Your search keyword '"Rodríguez-Sasiaín JM"' showing total 20 results

1. Influence of changes in protein binding on the central activity of antidepressants

Author

Rodríguez-Sasiaín Jm, R Calvo, Elena Suarez, E Gomez, I Torres, and E. Garcia

Subjects

Male, Turpentine, Ratón, Analgesic, Central nervous system, Pharmaceutical Science, Orosomucoid, Inflammation, Mianserin, Pharmacology, Tritium, Mice, Pharmacokinetics, medicine, Animals, Pain Measurement, Dose-Response Relationship, Drug, biology, business.industry, Brain, Nociception, medicine.anatomical_structure, biology.protein, medicine.symptom, business, Protein Binding, medicine.drug

Abstract

The central effect (expressed as analgesic response), protein binding and brain uptake of mianserin were measured in mice receiving drug intraperitoneally. A significant decrease of the central effect of mianserin (30 mg kg−1) was seen in mice with experimental inflammation when compared with control animals (reaction time (s)= 12·12 ± 1·22 vs 25·56 ± 2·92; P < 0·001) and the dose-analgesia response curve (10−60 mg kg−1) was significantly shifted to the right in mice with inflammation. In serum of mice with inflammation, unbound concentration of mianserin was decreased from 19·37 ± 0·73 to 17·83 ± 0·30% (P < 0·05) and seromucoid levels were significantly increased (P < 0·001). Following the intraperitoneal administration of 30 mg kg−1 of mianserin, brain uptake decreased in diseased mice when compared with control animals (P < 0·02), suggesting that the decrease in analgesia was secondary to a decrease in drug delivery to the brain because of increased protein binding.

Published

1992

2. Differential effect of cancer on the serum protein binding to mianserin and imipramine

Author

Rosario Calvo, Elena Suarez, I Torres, Rodríguez-Sasiaín Jm, and Carmelo Aguirre

Subjects

Adult, medicine.medical_specialty, Imipramine, Adolescent, Clinical chemistry, Analgesic, Alpha (ethology), Plasma protein binding, Mianserin, Antidepressive Agents, Tricyclic, Internal medicine, Neoplasms, medicine, Humans, Pharmacology (medical), Serum Albumin, Pharmacology, Chemistry, Albumin, Cancer, Blood Proteins, Orosomucoid, Middle Aged, medicine.disease, Endocrinology, Regression Analysis, medicine.drug, Protein Binding

Abstract

Protein binding of mianserin and imipramine in vitro was determined in sera from 10 patients with cancer and from 28 drug-free normal subjects. alpha 1-acid glycoprotein (AAG) concentrations ranged from 0.91 +/- 0.04 g/l in control subjects to 2.17 +/- 0.18 g/l in cancer patients. Albumin concentrations ranged from 55.80 +/- 1.68 g/l in control subjects to 39.71 +/- 4.40 g/l, respectively. Serum samples containing concentrations of 100 ng/ml for mianserin and 500 ng/ml for imipramine were ultrafiltered and the free concentration were measured with scintillation spectrophotometer. The mean free percentage of mianserin was significantly less in patients with cancer (8.70 +/- 0.29% in patients vs 14.30 +/- 0.50% in control subjects P < 0.001). A multiple regression analysis revealed a significant contribution of plasma AAG (r2 = 0.56, P < 0.01), but not of albumin to the overall variability in mianserin binding. No correlation was observed between protein binding of imipramine and AAG concentrations in serum of cancer patients. No significant changes were observed for protein binding of imipramine in cancer patients as compared with control subjects. Our results suggest that for antidepressant (AD) drugs, of which the binding depends on AAG, variability in protein binding could be expected in cancer patients. Thus, in cancer therapy, changes in analgesic doses could be necessary with this kind of antidepressant drug.

