Thursday, April 25, 2024 4/25/2024

Define the role of NUCKS1 in homologous recombination DNA repair and cancer biology

Award Number: R56ES021454
ORGANIZATION: NATIONAL INSTITUTE OF ENVIRONMENTAL HEALTH SCIENCES
OPDIV: NIH
AWARD CLASS: DISCRETIONARY
AWARD ACTIVITY TYPE: SCIENTIFIC/HEALTH RESEARCH (INCLUDES SURVEYS)

Group Awards By Issue Date FY or Funding FY:

View Award Abstract

PROJECT SUMMARY/ABSTRACT DNA double-strand breaks (DSBs) are highly toxic DNA lesions that can occur spontaneously during DNA replication, but also are introduced upon exposure of cells to chemical mutagens or ionizing radiation. DSBs can lead to genome instability and mutations, and defects in DSB repair underlie many human diseases, including disorders associated with cancer predisposition. Nuclear Ubiquitous Casein and Cyclin-dependent Kinases Substrate 1 (NUCKS1) is a highly post- translationally modified, DNA-binding and vertebrate-specific protein. NUCKS1 is a paralog of RAD51- Associated Protein 1 (RAD51AP1) and functions in DNA repair by homologous recombination (HR). Downregulation of NUCKS1 impairs HR, renders human cells hypersensitive to chemotherapeutic agents, compromises replication fork stability, and increases the susceptibility to radiation carcinogenesis in mice. NUCKS1 is phosphorylated at several residues upon exposure of cells to DNA damaging agents. However, the phenotypic consequences of these modifications on the HR reaction are not understood. Of note, loss of NUCKS1 downregulates the formation of early DNA damage-induced RAD51 foci and leads to greatly elevated and persistent levels of DNA damage-induced RAD54 foci. Moreover, NUCKS1 functionally interacts with RAD54. Yet, how NUCKS1-RAD54 complex formation impacts upon HR and cancer avoidance is not known. This application will delineate the biology of NUCKS1 and its functional interaction with the DNA motor protein RAD54 in biochemical and cell-based genetic assays. We will also include the analysis of post-translationally modified NUCKS1 and of a few select cancer-associated NUCKS1 variants to better understand how these impact upon HR and DNA replication. Taken together, our study will fill critical knowledge gaps in our understanding of NUCKS1 function in HR and tumor suppression. Given the importance of DSB repair and HR in tumor suppression and in the removal of DNA lesions induced by ionizing radiation and other environmental mutagens, the results from our investigation likely will have direct relevance to improved risk predictions for human health from environmental factors.


Issue Date FY	Funding FY	Legal Entity Name	Legal Entity Address	Legal Entity City	Legal Entity State	Legal Entity Zip Code	Legal Entity COUNTY	Legal Entity COUNTRY	Assistance Listing	Award Code	Budget Year	Action Date	Action Type	Action Amount

Issue Date FY: 2021 ( Subtotal = $0 )
2021	2019	COLORADO STATE UNIVERSITY	601 S HOWES ST	FORT COLLINS	CO	80521	LARIMER	USA	Environmental Health	000	7	1/31/2021	COMPETING CONTINUATION	$0
														Subtotal = $0

Issue Date FY: 2019 ( Subtotal = $225,000 )
2019	2019	COLORADO STATE UNIVERSITY	601 S HOWES ST	FORT COLLINS	CO	80521	LARIMER	USA	Environmental Health	000	7	9/9/2019	COMPETING CONTINUATION	$225,000
														Subtotal = $225,000

Grand Total All Awards = $225,000

Top

All Categories

About

Search

Reports

Data Submission

Award Information

Define the role of NUCKS1 in homologous recombination DNA repair and cancer biology

Award Number: R56ES021454

ORGANIZATION: NATIONAL INSTITUTE OF ENVIRONMENTAL HEALTH SCIENCES

OPDIV: NIH

AWARD CLASS: DISCRETIONARY

AWARD ACTIVITY TYPE: SCIENTIFIC/HEALTH RESEARCH (INCLUDES SURVEYS)

Federal Websites

Department of Health & Human Services

HHS Operating Divisions

HHS Staff Divisions

Download A Document Viewer