC)。我们进行了结合和结构研究,以研究SUVH5蛋白(SUVH5 SRA)的SET和RING相关域(SRA)在CG序列中识别5 mC氧化衍生物的分子基础。使用量热法测量,我们证明了SRA域以与甲基化CG(5mCG)相似的方式与羟甲基化CG(5hmCG)DNA双链体结合。有趣的是,SUVH5 SRA结构域对羧化CG(5caCG)和甲酰化CG(5fCG)的亲和力较弱。我们报告SUVH5 SRA域与完全羟甲基-CG的复合物中的2.6Å分辨率晶体结构,并证明了双重翻转机制,其中对称的5hmCs同时从DNA双链体的伴侣链中挤出,并位于绑定各个SRA域的口袋。 5hmC的羟基在结合口袋中建立分子内和分子间相互作用。总的来说,我们表明SUVH5 SRA以与5 mC相似的方式识别5hmC,但对5 hmC氧化衍生物的亲和力较弱。

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