Published

1995

3. Effect of sodium valproate on midazolam distribution

Author

R Calvo, Rodríguez-Sasiaín Jm, Elena Suarez, and L Aguilera

Subjects

Adult, Male, medicine.medical_specialty, medicine.drug_class, Midazolam, medicine.medical_treatment, Sodium, Pharmaceutical Science, chemistry.chemical_element, In Vitro Techniques, Pharmacology, Pharmacokinetics, Internal medicine, Blood plasma, medicine, Animals, Humans, Tissue Distribution, Brain Chemistry, Benzodiazepine, Chemistry, Valproic Acid, Blood Proteins, Middle Aged, Drug interaction, Endocrinology, Anticonvulsant, Free fraction, Female, Rabbits, Protein Binding, medicine.drug

Abstract

The displacement of midazolam, a new water-soluble, short-acting benzodiazepine, from its plasma binding sites by sodium valproate, has been studied in man. An increase of its free fraction (ranging from 2.71 to 5.35%) in plasma from epileptic patients receiving sodium valproate was observed. A similar situation was created in rabbits by pretreatment with sodium valproate (600 mg kg−1 day−1) and posterior hypnosis with midazolam. Due to the interaction, sodium valproate-pretreated rabbits showed an increase in midazolam brain levels (130.91 μg g−1 in cortex vs 84.55 μg g−1 in control animals). Therefore, it seems likely that displacement of midazolam by sodium valproate in epileptic patients could lead to an increase of the midazolam response.

Published

1988

4. Plasma protein binding of penbutolol in pregnancy

Author

R. Calvo, P. Navajas, Rodríguez-Sasiaín Jm, and C. Aquirre

Subjects

Adult, medicine.medical_specialty, Clinical chemistry, Contraceptives, Oral, Hormonal, Propanolamines, Pharmacokinetics, Penbutolol, Pregnancy, Internal medicine, Medicine, Humans, Pharmacology (medical), Drug Interactions, Volunteer, Serum Albumin, Pharmacology, business.industry, Albumin, Blood Proteins, Orosomucoid, medicine.disease, Endocrinology, Free fraction, Gestation, Female, business, medicine.drug

Abstract

Penbutolol is a not cardioselective beta-adrenergic blocking drug; it is lipid soluble and differs in its protein binding from the other members of its group because shows linkage to alpha 1-glycoprotein, with no detectable binding to albumin. AAG levels change during pregnancy and so the binding of [3H]-penbutolol was compared in 11 pregnant patients and in 10 healthy women. Binding was obtained by ultrafiltration and measurement of the free fraction by scintillation spectrometry. The free penbutolol fraction was significantly higher in the pregnant women than in the controls (6.06 +/- 0.34 compared with 3.55 +/- 0.29, P less than 0.001). The AAG levels in the pregnant women were significantly lower (0.40 +/- 0.03 g/l) than in the controls (0.77 +/- 0.06 g/l) (P less than 0.001) which showed a significant correlation with the bound/free penbutolol ratio (r = 0.61, P less than 0.005). On the other hand there was no significant correlation with the extent of penbutolol's protein binding even though the albumin levels were lower in the pregnant women (2.83 +/- 0.17 compared with 4.86 +/- 0.17; P less than 0.001). Penbutolol's nK1a for AAG was lower in pregnant women, and this suggests that the fall in AAG levels is not the only factor involved in the reduced binding of penbutolol in pregnancy.

Published

1988

5. A cost-analysis of suspected adverse drug reactions in a hospital emergency ward.

Author

Ayani I, Aguirre C, Gutiérrez G, Madariaga A, Rodríguez-Sasiaín JM, and Martínez-Bengoechea MJ

