Time-Resolved Analysis Reveals Rapid Dynamics and Broad Scope of the CBP/p300 Acetylome

Brian T. Weinert,Takeo Narita,Shankha Satpathy,Balaji Srinivasan,Bogi Karbech Hansen,Christian Schölz,William B. Hamilton,Beth E. Zucconi,Wesley Wei Wang,Wenshe R. Liu,Joshua M. Brickman,Edward A. Kesicki,Albert Lai,Kenneth D. Bromberg,Philip A. Cole,Chunaram Choudhary

Time-Resolved Analysis Reveals Rapid Dynamics and Broad Scope of the CBP/p300 Acetylome

2018

Brian T. Weinert
Takeo Narita
Shankha Satpathy
Balaji Srinivasan
Bogi Karbech Hansen
Christian Schölz
William B. Hamilton
Beth E. Zucconi
Wesley Wei Wang
Wenshe R. Liu
Joshua M. Brickman
Edward A. Kesicki
Albert Lai
Kenneth D. Bromberg
Philip A. Cole
Chunaram Choudhary

Summary The acetyltransferases CBP and p300 are multifunctional transcriptional co-activators. Here, we combined quantitative proteomics with CBP/p300-specific catalytic inhibitors, bromodomain inhibitor, and gene knockout to reveal a comprehensive map of regulated acetylation sites and their dynamic turnover rates. CBP/p300 acetylates thousands of sites, including signature histone sites and a multitude of sites on signaling effectors and enhancer-associated transcriptional regulators. Time-resolved acetylome analyses identified a subset of CBP/p300-regulated sites with very rapid (

Keywords:

Computational biology
Genetics
Gene knockout
Transcription (biology)
Quantitative proteomics
Acetylation
Histone
Enhancer
Bromodomain
Proteomics
Biology

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

147

Citations