Abstract

The Quantitative Proteomics core will provide high-end mass spectrometry based proteomic support to the P01 Project team members to help identify and quantify protein expression and post-translational modifications (PTMs) on histone and non-histone proteins from various cell lines and brain tumors. Histones are small proteins that help organize eukaryotic DNA information into nucleosomes, the repeating building blocks of chromatin. Gene regulation modulated via chromatin remodeling is achieved by the addition of PTMs to histones or by the incorporation of specialized histone variant members. Dysregulation of these pathways have been identified in many human disorders and cancers. Most histone related research work is centered on the use of antibodies that recognize a single histone PTM (Western blot, immunofluorescence, etc.). However, these types of experiments have drawbacks such as cross-reactivity, potentially limited specificity, and cannot be used to discover novel histone PTMs. Additionally, these antibodies often have issues with the recognition of their intended single modification site in modification-dense regions, a phenomenon known as epitope occlusion. Here we will use our novel mass spectrometry based proteomics platforms and integrated bioinformatics to comprehensively interrogate the PTM profiles of histones extracted from model cell lines, primary cells and tumor tissue harboring histone mutations. These experiments will allow for precise measurement of the abundance of over 100 different histone modification and variant proteoforms. Additionally, the Garcia lab has produced arguably the best platform for analysis of combinatorial histone modifications to determine crosstalk relationships between different modified sites. Studies aimed to isolate chromatin from specific cancer related genes will also be performed to understand the local histone environment contributing to tumoregenesis. We will also perform experiments to identify proteins that bind to specific cancer enriched histone PTMs (e.g. histone readers), or non-histone proteins that are modified themselves and may affect chromatin networks that modulate crucial gene expression programs.

Public Health Relevance

Mutation to histone genes have been found in different types of cancers. This research will help define altered chromatin pathways due to these mutations, thus laying down the foundation for potential development of novel targeted drug therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA196539-01
Application #
8934751
Study Section
Special Emphasis Panel (ZCA1-RPRB-B (M1))
Project Start
Project End
Budget Start
2015-07-01
Budget End
2016-06-30
Support Year
1
Fiscal Year
2015
Total Cost
$394,519
Indirect Cost
$133,045

  Institution

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

  Publications

Yuan, Zuo-Fei; Sidoli, Simone; Marchione, Dylan M et al. (2018) EpiProfile 2.0: A Computational Platform for Processing Epi-Proteomics Mass Spectrometry Data. J Proteome Res 17:2533-2541
Zhang, Hanghang; Pandey, Somnath; Travers, Meghan et al. (2018) Targeting CDK9 Reactivates Epigenetically Silenced Genes in Cancer. Cell 175:1244-1258.e26
Kreher, Jeremy; Takasaki, Teruaki; Cockrum, Chad et al. (2018) Distinct Roles of Two Histone Methyltransferases in Transmitting H3K36me3-Based Epigenetic Memory Across Generations in Caenorhabditis elegans. Genetics 210:969-982
Karch, Kelly R; Coradin, Mariel; Zandarashvili, Levani et al. (2018) Hydrogen-Deuterium Exchange Coupled to Top- and Middle-Down Mass Spectrometry Reveals Histone Tail Dynamics before and after Nucleosome Assembly. Structure 26:1651-1663.e3
Simithy, Johayra; Sidoli, Simone; Garcia, Benjamin A (2018) Integrating Proteomics and Targeted Metabolomics to Understand Global Changes in Histone Modifications. Proteomics 18:e1700309
Di Marcantonio, Daniela; Martinez, Esteban; Sidoli, Simone et al. (2018) Protein Kinase C Epsilon Is a Key Regulator of Mitochondrial Redox Homeostasis in Acute Myeloid Leukemia. Clin Cancer Res 24:608-618
Valera, Elvis Terci; McConechy, Melissa K; Gayden, Tenzin et al. (2018) Methylome analysis and whole-exome sequencing reveal that brain tumors associated with encephalocraniocutaneous lipomatosis are midline pilocytic astrocytomas. Acta Neuropathol 136:657-660
Wojcik, Felix; Dann, Geoffrey P; Beh, Leslie Y et al. (2018) Functional crosstalk between histone H2B ubiquitylation and H2A modifications and variants. Nat Commun 9:1394
Lee, Chul-Hwan; Yu, Jia-Ray; Kumar, Sunil et al. (2018) Allosteric Activation Dictates PRC2 Activity Independent of Its Recruitment to Chromatin. Mol Cell 70:422-434.e6
Guo, Qi; Sidoli, Simone; Garcia, Benjamin A et al. (2018) Assessment of Quantification Precision of Histone Post-Translational Modifications by Using an Ion Trap and down To 50?000 Cells as Starting Material. J Proteome Res 17:234-242

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