Abstract

Posttranslational modifications (PTMs) of histones play fundamental roles in diverse biological processes such as transcriptional regulation and genome maintenance, and aberrant regulations of histone PTMs have been increasingly implicated in many diseases including cancer. Basic research on well-studied histone lysine acetylation and methylation has led to the development of epigenetic therapies that are transitioning to the clinic, especially for treating hematological malignancies. In contrast, littl is known about an expanding group of newly discovered histone PTMs that include crotonylation, propionylation, butyrylation, malonylation succinylation, and 2-hydroxyisobutyrylation all of which are chemically related to histone acetylation and collectively termed lysine acylations. The existence of such diverse histone acylations in addition to Kac suggests that differential regulation of these PTMs has broad and important biological roles yet to be discovered. Focusing on histone lysine crotonylation, our recently published and preliminary studies support a role of histone crotonylation in transcriptional activation and reveal its potential link to oncogenesis through its interaction with cancer-related proteins. The general objective of our proposed research is to understand the fundamental role and mechanism of histone lysine crotonylation in the regulation of transcription in physiological and pathological conditions. To reach this goal we propose a multi-disciplinary approach where we will combine expertise from three labs to tackle this project. Through approaches in chromatin biology (Allis Lab, Aim 1), we will identify and characterize (a) the factors responsible for the enzymatic and metabolic regulation of histone Kcr and (b) the proteins that bind with Kcr and mediate its downstream effect. Through the lens of transcription (Roeder Lab, Aim 2) we will determine the direct contribution of histone lysine crotonylation and its associated proteins to gene activation and define the underlying mechanism of action using biochemically defined systems with reconstituted normal and disease-associated factors. Finally, by focusing on the role of Kcr in leukemias (Armstrong Lab, Aim3) we will define the genome-wide consequences histone lysine crotonylation has on chromatin landscape and gene expression in normal and transformed cells, and examine the functional importance of these modifications in leukemias via cell based assays and mouse models. Through this integrated approach we will work towards identifying and characterizing new proteins and pathways involved in normal and pathogenic gene regulation with the potential to uncover novel targets for epigenetic therapy of cancer.

Public Health Relevance

The initiation and maintenance of cancer is the product of aberrant gene regulation, a complex process involving many factors. Histones, the proteins that package DNA within the cell, the chemical modifications of histones, and the proteins that control and are controlled by these chemical modifications are known to play a critical role in the regulation of gene expression and have been implicated in a number of leukemias. A deep understanding of how these histone modifications operate within leukemias promises to identify targets for therapies that could potentially correct the cancer-causing mis-regulation of genes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA204639-04
Application #
9635621
Study Section
Molecular Genetics B Study Section (MGB)
Program Officer
Mietz, Judy
Project Start
2016-03-04
Project End
2021-02-28
Budget Start
2019-03-01
Budget End
2020-02-29
Support Year
4
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Rockefeller University
Department
Biology
Type
Graduate Schools
DUNS #
071037113
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Hoshii, Takayuki; Cifani, Paolo; Feng, Zhaohui et al. (2018) A Non-catalytic Function of SETD1A Regulates Cyclin K and the DNA Damage Response. Cell 172:1007-1021.e17
Sabari, Benjamin R; Tang, Zhanyun; Huang, He et al. (2018) Intracellular Crotonyl-CoA Stimulates Transcription through p300-Catalyzed Histone Crotonylation. Mol Cell 69:533
Huang, He; Tang, Shuang; Ji, Ming et al. (2018) p300-Mediated Lysine 2-Hydroxyisobutyrylation Regulates Glycolysis. Mol Cell 70:984
Wang, Shu-Ping; Tang, Zhanyun; Chen, Chun-Wei et al. (2017) A UTX-MLL4-p300 Transcriptional Regulatory Network Coordinately Shapes Active Enhancer Landscapes for Eliciting Transcription. Mol Cell 67:308-321.e6
Dann, Geoffrey P; Liszczak, Glen P; Bagert, John D et al. (2017) ISWI chromatin remodellers sense nucleosome modifications to determine substrate preference. Nature 548:607-611
Wan, Liling; Wen, Hong; Li, Yuanyuan et al. (2017) ENL links histone acetylation to oncogenic gene expression in acute myeloid leukaemia. Nature 543:265-269
Sabari, Benjamin R; Zhang, Di; Allis, C David et al. (2017) Metabolic regulation of gene expression through histone acylations. Nat Rev Mol Cell Biol 18:90-101
Goudarzi, Afsaneh; Zhang, Di; Huang, He et al. (2016) Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters. Mol Cell 62:169-180
Xiong, Xiaozhe; Panchenko, Tatyana; Yang, Shuang et al. (2016) Selective recognition of histone crotonylation by double PHD fingers of MOZ and DPF2. Nat Chem Biol 12:1111-1118
Zhao, Dan; Guan, Haipeng; Zhao, Shuai et al. (2016) YEATS2 is a selective histone crotonylation reader. Cell Res 26:629-32

Showing the most recent 10 out of 11 publications