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Literature DB >> 6832198

Acute effects of alinidine on heart rate and blood pressure in healthy subjects and patients with hyperkinetic heart syndrome.

B Stanek, W Reiterer, P Placheta, G Raberger.

Abstract

The effects of a single dose of alinidine (0.5 mg/kg i.v.), the N-allyl-derivative of clonidine, on heart rate and blood pressure were investigated in healthy volunteers and in patients with hyperkinetic heart syndrome, at rest and during bicycle exercise. In healthy volunteers plasma catecholamine levels were also determined. Alinidine did not change heart rate at rest in the healthy volunteers but it did significantly reduce exercise-induced tachycardia, whereas blood pressure and plasma catecholamine levels were not significantly affected by alinidine, either at rest or during exercise. In patients with hyperkinetic heart syndrome, alinidine reduced heart rate at rest and during exercise to a similar extent as propranolol (0.1 mg/kg i.v.). The blood pressure did not change with alinidine but it was significantly reduced by propranolol. The observation that an alinidine-induced reduction of heart rate occurs without a concomitant fall in blood pressure, and without a clonidine-like symphatho-inhibitory action, is in line with experimental findings suggesting a specific bradycardic action of alinidine under short-term conditions.

Entities: Chemical Disease Species

Mesh：

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Year: 1983 PMID： 6832198 DOI： 10.1007/bf00613923

Source DB: PubMed Journal: Eur J Clin Pharmacol ISSN： 0031-6970 Impact factor: 2.953

13 in total

1. Use of plasma norepinephrine for evaluation of sympathetic neuronal function in man.

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Journal: Eur J Clin Pharmacol Date: 1975-10-10 Impact factor: 2.953

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Authors: E Haber; T Koerner; L B Page; B Kliman; A Purnode
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Authors: N J Christensen; O Brandsborg
Journal: Eur J Clin Invest Date: 1973-07 Impact factor: 4.686

5. Cardiovascular actions of N-allyl-clonidine (ST 567), a substance with specific bradycardic action.

Authors: W Kobinger; C Lillie; L Pichler
Journal: Eur J Pharmacol Date: 1979-09-15 Impact factor: 4.432

6. Evaluation of physical performance by rectangular-triangular bicycle ergometry and computer-assisted ergospirometry.

Authors: W Reiterer
Journal: Basic Res Cardiol Date: 1976 Sep-Oct Impact factor: 17.165

7. Suppression of plasma catecholamines and flushing by clonidine in man.

Authors: S A Metz; J B Halter; D Porte; R P Robertson
Journal: J Clin Endocrinol Metab Date: 1978-01 Impact factor: 5.958

8. Relative roles of heart rate and ventricular stroke volume for the regulation of cardiac output during controlled hypotension with sodium nitroprusside in man.

Authors: M Zimpfer; S Fitzal; M Semsroth
Journal: Eur J Clin Invest Date: 1982-02 Impact factor: 4.686

Acute effects of alinidine on heart rate and blood pressure in healthy subjects and patients with hyperkinetic heart syndrome.

1. Use of plasma norepinephrine for evaluation of sympathetic neuronal function in man.

2. Long term treatment of moderate hypertension with penbutolol (Hoe 893d). I. Effects on blood pressure, pulse rate, catecholamines in blood and urine, plasma renin activity and urinary aldosterone under basal conditions and following exercise.

3. Application of a radioimmunoassay for angiotensin I to the physiologic measurements of plasma renin activity in normal human subjects.

4. The relationship between plasma catecholamine concentration and pulse rate during exercise and standing.

5. Cardiovascular actions of N-allyl-clonidine (ST 567), a substance with specific bradycardic action.

6. Evaluation of physical performance by rectangular-triangular bicycle ergometry and computer-assisted ergospirometry.

7. Suppression of plasma catecholamines and flushing by clonidine in man.

8. Relative roles of heart rate and ventricular stroke volume for the regulation of cardiac output during controlled hypotension with sodium nitroprusside in man.

9. Haemodynamic and electrophysiologic actions of alinidine in the dog.

10. Alinidine reduces heart-rate without blockade of beta-adrenoceptors.

1. [Treatment of hyperkinetic heart syndrome with alinidine and propranolol].

2. Effect of indoramin, labetalol and alinidine on sympathetic function in normal man.