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Finding the gas pedal on a slow sirtuin

机译:在缓慢的Sirtuin上找到油门踏板

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摘要

The class III histone deacetylase sirtuin 6 (SIRT6) modulates numerous functions in the cell by deacetylating histone lysine residues. Interestingly, SIRT6's efficiency in in vitro experiments is far greater against substrates carrying long-chain fatty acyl modifications such as myristoylated lysine compared with acetylated counterparts, but the deacetylase activity can be stimulated by fatty acids and small-molecule allosteric modulators. A new study helps to explain this puzzling activation using a novel activator, thorough kinetic investigation, and mutagenesis studies. These data help elucidate the molecular requirements for activation of SIRT6 and provide a foundation for development of activators for therapeutic purposes.
机译:III类组蛋白脱乙酰基酶Sirtuin 6(SIRT6)通过使组蛋白赖氨酸残基脱乙酰基来调节细胞中的许多功能。有趣的是,与乙酰化的对应物相比,SIRT6在体外实验中对带有长链脂肪酰基修饰物(如肉豆蔻酰赖氨酸)的效率要高得多,但是脂肪酸和小分子变构调节剂可以刺激脱乙酰酶活性。一项新的研究有助于使用新型激活剂,彻底的动力学研究和诱变研究来解释这种令人费解的激活。这些数据有助于阐明激活SIRT6的分子要求,并为开发用于治疗目的的激活剂奠定基础。

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