Abstract

The main objective of this study was to analyse the minimum direct cost to the Public Health System (PHS) of diagnosing and treating those patients attended to in the emergency ward (EW) for suspected adverse drug reaction (ADR). The cases were collected during March 1995 in the emergency ward of a 900-bed tertiary teaching hospital that covers 900,000 inhabitants. ADR was considered according to the WHO definition. The following EW costs were used: EW physician visit 78.5 ecus (1 ecu=156 pesetas), thorax or abdomen radiograph 21.5 ecus, computerized tomography 112.7 ecus, endoscopy 48 ecus, specialist physician visit 62 ecus. Three types of laboratory costs were considered: block of biochemical tests 16 ecus, biochemical tests with blood count 22.5 ecus, and biochemical tests with blood count and coagulation study 41.6 ecus. Pharmacotherapy of the ADR and changes in patient's usual drug therapy due to ADR were estimated. For patients admitted in the hospital, a per day cost of 391 ecus was considered. A mean ADR cost per organ or system affected (cutaneous, metabolic, gastrointestinal, nervous) was computed. The main conclusion of this study is that ADR, apart from inflicting damage on the patients, also incur PHS costs. The quantity of 42,732 ecus during the month of March, in a single hospital, can seem small when compared with the cost of some diseases such as AIDS or ischemic heart disease. But remembering that about 40% of all ADR attended to in hospitals is avoidable, a decrease of 40% could produce an annual saving of 205,216 ecus to the hospital, which is twice the annual budget of the Pharmacovigilance Centre of the Basque Country. Pharmacovigilance centres should include cost analysis of ADR among their objectives, to provide health systems managers with enough information to implement those measures that will result in a better utilization of the scarce resources of the Public Health System., (Copyright 1999 John Wiley & Sons, Ltd.)

Published

1999

6. The effect of changes in gastric pH induced by omeprazole on the absorption and respiratory depression of methadone.

Author

de Castro J, Aguirre C, Rodríguez-Sasiaín JM, Gómez E, Garrido MJ, and Calvo R

Subjects

Administration, Oral, Animals, Area Under Curve, Drug Interactions, Female, Gastric Mucosa drug effects, Hydrogen-Ion Concentration drug effects, Intestinal Absorption drug effects, Methadone blood, Methadone pharmacology, Omeprazole administration & dosage, Pulmonary Gas Exchange, Rats, Rats, Sprague-Dawley, Respiration drug effects, Sodium Bicarbonate pharmacology, Methadone pharmacokinetics, Omeprazole pharmacology, Respiratory Insufficiency chemically induced

Abstract

The effect of omeprazole (2 mg kg-1 i.v.) on respiratory depression induced in rats by acute oral methadone administration (5 mg kg-1) was examined and compared with control animals that only received methadone. Quantitative assessments of arterial Pco2,Po2, pH, and respiratory rate were employed as criteria for evaluation. Intragastric pH was measured in each rat immediately before and 2 h after methadone. Plasma concentration of methadone was measured for 3 h. The relationship between drug effect and the systemic bioavailability of methadone, measured as the area under the plasma concentration-time curve (AUC0-180), was also evaluated. The intensity of the methadone-induced respiratory depression was significantly greater in the omeprazole group than in control rats. A significant variation (p < 0.01) in all respiratory parameters was detected from 30 to 120 min after methadone. Omeprazole caused a significant increase in methadone levels (Cmax = 156 +/- 6.5 ng mL-1 against 51 +/- 5.8 ng mL-1 in control; p < 0.05). AUC0-180 was higher (p < 0.05) after omeprazole treatment (18.6 +/- 1.4 micrograms mL-1 min) than in control (6.8 +/- 0.6 microgram mL-1 min). Two hours after treatment with omeprazole, intragastric pH values were significantly elevated (4.7 +/- 0.1 against 2.2 +/- 0.04) and continued increasing, being 6.4 +/- 0.1 at the end of the experiment. Correlation was observed between intragastric pH and the area under the effect- (respiratory depression-) time curve (r = 0.74; p < 0.001). A relationship between plasma methadone levels at 120 min and gastric pH (r = 0.92; p < 0.001) was detected. A significant correlation between the area under the effect-time curve (0-120 min) and AUC0-180 has been also observed (r = 0.90; p < 0.01). These pharmacokinetic and pharmacodynamic changes could be gastric pH dependent because they were mimicked when gastric pH was experimentally modified by bicarbonate whereas opposite results were obtained with acidic pH2 solution.

