生物
乙酰化
糖酵解
赖氨酸
组蛋白
细胞生物学
酶
生物化学
氨基酸
基因
作者
He Huang,Shuang Tang,Ming Ji,Zhanyun Tang,Miho Shimada,Xiaojing Liu,Shankang Qi,Jason W. Locasale,Robert G. Roeder,Yingming Zhao,Xiaoling Li
出处
期刊:Molecular Cell
[Elsevier]
日期:2018-05-01
卷期号:70 (4): 663-678.e6
被引量:150
标识
DOI:10.1016/j.molcel.2018.04.011
摘要
Lysine 2-hydroxyisobutyrylation (Khib) is an evolutionarily conserved and widespread histone mark like lysine acetylation (Kac). Here we report that p300 functions as a lysine 2-hyroxyisobutyryltransferase to regulate glycolysis in response to nutritional cues. We discovered that p300 differentially regulates Khib and Kac on distinct lysine sites, with only 6 of the 149 p300-targeted Khib sites overlapping with the 693 p300-targeted Kac sites. We demonstrate that diverse cellular proteins, particularly glycolytic enzymes, are targeted by p300 for Khib, but not for Kac. Specifically, deletion of p300 significantly reduces Khib levels on several p300-dependent, Khib-specific sites on key glycolytic enzymes including ENO1, decreasing their catalytic activities. Consequently, p300-deficient cells have impaired glycolysis and are hypersensitive to glucose-depletion-induced cell death. Our study reveals an p300-catalyzed, Khib-specific molecular mechanism that regulates cellular glucose metabolism and further indicate that p300 has an intrinsic ability to select short-chain acyl-CoA-dependent protein substrates.
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