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Wangila Research

Abstract Dr. G. Wangila

Title of Project         Metal Chelates in Prevention of Cisplatin-Induced Kidney Cell Death

Abstract                  We propose to synthesize, characterize, and test several new metal (Cu and Zn) complexes of salicylic acid and aminothiol derivatives as catalytic antioxidants that scavenge a wide range of reactive oxygen species (ROS), such as superoxide dismutase (SOD), hydrogen peroxide, peroxynitrite, and lipid peroxyl radicals. Several compounds in this class have been shown to be efficacious in a variety of ways in in vitro and in vivo oxidative stress models of human diseases. Our preliminary data strongly indicate that these metal complexes satisfy many of the criteria for prevention and treatment of cisplatin-induced nephrotoxicity, as they are active, stable, and nontoxic antioxidants. Thus, we hypothesize that Cu- and Zn-metallo-element chelates will protect kidney tubular epithelial cells from cisplatin injury because these chelates have antioxidant activity, and can suppress apoptosis and facilitate recovery. We propose two specific aims: Aim 1: Synthesize and characterize the Cu- and Zn-metalloelement chelates. This aim will focus on chemical studies of new and previously known but not fully characterized compounds. And Aim 2: Test the nephroprotective activity of the metallocompounds in biological systems. The study will involve (1) an assessment of antiapoptotic activity of the SOD-mimetic metal chelates with regard to cellular mechanisms by which metal chelates may prevent cisplatin-induced proximal tubule cell death; (2) an examination of the mechanism by which metal chelates suppress apoptosis by preventing cisplatin-induced translocation of proapoptotic Bax from the cytosol to the mitochondria; (3) a study of how metal chelates prevent cisplatin-induced cytochrome c release from the inner mitochondrial membrane and its appearance in the cytosol, and significantly reduces cisplatin-induced caspase-3 activation, based on the SOD-mimetic, catalase-mimetic, and/or peroxidase-mimetic reactivities of metal chelate enzymes required to overcome cisplatin-induced pathology; and (4) a determination of the effects of metal chelates on endonuclease G leakage from mitochondria, its nuclear import, and apoptotic DNA fragmentation. A logical extension of the studies in this proposal carried out in vitro will be extended in vivo. More specifically, we plan to study the mechanisms by which the SOD-mimetic and metal chelates offer protection to cisplatin-induced biological system. For these studies, we will collaborate with investigators at UAMS who have a long-standing interest and enthusiasm in studying metal chelates and mimetic activities of essential metal chelates.

 

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Updated 07/23/2008

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