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Gap Junctions and Cancer Drug Therapy

$49,924F33FY2005CANIH

University Of Toledo Health Sci Campus, Toledo OH

Investigators

Abstract

DESCRIPTION (provided by applicant): Gap junctions (GJs) connect the interiors of neighboring cells and permit the passive cell-to-cell flux of molecules and ions less than approximately 1 kDa. GJs have the potential to modify conventional and non-conventional cancer therapies in several ways, but this has seen little investigation. I propose to investigate how GJs alter the cytotoxicity of chemotherapeutic agents known as ribonucleotide reductase (RR) inhibitors. These agents induce nucleotide imbalances in cells, and I hypothesize nucleotide buffering via GJs will impact RR toxicity. I have proposed two Specific Aims to address the hypothesis: Aim 1: Isolate clones of GJ-competent and GJ-incompetent WB cells that are sensitive and resistant to the RR inhibitor, hydroxyurea (HU). We will use WB-F344 (GJ+) and WB-aB1 (GJ-) cells for this purpose and will characterize HU cytotoxic dose response, nucleotide pools, and RR activity and expression. Aim 2: Quantify the effects of GJs on cytotoxic response and nucleotide buffering in co-cultures of HU-sensitive and resistant cells. HU-sensitive and resistant, GJ+ or GJ- cells will be co-cultured and treated with HU, then cytotoxicity and nucleotides will be quantified in each type of cell. These studies may lead to new cancer therapy paradigms and treatments.

View original record on NIH RePORTER →