Abstract

Major class III anti-arrhythmic agents (C3As) acts by prolonging action potential duration. K+ channels act as receptors for these agents and the actions of these agents differently modulate these channel subtypes. Dysfunction of some of these channel subtypes may also be the underlying cause in many types of cardiac arrhythmic during the ischemic and post-ischemic periods in patients. Anti-arrhythmic drug research attempts to invent drugs that rate unlike many of the available C3As. One the other hand may of the potassium channel openers (PCOs) used mainly as anti-hypertensive agents have anti-arrhythmic properties. Thus, there is a need to invent drugs that are like C3As, but would be effective (at faster heart rate) in dealing with early depolarization induced extrasystoles (""""""""Torsades de pointes""""""""). These last events are mostly calcium mediated. The long term aim of this proposal would be to determine the effects of several new classes of K+ channel modulators ( e.g., 2,3 Butanedione monoxime containing compounds which are also possible Ca2+ channel blockers, others are PCOs) besides C3As in whole cells (atrial tumor cells and native rat myocytes) and test the effectiveness of theses agents on drug induced or physiologically induced arryhthmias in canine cardiac tissue. A major strategy will be to use two functionally diverse K+ channel subtypes in two different cell types: atrial tumor cells (AT-1 cells, prominently studied for delayed rectifier type K+ channel) and rat myocyte (prominently generates transient outward K+ current). One rationale for extending the study to the tissue level is that many C3As reduce force of contradiction while some of the monoxime containing compounds increased contracted force in ventricular muscle tissue in our laboratory.
The specific aims of this proposal will be: 1) Investigate the effects of C3As, monoxime containing compounds and PCOs on K+ currents in rat myocytes and AT-1 cells; 2) Investigate the effects of physiologically (metabolic blockage/hypoxia) induced changes in K+ currents and contrast these with those in aim 1; 3) Investigate the effects of several of these anti-arrhythmic drugs on myocardial force and drug (or physiologically) induced arryhthmias (or membrane potential perturbations). Parallel comparison and contrast of whole cell current and potential in the presence of these novel channel modulators with their effects in whole tissue will facilitate the understanding and development of more specific and effective anti-arrhythmic agents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
5S06GM008037-30
Application #
6485257
Study Section
Project Start
2001-08-01
Project End
2002-07-31
Budget Start
Budget End
Support Year
30
Fiscal Year
2001
Total Cost
$179,091
Indirect Cost

  Institution

Name
Meharry Medical College
Department
Type
DUNS #
City
Nashville
State
TN
Country
United States
Zip Code
37208

  Publications

Pulliam, Stephanie R; Pellom Jr, Samuel T; Shanker, Anil et al. (2016) Butyrate regulates the expression of inflammatory and chemotactic cytokines in human acute leukemic cells during apoptosis. Cytokine 84:74-87
Chen, Chau-Kuang; Bruce, Michelle; Tyler, Lauren et al. (2013) Analysis of an environmental exposure health questionnaire in a metropolitan minority population utilizing logistic regression and Support Vector Machines. J Health Care Poor Underserved 24:153-71
Boadi, William Y; Harris, Shalandus; Anderson, Justin B et al. (2013) Lipid peroxides and glutathione status in human progenitor mononuclear (U937) cells following exposure to low doses of nickel and copper. Drug Chem Toxicol 36:155-62
Choudhury, Shahana A; Ladson, Gwinnett; Kabir, Madina S (2012) Evaluation of serotype-specific immunity to Streptococcus pneumoniae in pregnant women and cord blood of infants: impact of race and ethnicity. J Natl Med Assoc 104:251-7
Hall 3rd, Mack; Misra, Smita; Chaudhuri, Minu et al. (2011) Peptide aptamer mimicking RAD51-binding domain of BRCA2 inhibits DNA damage repair and survival in Trypanosoma brucei. Microb Pathog 50:252-62
Kawai, Yumiko; Garduño, Lakisha; Theodore, Melanie et al. (2011) Acetylation-deacetylation of the transcription factor Nrf2 (nuclear factor erythroid 2-related factor 2) regulates its transcriptional activity and nucleocytoplasmic localization. J Biol Chem 286:7629-40
Rana, Tanu; Misra, Smita; Mittal, Mukul K et al. (2011) Mechanism of down-regulation of RNA polymerase III-transcribed non-coding RNA genes in macrophages by Leishmania. J Biol Chem 286:6614-26
Farrow, Anitra L; Rana, Tanu; Mittal, Mukul K et al. (2011) Leishmania-induced repression of selected non-coding RNA genes containing B-box element at their promoters in alternatively polarized M2 macrophages. Mol Cell Biochem 350:47-57
Sharma, Shvetank; Singha, Ujjal K; Chaudhuri, Minu (2010) Role of Tob55 on mitochondrial protein biogenesis in Trypanosoma brucei. Mol Biochem Parasitol 174:89-100
Sheng, Liu; Ding, Xinxin; Ferguson, Marcus et al. (2010) Prenatal polycyclic aromatic hydrocarbon exposure leads to behavioral deficits and downregulation of receptor tyrosine kinase, MET. Toxicol Sci 118:625-34

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