Journal ArticleDOI
Pharmacokinetics and concentration‐effect relationships of intravenous and oral clonidine
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TLDR
Oral and intravenous clonidine induced significant falls in blood pressure and consistently caused marked sedation and dryness of the mouth and it is proposed that a two‐compartment model adequately describes the disposition of the drug.Abstract:
The kinetics of the disposition of intravenous and oral clonidine in five normotensive subjects have been determined. It is proposed that a two-compartment model adequately describes the disposition of the drug. The drug is rapidly distributed (t1/2alpha = 10.8 +/- 4.7 min) but slowly elimainated (t1/2beta = 8.5 +/- 0.9 hr). The bioavailability of oral clonidine in the tablets tested averaged 75.2% and 40 to 50% of the bioavailable dose is excreted unchanged in urine. Renal clearance of the drug showed considerable intersubject variation (1.82 +/- 0.34 ml/min/kg) and exceed the calculated glomerular filtration rate in some subjects. Oral and intravenous clonidine induced significant falls in blood pressure (greater than 20/15 mm Hg) in our normotensive subjects and consistently caused marked sedation and dryness of the mouth. Sedation and salivary flow correlated with plasma clonidine concentration over the range 0 to 4 ng/ml. Falls in blood pressure were related to plasma concentration to 1.5 to 2 ng/ml but at higher concentrations the hypotensive effect was attenuated.read more
Citations
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The effects of increasing plasma concentrations of dexmedetomidine in humans.
TL;DR: In this article, the responses to increasing plasma concentrations of dexmedetomidine in humans were determined, and 10 healthy men (20-27 yr) provided informed consent and were monitored (underwent electrocardiography, measured arterial, central venous [CVP] and pulmonary artery [PAP] pressures,
Journal ArticleDOI
Sedative, amnestic, and analgesic properties of small-dose dexmedetomidine infusions.
TL;DR: Small-dose dexmedetomidine infusions resulted in reversible sedation, mild analgesia, and memory impairment without cardiorespiratory compromise, and these properties might prove useful in a postoperative or intensive care unit setting.
Journal ArticleDOI
Evaluation of human intestinal absorption data and subsequent derivation of a quantitative structure-activity relationship (QSAR) with the Abraham descriptors.
Yuan H. Zhao,Joelle Le,Michael H. Abraham,Anne Hersey,Peter J. Eddershaw,Chris N. Luscombe,Darko Boutina,Gordon Beck,Brad Sherborne,Ian Cooper,James Alexis Platts +10 more
TL;DR: The results show that Abraham descriptors can successfully predict human intestinal absorption if the human absorption data is carefully classified based on solubility and administration dose to humans.
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Prediction of human intestinal absorption of drug compounds from molecular structure.
TL;DR: A nonlinear computational neural network model developed by using the genetic algorithm with a neural network fitness evaluator to estimate percent human intestinal absorption (%HIA) is an attractive alternative to experimental measurements.
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Noradrenergic modulation of cognitive function in rat medial prefrontal cortex as measured by attentional set shifting capability.
M.D.S. Lapiz,David A. Morilak +1 more
TL;DR: Results indicate that elevating noradrenergic activity at alpha1-receptors in medial prefrontal cortex facilitates cognitive performance of rats in an attentional set-shifting task, which may contribute to the role of norepinephrine in behavioral state changes such as arousal, or to the beneficial cognitive effects of psychotherapeutic drugs that target nor adrenergic neurotransmission.
References
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Journal ArticleDOI
New Method for Calculating the Intrinsic Absorption Rate of Drugs
J.C.K. Loo,Sidney Riegelman +1 more
TL;DR: It is shown that methods based on the single-compartment concept do not result in acceptable estimates of the absorption rates, and a new equation is presented, presuming the drug distributes between a central and one peripheral compartment, which results in an accurate estimate of the known rates of infusion (absorption) for the drugs studied to date.
Journal ArticleDOI
Shortcomings in Pharmacokinetic Analysis by Conceiving the Body to Exhibit Properties of a Single Compartment
TL;DR: The two-compartmental open-system model is discussed in respect to the error introduced into the usual absorption rate and elimination rate calculations and on the estimation of the volume of distribution of various drugs.
Journal ArticleDOI
Clinical pharmacology and pharmacokinetics of clonidine.
Colin T. Dollery,Donald S. Davies,G. H. Draffan,H. J. Dargie,C. R. Dean,J. L. Reid,R. A. Clare,Stephen Murray +7 more
TL;DR: A 300‐µg oral dose of clonidine was administered to 5 normal volunteers and measurements of plasma concentration and effects upon blood pressure, heart rate, circulatory reflexes, sedation, and dry mouth were made.
Journal ArticleDOI
Investigations into the mechanism of the hypotensive effect of 2-(2,6-dichlorphenylamino)-2-imidazoline-HCl.
W. Kobinger,A. Walland +1 more
TL;DR: The results are considered to show a speficic inhibitory effect of St 155 on sympathetic cardiovascular centres of the nervous system in dogs anaesthetized with pentobarbital.
Journal ArticleDOI
Localization of the hypotensive effect of 2-(2-6-dichlorophenylamino)-2-imidazoline hydrochloride (St 155, catapresan)
Henri Schmitt,Mme Hélène Schmitt +1 more
TL;DR: The central action of St 155 was confirmed and the medulla oblongata was found to be the main site of this action, and it was suggested that this long latency period was due to the slow passage of the drug from the cerebro spinal fluid into the nervous tissue.