化学
生物正交化学
染色质
组蛋白
功能(生物学)
表观遗传学
细胞生物学
染色质重塑
生物化学
DNA
基因
组合化学
点击化学
生物
作者
Nan Zhang,Jinghua Wu,Farzana Hossain,Haidong Peng,Huapeng Li,Connor Gibson,Min Chen,Huan Zhang,Shuaixin Gao,Xinru Zheng,Yong‐Dong Wang,Jiangjiang Zhu,Jing Jing Wang,Ian Maze,Qingfei Zheng
摘要
Histone monoaminylation (i.e., serotonylation and dopaminylation) is an emerging category of epigenetic mark occurring on the fifth glutamine (Q5) residue of H3 N-terminal tail, which plays significant roles in gene transcription. Current analysis of histone monoaminylation is mainly based on site-specific antibodies and mass spectrometry, which either lacks high resolution or is time-consuming. In this study, we report the development of chemical probes for bioorthogonal labeling and enrichment of histone serotonylation and dopaminylation. These probes were successfully applied for the monoaminylation analysis of in vitro biochemical assays, cells, and tissue samples. The enrichment of monoaminylated histones by the probes further confirmed the crosstalk between H3Q5 monoaminylation and H3K4 methylation. Finally, combining the ex vivo and in vitro analyses based on the developed probes, we have shown that both histone serotonylation and dopaminylation are highly enriched in tumor tissues that overexpress transglutaminase 2 (TGM2) and regulate the three-dimensional architecture of cellular chromatin.
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