Published

1996

7. Characteristics of serum protein binding of felodipine.

Author

Valle M, Esteban M, Rodríguez-Sasiaín JM, Calvo R, and Aguirre C

Subjects

Adult, Age Factors, Aged, Chronic Disease, Diabetes Mellitus, Type 1 blood, Diabetes Mellitus, Type 2 blood, Female, Humans, Kidney Diseases blood, Liver Cirrhosis blood, Male, Middle Aged, Neoplasms blood, Orosomucoid metabolism, Protein Binding, Serum Albumin metabolism, Antihypertensive Agents blood, Blood Proteins metabolism, Calcium Channel Blockers blood, Felodipine blood

Abstract

The protein binding of felodipine in concentrations ranging from 3 to 65 nmol L-1 has been characterized in pooled serum, and in isolated human plasma proteins: albumin (HSA) and a1-acid glycoprotein (AAG). Protein binding was determined by an ultrafiltration technique using an Amicon Micropartition System. Serum protein binding of felodipine (16 nmol L-1) was measured in five groups of individuals: I: healthy subjects (n = 16). II: patients with chronic renal disease before and after dialysis (n = 10). III: patients with liver disease (n = 9). IV: diabetics Type I (n = 10) and Type II (n = 12) and V: cancer patients (n = 12). Concentrations of HSA, AAG, lipoproteins and non esterified fatty acids (NEFA) were also measured. The drug was extensively bound in pooled serum and the protein binding was essentially unchanged over the concentrations of felodipine studied (99.60 +/- 0.31% at 3 nmol L-1; 99.70 +/- 0.15% at 65 nmol L-1). In albumin solution (40 g L-1) felodipine was also highly bound. The mean of percentage bound was not significantly different from that in serum and was also independent of the felodipine concentrations (98.57 +/- 0.35 at 3 nmol L-1; 98.31 +/- 0.90 at 65 nmol L-1). The extent of binding to AAG was significantly lower than in serum (p < 0.01) and HSA (p < 0.01) and was independent of felodipine concentrations (85.64 +/- 2.25 at 3 nmol L-1; 85.68 +/- 2.3 at 65 nmol L-1). The percentage of bound felodipine in group II (before dialysis) was significantly lower than in group I (p < 0.001). The variability in the percentage of bound felodipine was greater in group II, before dialysis, than in the rest of the groups. After dialysis, protein binding was similar to that in group I. HSA did not change and AAG was increased. NEFA was significantly higher after dialysis when compared with group I (p < 0.01). In vitro carbamylation of serum did not change felodipine protein binding. HSA was decreased significantly in group III patients (p < 0.05). However, protein binding did not change. Binding of felodipine in the rest of the groups was not significantly different from that in group I. Linear regression analysis of the data for all individuals indicated that the binding of felodipine was related to serum lipoproteins and that age, HSA, AAG, and NEFA were not significant determinants of binding.

Published

1996

8. Pharmacokinetics and pharmacodynamics of penbutolol in healthy and cancer subjects: role of altered protein binding.

Author

Aguirre C, Trocóniz IF, Valdivieso A, Jiménez RM, González JP, Calvo R, and Rodríguez-Sasiaín JM

Subjects

Adult, Aged, Binding, Competitive, Humans, Male, Middle Aged, Gastrointestinal Neoplasms metabolism, Penbutolol pharmacokinetics, Penbutolol pharmacology, Protein Binding physiology

Abstract

The pharmacokinetic and pharmacodynamic profiles of penbutolol were examined in healthy volunteers and in cancer patients using a pharmacokinetic/pharmacodynamic (pk/pd) model. After receiving a 40 mg single oral dose of penbutolol, the absorption rate constant, apparent volume of distribution and serum clearance of penbutolol were found to be reduced in the cancer group. Changes in the disposition of the conjugate metabolite were also observed in the cancer patients. Penbutolol unbound fraction in serum was statistically decreased (p < 0.005) in the cancer group, according to the increase in the serum levels of alpha 1-acid glycoprotein seen in that group (p < 0.05). The pharmacodynamic effect of penbutolol was measured as the reduction in heart rate (HR); in healthy volunteers, a linear relationship (p < 0.01) between effect and penbutolol serum concentrations (total or unbound) was found. In contrast, in cancer patients, values of HR did not vary statistically in respect to baseline values. These results show that in cancer patients, a change in the pharmacokinetics of penbutolol occurs (associated with changes in drug protein binding), together with an alteration in the pharmacodynamics.

