Abstract

Digitalis intoxication has been reported to occur in as many as 20 percent of hospitalized patients receiving a cardiac glycoside. There is overlap in serum glycoside concentrations in patients with and without toxicity, indicating a narrow margin of safety of these drugs, and also patient-to-patient variation in drug sensitivity which limits the usefulness of a target concentration strategy. Old age, acute myocardial infarction or ischemia, hypoxemia, hypokalemia and several other conditions reduce the tolerance of the patient to the digitalis glycosieds. Thus, the mechanisms by which the glycoside sensitivity of the heart is altered by old age, ischemic heart disease or other drugs will be studied using animal models. Digitalis sensitivity of the heart may be altered at three levels, i.e., changes in pharmacokinetics, receptor kinetics and events that follow drug binding to the receptor. The proposed project primarily focuses on alterations in drug-receptor interactions. Experiments in aged animals an drug-interaction studies will be performed in rats, hamsters, guinea pigs and dogs. The interaction of cardiac glycosides with their putative pharmacological and toxic receptor, the Na,K-ATPase enzyme system, is markedly affected by intracellular sodium and extracellular potassium. This enzyme system is intimately related to the membrane sodium pump, and therefore the interaction of the glycoside with this system in turn results in an alteration in the movement of sodium and potassium across the cell membrane. Thus, whether the aging process causes alterations in transmembrane sodium movement, properties or tissue concentration of Na,K-ATPase, the reserve capacity of the sodium pump, and other factors which can alter sodium pump activity will be examined. Furthermore, whether the changes in transmembrane ion movement brough about by aging, ischemia, anoxia, quinidine, lidocaine or beta adrenergic blocking agents effect the glycoside sensitivity of cardiac muscle will be studied. Results of these studies will help us understand the mechanisms of action of these drugs as well as providing a rational basis for identifying hypersensitive patients as a group, and to set a lower target concentration suitable for those individuals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG002398-05
Application #
3114435
Study Section
Cardiovascular Study Section (CVA)
Project Start
1982-03-01
Project End
1987-07-31
Budget Start
1986-03-01
Budget End
1987-07-31
Support Year
5
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Michigan State University
Department
Type
Schools of Medicine
DUNS #
193247145
City
East Lansing
State
MI
Country
United States
Zip Code
48824

  Publications

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Sealey, David C F; Zheng, Le; Taboski, Michael A S et al. (2010) The N-terminus of hTERT contains a DNA-binding domain and is required for telomerase activity and cellular immortalization. Nucleic Acids Res 38:2019-35
Erdmann, Natalie; Harrington, Lea A (2009) No attenuation of the ATM-dependent DNA damage response in murine telomerase-deficient cells. DNA Repair (Amst) 8:347-53
Meznikova, Marie; Erdmann, Natalie; Allsopp, Rich et al. (2009) Telomerase reverse transcriptase-dependent telomere equilibration mitigates tissue dysfunction in mTert heterozygotes. Dis Model Mech 2:620-6
Attwooll, Claire L; Akpinar, Müge; Petrini, John H J (2009) The mre11 complex and the response to dysfunctional telomeres. Mol Cell Biol 29:5540-51
Lebel, Catherine; Rosonina, Emanuel; Sealey, David C F et al. (2009) Telomere maintenance and survival in saccharomyces cerevisiae in the absence of telomerase and RAD52. Genetics 182:671-84
Tona, L; Ng, Y C; Akera, T et al. (1990) Depressant effects of chloroquine on the isolated guinea-pig heart. Eur J Pharmacol 178:293-301
Ye, Y X; Bombick, D; Hirst, K et al. (1990) The modulation of gap junctional communication by gossypol in various mammalian cell lines in vitro. Fundam Appl Toxicol 14:817-32
Ng, Y C; Yao, A Z; Akera, T (1989) Tissue-specific isoform regulation of Na+-K+-ATPase by thyroid hormone in ferrets. Am J Physiol 257:H534-9
Stemmer, P; Akera, T; Brody, T M et al. (1989) Isolation and enrichment of Ca2+-tolerant myocytes for biochemical experiments from guinea-pig heart. Life Sci 44:1231-7

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