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1. Contribution of the Gastrointestinal Tract to Lorazepam Conjugation and Clonazepam Nitroreduction

Author

David J. Greenblatt, Hermann R. Ochs, Wolfgang Eichelkraut, Norbert Hahn, James F. Powers, and Barbara W. LeDuc

Subjects
Chromatography, Gas, Swine, medicine.drug_class, Metabolite, Administration, Oral, Pharmacology, Lorazepam, Clonazepam, chemistry.chemical_compound, Pharmacokinetics, Oral administration, medicine, Animals, Biotransformation, Chromatography, High Pressure Liquid, Gastrointestinal tract, Benzodiazepine, business.industry, General Medicine, Nitro Compounds, Bioavailability, Kinetics, chemistry, Injections, Intravenous, business, Digestive System, Oxidation-Reduction, medicine.drug
Abstract

Domestic pigs received single intravenous and oral doses of lorazepam or clonazepam (1 mg/kg), benzodiazepine derivatives biotransformed by glucuronide conjugation and nitroreduction, respectively. Blood samples were simultaneously drawn from portal venous and systemic venous sampling sites during 8 h after dosage. After intravenous dosage with either drug, the area under the serum concentration curve (AUC) for the intact drug, as well as for the principal metabolites (lorazepam glucuronide and 7-aminoclonazepam, respectively), was nearly identical between portal and systemic serum. After oral dosage, absolute systemic availability (relative to intravenous administration) of both lorazepam and clonazepam was incomplete (mean values: 29 and 49%, respectively); however, metabolite levels were also correspondingly lower between oral and intravenous dosages. First-pass hepatic extraction also occurred for both drugs, with mean systemic/portal AUC ratios of 0.60 for lorazepam and 0.74 for clonazepam. Pretreatment with neomycin (1.0 g) had a minimal effect on portal or systemic AUC for intact clonazepam after oral dosage, but 7-aminoclonazepam concentrations were reduced by neomycin pretreatment. Thus incomplete absorption, together with first-pass hepatic biotransformation, appears to explain the incomplete systemic availability of orally administered lorazepam or clonazepam. Biotransformation within the gastrointestinal tract or during absorption through the gastrointestinal mucosa contributes minimally.

Published
1991

2. Automated Electron-Capture Gas Chromatographic Analysis of Flunitrazepam in Plasma

Author

David J. Greenblatt, Hermann R. Ochs, Lauven Pm, and Ann Locniskar

Subjects
Adult, Pharmacology, Chromatography, Gas, Chromatography, Electron capture, Metabolite, Flunitrazepam, General Medicine, Isoamyl alcohol, Kinetics, chemistry.chemical_compound, Anti-Anxiety Agents, chemistry, Pharmacokinetics, medicine, Humans, Desmethylflunitrazepam, Female, Gas chromatography, Benzene, medicine.drug
Abstract

Nanogram quantities of flunitrazepam and its major metabolite, desmethylflunitrazepam, can be reliably quantitated in human plasma using electron-capture gas-liquid chromatography. After addition of methylnitrazepam as the internal standard, plasma samples are extracted with an organic solvent (benzene:isoamyl alcohol). The organic extract is separated, evaporated to dryness, reconstituted, and injected onto the chromatograph using an automatic sampling system which allows up to 100 analyses/24 h. The sensitivity limits are 0.5 ng/ml for flunitrazepam and 1-2 ng/ml for desmethylflunitrazepam. Use of the method is illustrated in a study of the pharmacokinetic properties of flunitrazepam following a single 1.0-mg intravenous dose.

Published
1982

3. Single and multiple dose kinetics of clobazam, and clinical effects during multiple dosage

Author

Hermann R. Ochs, Birgitt Verburg-Ochs, M. Lüttkenhorst, and David J. Greenblatt

Subjects
Adult, Male, Time Factors, Clobazam, Consciousness, Sedation, Pharmacology, Benzodiazepines, Pharmacokinetics, Oral administration, medicine, Humans, Pharmacology (medical), Volunteer, Morning, Volume of distribution, Benzodiazepinones, business.industry, Half-life, General Medicine, Middle Aged, Kinetics, Anti-Anxiety Agents, Anesthesia, Female, medicine.symptom, business, Half-Life, medicine.drug
Abstract