Published

1996

9. Resistance to atracurium in rats with experimental inflammation: role of protein binding.

Author

García E, Calvo R, Rodríguez-Sasiaín JM, Jiménez R, Trocóniz IF, and Suárez E

Subjects

Animals, Atracurium metabolism, Dose-Response Relationship, Drug, Drug Resistance, Inflammation metabolism, Male, Protein Binding, Rats, Rats, Sprague-Dawley, Atracurium pharmacology, Neuromuscular Nondepolarizing Agents pharmacology

Abstract

The influence of altered protein binding on the neuromuscular effect of atracurium has been studied in rats with experimental inflammation induced by subcutaneous injection of turpentine oil. Doses of atracurium ranging from 0.45 to 1.5 mg.kg-1 were administered to control (n = 30) and to experimental inflammation induced rats (n = 30). Neuromuscular transmission was monitored by recording the twitch tension of the tibialis-anterior muscle elicited by stimulation of the sciatic nerve. Three effect parameters were recorded: (i) intensity of the effect, measured as percentage depression of baseline twitch tension, (ii) duration of drug action (min) and (iii) recovery time (min). The dose-intensity of the effect relationship was modelled using a sigmoid Emax model. The ED50 (effective dose eliciting 50% of the maximum effect) was significantly increased (P < 0.01) in the inflammation group as compared to the control group (0.94 vs. 0.68 mg.kg-1). This change was reflected in a shift of the dose-response curve to the right in the pretreated rats. For equipotent doses ED95 (defined as the effective dose eliciting 95% of maximum effect), no differences were found in recovery time and duration of action between the two groups of rats. Mucoproteins levels (index of alpha 1-acid glycoprotein (AAG) and protein binding were significantly increased in rats with experimental inflammation as compared to control rats. Based on these results, altered serum protein binding of atracurium appears to be responsible, at least in part, for the resistance to atracurium.

Published

1995

10. Changes in the analgesic effects of mianserin associated with altered plasma protein binding in experimental cancer.

Author

Torres I, Suárez E, Rodríguez-Sasiaín JM, Gomez E, and Calvo R

Subjects

Animals, Binding, Competitive, Dose-Response Relationship, Drug, Glycoproteins blood, In Vitro Techniques, Mice, Mice, Inbred C57BL, Mucoproteins blood, Neoplasms, Experimental, Analgesics pharmacology, Blood Proteins drug effects, Brain metabolism, Mianserin pharmacology

Abstract

In a group of mice bearing experimentally induced tumors, the protein binding of mianserin in vitro was measured and compared with a control group. The analgesic effect and the brain uptake of drug was also compared with a control group after an intraperitoneal dose of mianserin. The unbound percentage of mianserin in the plasma of mice with experimental cancer decreased with respect to control animals (5.20 +/- 0.12 vs 6.06 +/- 0.26; p<0.05) and alpha1-acid glycoprotein (AAG) levels, measured as plasma mucoprotein concentrations, were significantly increased (p<0.05). The brain/plasma drug concentration ratio of mianserin decreased in mice with experimental cancer when compared with control mice (1.11 +/- 0.03 vs 1.42 +/- 0.10; p<0.02). In both groups of mice, the mianserin analgesic effect was evaluated by the hot plate test after intraperitoneal drug administration. When the analgesia response-dose curve (0-60 mg/kg) was studied, a significant decrease in the response in mice with experimental cancer versus control mice was observed. These results suggest that resistance to the mianserin analgesic response may occur in animals with cancer disease. This resistance may be associated, in part, with an altered plasma protein binding, but other mechanisms could be involved.

