S T Conahan scite author profile

S T Conahan

4Publications

19Citation Statements Received

0Citation Statements Given

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Affiliations

Thomas Jefferson University, Drexel University

Publications

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Changes in Vagal Activity and Response to Muscarinic Receptor Agonists With Age

Kelliher¹,

Conahan

1980

Journal of Gerontology

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The response to vagal nerve and muscarinic receptor stimulation was evaluated in young (90 day), adult (365 day) and old (730 day) male F-344 rats anesthetized with urethane. Bilateral vagotomy produced a significant increase in heart rate in the young and adult animals (p < 0.05), while no change in heart rate occurred in the old animals. Stimulation of the right vagus nerve produced a frequency dependent decrease in response to right vagus nerve stimulation with age (p < 0.05; analysis of variance), i.e., old animals had a smaller decrease in heart rate over the same frequency range of nerve stimulation than either the young or adult animals. The effect of age on the response of the muscarinic receptor was examined using cumulative doses of methacholine administered by bolus injection. Methacholine produced a dose dependent decrease in heart rate and blood pressure. The heart rate response to methacholine was diminished in the older animals (p < 0.05; analysis of variance). Similar results were obtained after atropine although the doses of methacholine employed were much greater. In contrast, although methacholine decreased blood pressure in all animals at each age there was no change in the hypotensive response to methacholine with age. These data indicate that there is a diminution in vagal control of heart rate with age as well as the response of the vagus nerve to stimulation. Furthermore, the response of the muscarinic receptor in the heart declines with age while that in the peripheral vasculature does not.

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Alprazolam decreases isoproterenol induced myocardial damage in the rat

Berkowitz

Conahan

Vogel

1988

Cardiovascular Research

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Myocardial trauma and damage were induced by two doses of isoproterenol 40 mg.kg-1 in rats. Isoproterenol injections alone caused the expected cardiotoxicity. Two doses of alprazolam 0.5 mg.kg-1 decreased the severity of electrocardiographic changes after isoproterenol injection and the amount of myocardial tissue damage. The frequency of ischaemic ST-T changes, flat or inverted T waves, Q wave appearance, and heart block was significantly reduced in the alprazolam group. The alprazolam treated group had a significantly smaller proportion of infarcted tissue in the ventricular section (2.3%) and in the apical sections (1.8%) than the vehicle injected rats (6.5% and 14.7% respectively). There was no difference in wet heart weight or in heart rate between the alprazolam group and the control group. These results show that alprazolam has a cardioprotective effect in rats treated with cardiac damaging doses of isoproterenol.

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Effects of Ethanol and Cocaine on Electrically Triggered Calcium Transients in Cardiac Muscle Cells^a

Thomas

Stewart

Bolton

et al. 1991

Annals of the New York Academy of Sciences

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Effect of decapitation and stress on some plasma electrolyte levels in rats

Conahan

Narayan

Vogel

1985

Pharmacology Biochemistry and Behavior

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S T Conahan

Changes in Vagal Activity and Response to Muscarinic Receptor Agonists With Age

Alprazolam decreases isoproterenol induced myocardial damage in the rat

Effects of Ethanol and Cocaine on Electrically Triggered Calcium Transients in Cardiac Muscle Cells^a

Effect of decapitation and stress on some plasma electrolyte levels in rats

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S T Conahan

Changes in Vagal Activity and Response to Muscarinic Receptor Agonists With Age

Alprazolam decreases isoproterenol induced myocardial damage in the rat

Effects of Ethanol and Cocaine on Electrically Triggered Calcium Transients in Cardiac Muscle Cellsa

Effect of decapitation and stress on some plasma electrolyte levels in rats

Contact Info

Product

Resources

About

Effects of Ethanol and Cocaine on Electrically Triggered Calcium Transients in Cardiac Muscle Cells^a