Sixteen healthy volunteers, aged 19 to 62 years, took a single 20-mg oral dose of clobazam and the serum concentrations of clobazam and desmethylclobazam were measured for the following 7 days. The mean kinetic variables for clobazam were: volume of distribution 1.31/kg, elimination half-life 24 h, total clearance 0.47 ml/min/kg. 13 of the volunteers then took clobazam 5 mg twice daily for 22 consecutive days. Serum concentrations were measured during and after this period. Both clobazam and desmethylclobazam showed slow and extensive accumulation, their steady-state kinetics being entirely consistent with those observed after single doses. Elimination of both compounds after termination of treatment was equally slow. Clinical self-rating of morning sedation indicated a significant increase over baseline in subjective perception of sedation during the treatment period, and this effect persisted into the washout period. However, sedation did not increase in parallel with accumulating levels of clobazam and desmethylclobazam, probably due to functional adaptation or tolerance.

Published
1984

4. Ibuprofen kinetics in patients with renal insufficiency who are receiving maintenance hemodialysis

Author

Hermann R. Ochs, David J. Greenblatt, and Birgitt Verburg-Ochs

Subjects
Adult, Male, medicine.medical_specialty, Resuscitation, Immunology, Ibuprofen, Rheumatology, Pharmacokinetics, Renal Dialysis, Oral administration, medicine, Humans, Immunology and Allergy, Pharmacology (medical), In patient, Intensive care medicine, Chromatography, High Pressure Liquid, business.industry, Blood Proteins, Fasting, Maintenance hemodialysis, Middle Aged, Kinetics, Anesthesia, Kidney Failure, Chronic, business, Half-Life, Protein Binding, medicine.drug
Published
1985

5. Disposition of clotiazepam: Influence of age, sex, oral contraceptives, cimetidine, isoniazid and ethanol

Author

Jerold S. Harmatz, Birgitt Verburg-Ochs, H. Grehl, David J. Greenblatt, and Hermann R. Ochs

Subjects
Adult, Male, Aging, Metabolic Clearance Rate, Pharmacology, Contraceptives, Oral, Hormonal, chemistry.chemical_compound, Sex Factors, Pharmacokinetics, Healthy volunteers, Isoniazid, medicine, Humans, Drug Interactions, Pharmacology (medical), Cimetidine, Clotiazepam, Aged, Volume of distribution, Ethanol, business.industry, Azepines, General Medicine, Disposition, Middle Aged, Kinetics, chemistry, Female, business, Half-Life, medicine.drug
Abstract

Factors influencing the disposition of clotiazepam in man were evaluated in a series of pharmacokinetic studies in healthy volunteers given a single 5 mg dose. Old age caused an increased volume of distribution of clotiazepam in women, and its clearance tended to be reduced in elderly men. Use of oral contraceptives, cimetidine, isoniazid or a single dose of ethanol had no significant effect on the kinetics of clotiazepam. Although clotiazepam is biotransformed by microsomal oxidation, its clearance appears to be relatively uninfluenced by factors known to alter the clearance of other oxidized benzodiazepines.

Published
1984

6. Effect of cirrhosis and renal failure on the kinetics of clotiazepam

Author

Martin Knüchel, Hermann R. Ochs, and David J. Greenblatt

Subjects
Adult, Liver Cirrhosis, Male, Oral dose, medicine.medical_specialty, Cirrhosis, Gastroenterology, chemistry.chemical_compound, Pharmacokinetics, Renal Dialysis, Internal medicine, medicine, Humans, Pharmacology (medical), In patient, Clotiazepam, Aged, Pharmacology, Volume of distribution, business.industry, Azepines, General Medicine, Maintenance hemodialysis, Middle Aged, medicine.disease, Kinetics, Endocrinology, chemistry, Thienodiazepine, Kidney Failure, Chronic, Female, business, Half-Life, medicine.drug
Abstract

The kinetics of a single 5-mg oral dose of the thienodiazepine clotiazepam was evaluated in a series of patients with biopsy-proven cirrhosis, and in patients with renal insufficiency requiring maintenance hemodialysis, compared to healthy matched controls. Clotiazepam volume of distribution (Vz) was significantly smaller in cirrhotic patients than in controls (1.83 vs 2.57 l/kg), and total clearance was likewise reduced (2.15 vs 3.15 ml/min/kg). Elimination half-life was similar between groups (10.0 vs. 10.2 h). There were no significant differences between renal failure and control patients in clotiazepam Vz, oral clearance, or elimination half-life. Thus cirrhosis is associated with reduced clearance of clotiazepam, probably due to impairment of its microsomal oxidation. However clotiazepam disposition is not significantly altered in dialysis-dependent renal insufficiency patients.