Published

1995

11. Influence of vitamin C on the absorption and first pass metabolism of propranolol.

Author

Gonzalez JP, Valdivieso A, Calvo R, Rodríguez-Sasiaín JM, Jimenez R, Aguirre C, and du Souich P

Subjects

Administration, Oral, Adult, Female, Humans, Male, Pharmacokinetics, Time Factors, Volunteers, Ascorbic Acid pharmacology, Biological Availability, Drug Interactions, Propranolol metabolism

Abstract

The effect of ascorbic acid on the availability of propranolol has been examined. After oral administration of propranolol 80 mg with or without ascorbic acid pretreatment (2 g), the plasma concentrations and urinary excretion of propranolol and its metabolites, 4-hydroxy-propranolol and propranolol-conjugated, were determined by HPLC. Compared to controls, vitamin C decreased the maximum concentration of propranolol from 463 to 334 nmol.l-1, and the area under the propranolol concentration-time curve (from 0 to 24 hours) from 3.13 to 1.96 mumol.l-1.h. The time to reach maximum propranolol concentration was increased from 1.9 to 2.7. The total amount of drug recovered in urine has also significantly diminished (from 12.6 to 4.29 mg). No change in elimination rate was observed, indicating that ascorbic acid had affected both the absorption process and the first pass metabolism. The heart-rate decreased less when propranolol was administered with ascorbic acid in comparison to control subjects, although this interaction has little biological importance.

Published

1995

12. [Characterization of propofol binding to plasma proteins and possible interactions].

Author

Garrido MJ, Jiménez RM, Rodríguez-Sasiaín JM, Aguirre C, Aguilera L, and Calvo R

Subjects

Drug Interactions, Humans, Orosomucoid metabolism, Pharmaceutical Preparations metabolism, Propofol blood, Protein Binding, Serum Albumin metabolism, Blood Proteins metabolism, Propofol pharmacokinetics

Abstract

Objectives: a) To study the binding of propofol to proteins in plasma samples from healthy volunteers and in solutions of albumin and alpha 1-acid glycoprotein (AGA); b) to describe the nature of the bond and possible interactions with other substances that are potential displacers: salicylate, phenylbutazone, sulfisoxazole, tolbutamide, sodium valproate, sodium oleate and penbutolol; c) to assess the effect of propofol on the binding of specific markers and possible binding sites in the following proteins: 14C-warfarin, 3H-diazepam, 3H-midazolam, 3H-imidazole, 3H-penbutolol and 3H-morphine., Material and Methods: The free fraction was obtained in all samples by ultrafiltration and measurement of the free concentration of propofol by liquid chromatography and of the markers by scintillation spectrometry., Results: The free fraction of propofol in plasma was 0.98 +/- 0.12% and binding was not saturable. Albumin seems to play an important role (95% bound), whereas the participation of AGA was low (54% bound). Propofol did not affect the binding of any of the markers studied. Nor did the presence of other drugs at therapeutic plasma concentrations affect the binding of propofol., Conclusions: The binding of propofol to plasma proteins seems unlikely to cause drug interactions in clinical practice.

Published

1994

13. Influence of halothane anaesthesia on protein binding of drugs.

Author

Calvo R, Suárez E, Aguilera L, and Rodríguez Sasiaín JM

Subjects

Drug Interactions, Humans, Warfarin blood, Anesthesia, Inhalation adverse effects, Halothane adverse effects, Protein Binding drug effects

Published

1994

14. In vivo potentiation of atracurium neuromuscular blockade by nimodipine in rabbits.

Author

Gómez-Iglesias E, García E, Suarez E, Martínez R, Rodríguez-Sasiaín JM, and Calvo R

Subjects

Animals, Atracurium administration & dosage, Dose-Response Relationship, Drug, Drug Interactions, Drug Synergism, Muscle Contraction drug effects, Muscles drug effects, Muscles innervation, Neuromuscular Blocking Agents administration & dosage, Neuromuscular Junction drug effects, Nimodipine administration & dosage, Rabbits, Sciatic Nerve drug effects, Synaptic Transmission drug effects, Time Factors, Atracurium pharmacology, Neuromuscular Blocking Agents pharmacology, Nimodipine pharmacology

Abstract

The interaction between nimodipine, a calcium channel blocker, used for the treatment of subarachnoid haemorrhage, and atracurium, was studied in rabbits. An intravenous dose of 0.1 mg.kg-1 of nimodipine given over 3 min caused a potentiation of the neuromuscular blocking action of atracurium (administered at an infusion rate of 7.5 micrograms.kg-1.min-1), measured on the indirectly stimulated tibialis-anterior muscle of the animal. (ED50)inf and (ED95)inf were significantly reduced (30.7% and 23.3%) in nimodipine-treated animals (P less than 0.05 and P less than 0.02, respectively). No changes were observed in recovery rate.

