Abstract

Application): Mechanisms of action of oxidative DNA-damaging agents and cellular responses to these agents are problems of considerable medical importance. However, all of the mechanisms cells use to defend against and repair the damage are not known. The long-term goal of this project is to determine mechanisms cells use to protect against oxidative damage. Specifically, the long- term objectives are to understand DNA repair pathways, recovery processes, and proteins important in cellular responses to oxidative DNA-damaging agents. Three classes of oxidative DNA-damaging agents are included in the study: ionizing radiation, anti-cancer bleomycins and structurally related phleomycins, and hydrogen peroxide. The bleomycin group of antibiotics is an important therapeutic agent useful as a single agent in treating several human cancers and widely used in combination chemotherapy and radiotherapy. Mutant blm5 strains will be used in the proposed work to investigate the genetic and biochemical controls of oxidative damage. The blm mutants of Saccharomyces cerevisiae were isolated on the basis of their hypersensitivities to lethal effects of oxidants.
Specific aims i nclude studies of the processing and repair of DNA lesions produced after exposure of cells to oxidative DNA-damaging agents, and establishing the role of the BLM5 gene in maintaining normal eukaryotic DNA function and repair after oxidative damage. The studies will add new knowledge of general importance to fields of DNA repair and metabolism, and genetics. Understanding the introduction and repair of lesions after oxidative damage, moreover, will not be completed until all the major genes involved have been identified and characterized. Data will be acquired from interrelated studies at the cellular and molecular levels, using genetic characterization, molecular biology, and biochemistry. These include DNA sequence analyses, methodologies for studying DNA damage and repair, and transmission and scanning electron microscopy. DNA repair will be studied using pulsed-field electrophoresis, recombinational repair of double DNA breaks using yeast plasmids, and mitototic recombination assays. Experiments also include in vitro mutagenesis, the production and characterization of null mutation, identifying interactions with proteins using the two-hybrid system of identifying interacting proteins using the two-hybrid system of identifying interacting proteins, and cloning human homologs from genomic libraries. The genetic sophistication, molecular flexibility, and availability of mutant strains of S. cerevisiae permit these studies and technical approaches. The unique knowledge gained in this project has signification implications for cellular studies directed toward determining mechanisms of oxidant injury and repair as well as clinical cancer management.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
5S06GM008168-20
Application #
6301685
Study Section
Project Start
2000-02-01
Project End
2001-01-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
20
Fiscal Year
2000
Total Cost
$25,678
Indirect Cost

  Institution

Name
City College of New York
Department
Type
DUNS #
603503991
City
New York
State
NY
Country
United States
Zip Code
10031

  Publications

Fried, Eric S; Li, Yue-Ming; Gilchrist, M Lane (2017) Phase Composition Control in Microsphere-Supported Biomembrane Systems. Langmuir 33:3028-3039
Gilchrist, M Lane; Ahn, Kwangwook; Li, Yue-Ming (2016) Imaging and Functional Analysis of ?-Secretase and Substrate in a Proteolipobead System with an Activity-Based Probe. Anal Chem 88:1303-11
Fried, Eric S; Luchan, Joshua; Gilchrist, M Lane (2016) Biodegradable, Tethered Lipid Bilayer-Microsphere Systems with Membrane-Integrated ?-Helical Peptide Anchors. Langmuir 32:3470-5
Banerjee, Shaibal; Sinha, Saikat; Pradhan, Padmanava et al. (2016) Regiospecifically Fluorinated Polycyclic Aromatic Hydrocarbons via Julia-Kocienski Olefination and Oxidative Photocyclization. Effect of Fluorine Atom Substitution on Molecular Shape. J Org Chem 81:3983-93
Beck, Cade; Singh, Tanya; Farooqi, Angela et al. (2016) Controlled microfluidics to examine growth-factor induced migration of neural progenitors in the Drosophila visual system. J Neurosci Methods 262:32-40
Salas-Ramirez, Kaliris Y; Bagnall, Ciara; Frias, Leslie et al. (2015) Doxorubicin and cyclophosphamide induce cognitive dysfunction and activate the ERK and AKT signaling pathways. Behav Brain Res 292:133-41
Thomson, Paul F; Parrish, Damon; Pradhan, Padmanava et al. (2015) Modular, Metal-Catalyzed Cycloisomerization Approach to Angularly Fused Polycyclic Aromatic Hydrocarbons and Their Oxidized Derivatives. J Org Chem 80:7435-46
Small, Chiyedza; Ramroop, Johnny; Otazo, Maria et al. (2014) An unexpected link between notch signaling and ROS in restricting the differentiation of hematopoietic progenitors in Drosophila. Genetics 197:471-83
Zhong, Lina; Tu, Raymond; Gilchrist, M Lane (2013) Tether-supported biomembranes with ?-helical peptide-based anchoring constructs. Langmuir 29:299-307
Guleyupoglu, Berkan; Schestatsky, Pedro; Edwards, Dylan et al. (2013) Classification of methods in transcranial electrical stimulation (tES) and evolving strategy from historical approaches to contemporary innovations. J Neurosci Methods 219:297-311

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