Published
1986

7. Propranolol interactions with diazepam, lorazepam, and alprazolam

Author

Hermann R. Ochs, Birgitt Verburg-Ochs, and David J. Greenblatt

Subjects
Adult, Male, Adolescent, Metabolite, Nordazepam, Propranolol, Pharmacology, Lorazepam, Benzodiazepines, chemistry.chemical_compound, medicine, Humans, Drug Interactions, Pharmacology (medical), Metaproterenol, Biotransformation, Chromatography, High Pressure Liquid, Diazepam, Alprazolam, Chemistry, Drug interaction, Kinetics, Injections, Intravenous, Female, Glucuronide, medicine.drug
Abstract

Healthy subjects received single doses of diazepam (5 to 10 mg iv), lorazepam (2 mg iv), or alprazolam (1 mg orally) on two occasions, once in the control state and once with propranolol, 80 mg three times a day. Compliance with the propranolol regimen was verified by measurement of serum propranolol levels (overall means: 100 ng/ml) and by reduction in sensitivity to intravenous metaproterenol to one-thirtieth that of the control value. Propranolol prolonged diazepam elimination t1/2 (58 and 49 hr), reduced its clearance (0.20 and 0.24 ml/min/kg), and increased the 168-hr AUC for desmethyldiazepam, the major metabolite of diazepam (5.63 and 4.81 micrograms/ml . hr). Propranolol had no significant effect on lorazepam t1/2 (13.2 and 12.7 hr) or clearance (1.33 and 1.36 ml/min/kg), nor on alprazolam t1/2 (15.9 and 18.5 hr) or clearance (1.1 and 0.8 ml/min/kg). Thus propranolol induces a small but significant reduction in clearance of diazepam, biotransformed mainly by the oxidative reaction of N-demethylation. Propranolol does not impair lorazepam clearance by glucuronide conjugation nor that of alprazolam by aliphatic hydroxylation.

Published
1984

8. Kinetics and cardiac effects of propranolol in humans

Author

Martin Knüchel, Hermann R. Ochs, Gunther Bodem, David J. Greenblatt, and Eberhard Grube

Subjects
Adult, Male, medicine.medical_specialty, Kinetics, Extraction ratio, Diastole, Administration, Oral, Propranolol, Pharmacology, Single oral dose, Pharmacokinetics, Internal medicine, Drug Discovery, medicine, Humans, Genetics (clinical), Volume of distribution, Dose-Response Relationship, Drug, Chemistry, General Medicine, Myocardial Contraction, Endocrinology, Injections, Intravenous, Molecular Medicine, Female, Steady state (chemistry), Half-Life, medicine.drug
Abstract

Six healthy volunteers received single 20-mg intravenous (IV) and 80-mg oral doses of propranolol on two occasions in random sequence. Serum propranolol concentrations were determined by gas chromatography in multiple samples drawn during 24 h after each dose. Mean (+/- SE) kinetic variables for IV propranolol were: elimination half-life (t 1/2 beta), 5.3 (+/- 0.6) h; volume of distribution, 2.3 (+/- 0.3) l/kg; total clearance, 4.9 (+/- 0.3) ml/min/kg; predicted extraction ratio, 0.23 (+/- 0.02). After single oral doses, t 1/2 beta (3.8 +/- 0.2 h) tended to be smaller than after the IV dose, and actual systemic availability (0.60 +/- 0.07) was less than that based on the predicted extraction ratio. During multiple oral dosage (80 mg every 12 h), observed steady state serum levels (47 +/- 5 ng/ml) tended to be less than those predicted based on the single oral dose (61 +/- 5 ng/ml), thus providing no evidence for reduced propranolol clearance at steady-state. Echocardiographic measurements of left ventricular performance (posterior wall velocity, diastolic dimensions) made during the single-dose oral study indicated significant impairment of function; impairment was maximal at 3 h post-dosage, and corresponded to the time of the peak serum propranolol concentration (341 ng/ml).