Published

1992

15. Effect of halothane anesthesia and trifluoroacetic acid on protein binding of benzodiazepines.

Author

Suárez E, Aguilera L, Calvo R, Rodríguez-Sasiaín JM, and Martínez-Jorda R

Subjects

Adult, Anesthesia, Inhalation, Binding, Competitive, Diazepam blood, Drug Interactions, Humans, Midazolam blood, Middle Aged, Preanesthetic Medication, Protein Binding drug effects, Trifluoroacetic Acid blood, Diazepam metabolism, Halothane pharmacology, Lorazepam metabolism, Midazolam metabolism, Trifluoroacetic Acid pharmacology

Abstract

The in vitro effect of the halothane metabolite, trifluoroacetic acid, on the protein binding of three different benzodiazepines (diazepam, lorazepam and midazolam) has been investigated. Furthermore, protein binding of these drugs was studied in serum from patients under the effect of halothane anesthesia (1-2.5%; 2.5 h). Trifluoroacetic acid, 4 mmol/l, displaced diazepam and midazolam from serum and produced a marked increase in the free percentage, but did not influence lorazepam binding. Moreover, 48 h after the end of halothane anesthesia, there were changes in protein binding of diazepam (3.9 +/- 0.3% at 48 h vs. 3.3 +/- 0.3% before halothane anesthesia; p less than 0.05). It can be concluded that halothane anesthesia (1-2.5%; 2.5 h) may temporarily potentiate the pharmacological effect of diazepam in the postoperative period following anesthetic procedures.

Published

1991

16. [Influence of verapamil and diltiazem on the muscle-relaxing effect of atracurium in vivo].

Author

Gómez Iglesias E, García Pascual E, Aguirre Gómez C, Rodríguez-Sasiaín JM, and Calvo Duo R

Subjects

Animals, Atracurium administration & dosage, Diltiazem administration & dosage, Dose-Response Relationship, Drug, Drug Interactions, Muscle Relaxation drug effects, Rabbits, Receptors, Nicotinic drug effects, Synaptic Transmission drug effects, Verapamil administration & dosage, Atracurium pharmacology, Diltiazem pharmacology, Neuromuscular Junction drug effects, Verapamil pharmacology

Abstract

The interaction between atracurium and the two calcium antagonists verapamil and diltiazem were studied in rabbits. It was observed that intravenous verapamil (0.2 mg/kg) reduced by 25% and 30% respectively, the dose of atracurium required to produce a 50% or 95% of neuromuscular blockade. In contrast, intravenous diltiazem (1 mg/kg) failed to produce significant changes.

Published

1991

17. Decrease in penbutolol central response as a cause of changes in its serum protein binding.

Author

Martínez Jordá R, Aguirre C, Calvo R, Rodríguez-Sasiaín JM, and Erill S

Subjects

Animals, Blood Proteins metabolism, Brain metabolism, Dose-Response Relationship, Drug, Electroshock, Inflammation metabolism, Injections, Intravenous, Male, Mice, Orosomucoid analysis, Penbutolol blood, Penbutolol pharmacokinetics, Protein Binding, Seizures prevention & control, Serum Albumin metabolism, Penbutolol pharmacology, Propanolamines pharmacology

Abstract

Penbutolol is a beta-adrenoceptor antagonist that is extensively bound to alpha 1-acid glycoprotein (alpha 1-AGP), a protein that increases in inflammatory diseases thereby binding more drug in such conditions. Changes in serum binding can lead to modifications in the pharmacokinetics and pharmacodynamics of a drug, therefore, the central effect (as the anticonvulsant response) and brain uptake of penbutolol given intravenously to mice with experimental inflammation have been measured. A significant decrease of the central effect of penbutolol and its brain uptake was seen in diseased when compared with control animals (P less than 0.01). A parallel decrease in free fraction of penbutolol in diseased vs normal animals was detected. These results suggest that there is an increase in serum binding of basic drugs related to increments in alpha 1-AGP concentration, which reduces their central pharmacological effect.

