Development of Site-specific O-GlcNAc Antibodies for Epigenetic Research

Information

• Research Project
• 9479196

• ApplicationId

  9479196

• Core Project Number

  R44GM110887

• Full Project Number

  5R44GM110887-03

• Serial Number

  110887

• FOA Number

  PA-16-157

• Sub Project Id

• Project Start Date

  7/1/2014 - 10 years ago

• Project End Date

  4/30/2020 - 4 years ago

• Program Officer Name

  MARINO, PAMELA

• Budget Start Date

  5/1/2018 - 6 years ago

• Budget End Date

  4/30/2019 - 5 years ago

• Fiscal Year

  2018

• Support Year

  03

• Suffix

• Award Notice Date

  4/23/2018 - 6 years ago

Organizations

• GLYCOSCIENTIFIC, LLC

Project Summary O-glycosylation of nuclear and cytoplasmic proteins by a single ?-N-acetyl-D-glucosamine moiety (O- GlcNAc) is a common post-translational modification that is highly dynamic and fluctuates in response to cellular stimuli. This type of glycosylation has been found on approximately a thousand human proteins to date, and is thought to be nearly as wide-spread and abundant as protein phosphorylation. In fact, O-GlcNAc often competes with protein phosphorylation, and these two modifications have extensive crosstalk in the regulation of signaling, transcription, and the functions of oncogenes and tumor suppressors. The modification appears to play a major role in key pathophysiological conditions including cancer, Alzheimer?s disease, and diabetes. Many of the first proteins identified carrying this modification were transcription factors, and it has become clear in the last several years that O-GlcNAc plays a major role in chromatin remodeling and gene expression. The focus of this proposal is to develop site-specific antibodies that can be used as tools in the elucidation of the role that O-GlcNAc plays in epigenetics. In the predecessor Phase I grant we focused on evaluating synthetic immunogens, the production of polyclonal antibodies (PAbs) to five sites of O-GlcNAc modification on the four core histones (Histone 2A, 2B, 3, and 4), and characterizing these antibodies. We were successful with each Aim of this previous project, which leads to this Phase II proposal. Here, we propose to utilize our proprietary immunization strategy to significantly expand our repertoire of site-specific O-GlcNAc antibodies to include the majority of proteins currently known to be modified in this manner that are also involved in gene expression. Consequently, if we are successful, researchers will have access to a wide-range of site-specific Abs developed for epigenetic research, and thus we feel that this study will have an immediate impact on epigenetic research and could have far reaching implications in disease research.

IC Name

• Activity

  R44

• Administering IC

  GM

• Application Type

  5

• Direct Cost Amount

• Indirect Cost Amount

• Total Cost

  350000

• Sub Project Total Cost

• ARRA Funded

  False

• CFDA Code

  859

• Ed Inst. Type

• Funding ICs

  NIGMS:350000\

• Funding Mechanism

  SBIR-STTR RPGs

• Study Section

  ZRG1

• Study Section Name

  Special Emphasis Panel

• Organization Name

  GLYCOSCIENTIFIC, LLC

• Organization Department

• Organization DUNS

  829734347

• Organization City

  ATHENS

• Organization State

  GA

• Organization Country

  UNITED STATES

• Organization Zip Code

  306021514

• Organization District

  UNITED STATES