Published

1990

18. A study of package inserts of potentially toxic drugs.

Author

Rodríguez-Sasiaín JM and Erill S

Subjects

Humans, Drug Labeling, Drug-Related Side Effects and Adverse Reactions

Abstract

Information contained in the package inserts of drugs chosen as potential causes of blood dyscrasia, renal toxicity, hepatotoxicity, and cardiac toxicity has been studied. Chloramphenicol and pyrazolones were chosen as representatives of drugs that could produce blood dyscrasia, aminoglycosides and cephaloridine as potential nephrotoxic agents, isoniazid and monoamine oxidase inhibitors as possible hepatotoxic drugs, and tricyclic antidepressants and digitalis as drugs of recognized cardiac toxicity. Adverse effects were clearly described in only 27.8% of the package inserts, whereas 40.3% did not mention them, and 15.7% specifically stated that the product was devoid of adverse effects. Information about the type of toxicity that led to the selection of drugs included in this study was uncommon in most cases.

Published

1982

19. Serum protein binding of penbutolol in patients with hepatic cirrhosis.

Author

Aguirre C, Calvo R, and Rodríguez Sasiaín JM

Subjects

Adult, Aged, Female, Humans, Male, Middle Aged, Protein Binding, Blood Proteins metabolism, Liver Cirrhosis metabolism, Penbutolol metabolism, Propanolamines metabolism

Abstract

Serum protein binding of penbutolol, a non-cardioselective beta-blocker agent of basic nature, has been studied in healthy subjects and in patients with hepatic cirrhosis. The percentage of free penbutolol in serum containing 200 ng/ml was markedly increased in patients with hepatic cirrhosis, when compared with the group of healthy volunteers (8.17 +/- 1.13% in patients vs 3.41 +/- 0.19 in control). No significant differences in the levels of serum alpha-acid-glycoprotein (the major protein implicated in the serum binding of penbutolol) were detected. Differences in the overall affinity constant for the binding were apparent between both groups (nKa = 5.28 X 10(5) M-1 in patients vs 12.03 X 10(5) M-1 in healthy volunteers). These results suggest a qualitative change in alpha-acid-glycoprotein molecule, from hepatic patients, but further studies are needed to clarify this point.

Published

1988

20. Effect of heparin administration on flunitrazepam protein binding.

Author

Calvo R, Aguilera L, Aguirre C, and Rodríguez Sasiaín JM

Subjects

Adult, Female, Humans, In Vitro Techniques, Male, Protein Binding drug effects, Flunitrazepam metabolism, Heparin pharmacology

Abstract

Non-esterified fatty acids have been shown to displace diazepam from its plasma binding sites both in vitro and in vivo. However, the binding of other benzodiazepines such as lorazepam is not affected in similar situations. Flunitrazepam exhibits a substantial degree of binding to plasma proteins, therefore it was deemed interesting to investigate the role of free fatty acids on flunitrazepam binding to human plasma proteins. Incubation of plasma with sodium oleate (1.5 and 3.0 microEq per ml) produced a decrease in the binding of flunitrazepam. The free fraction increased from 4.20 +/- 0.34 to 6.30 +/- 0.53 and to 22.18 +/- 1.28% respectively). Sodium heparin administration (10IU/kg, intravenously) increased free fatty acids levels and produced similar changes in the binding of flunitrazepam. After ten minutes of heparin administration free fatty acids increased from 0.16 +/- 0.03 mEq/l to 0.34 +/- 0.01 mEq/l and the free fraction of flunitrazepam in plasma increased from 3.70 +/- 0.22% to 6.20 +/- 1.24%. These binding data further support a relationship between increases in the concentrations of free fatty acids and decreases in the fraction of flunitrazepam bound to plasma proteins.

Published

1989