Published
1982

9. Intravenous quinidine in congestive cardiomyopathy

Author

Rainer M. Arendt, David J. Greenblatt, Hermann R. Ochs, and Eberhard Grube

Subjects
Adult, Male, Quinidine, medicine.medical_specialty, Cardiomyopathy, Electrocardiography, Internal medicine, Congestive Cardiomyopathy, medicine, Humans, Infusions, Parenteral, Pharmacology (medical), Aged, Pharmacology, Lv function, Volume of distribution, Ejection fraction, business.industry, General Medicine, Middle Aged, Serum samples, medicine.disease, Kinetics, Blood pressure, Anesthesia, Cardiology, Cardiomyopathies, business, medicine.drug
Abstract

Eight male patients with compensated congestive cardiomyopathy received single 300-mg doses of intravenous quinidine by 15-min infusion. Left ventricular (LV) performance was evaluated by echocardiography at multiple points in time during the next 24 h. Quinidine kinetics and protein binding were determined from multiple serum samples drawn for up to 36 h after dosage. LV function was not impaired. Instead, quinidine transiently increased ejection fraction (mean: +39%) and rate of circumferential shortening (mean: +46%). Endsystolic and end-diastolic LV internal diameter likewise were decreased (means: -13% and -7%). Blood pressure and ventricular rate were not significantly altered. Compared to 8 healthy controls matched for age, sex, and weight, quinidine volume of distribution among patients was smaller (means: 2.27 vs 1.90 l/kg), as was total quinidine clearance (3.49 vs 2.84 ml/min/kg); however, differences were not statistically significant. Well-controlled, slow intravenous infusion of quinidine does not impair LV performance and is safe for patients with compensated congestive cardiomyopathy. However, such patients may have reduced quinidine clearance and hence require lower doses than expected based on age and weight.

Published
1981

10. Cerebrospinal fluid uptake and peripheral distribution of centrally acting drugs: Relation to lipid solubility

Author

Hermann R. Ochs, Joachim Gerloff, Wolfgang Eichelkraut, David J. Greenblatt, Norbert Hahn, Darrell R. Abernethy, and Rainer M. Arendt

Subjects
Pharmacology, Volume of distribution, Chromatography, Chemistry, Pharmaceutical Science, Trimipramine, Lipids, High-performance liquid chromatography, Imipramine, Kinetics, Dogs, Cerebrospinal fluid, Pharmaceutical Preparations, Solubility, Lipophilicity, medicine, Animals, Kovats retention index, Distribution (pharmacology), Half-Life, medicine.drug
Abstract

In an anaesthetized dog model, serum kinetics and CSF entry were determined after i.v. administration of the following 8 drugs: salicylic acid (as acetylsalicylic acid), antipyrine, acetaminophen (paracetamol), lidocaine (lignocaine), trimipramine, amitriptyline, haloperidol, and imipramine. Kinetic variables were evaluated in relation to in-vitro lipophilicity, measured by the reverse-phase high-pressure liquid chromatographic (HPLC) retention index. After correction for individual values of serum binding (determined as the CSF: serum ratio at equilibrium), in-vivo volume of distribution was highly correlated with HPLC retention (r = 0.92). Conversely, the time of peak CSF concentration and the CSF entry half-life were negatively correlated with HPLC retention (r = −0.83 and −0.63, respectively). Thus lipophilicity is a physiochemical property which has an influence on the peripheral distribution of drugs as well as their rate of entry into CSF.

Published
1985

11. Metoprolol or Propranolol Does Not Alter the Kinetics of Procainamide

Author

Gerhard Carstens, Hermann R. Ochs, David J. Greenblatt, and Gerda-Marie Roberts

Subjects
Adult, Pharmacology, Intravenous dose, business.industry, Metabolite, Kinetics, Propranolol, Procainamide, Propanolamines, chemistry.chemical_compound, chemistry, Humans, Medicine, Drug Interactions, Metaproterenol, Cardiology and Cardiovascular Medicine, business, Metoprolol, medicine.drug, Procainamide Hydrochloride
Abstract

Eight healthy volunteers received a single 500 mg intravenous dose of procainamide hydrochloride by 30-min infusion on three occasions in random sequence. The three modes of administration were (a) control, without concurrent drugs; (b) during coadministration of propranolol, 80 mg three times daily; and (c) during coadministration of metoprolol, 100 mg two times daily. Procainamide kinetics were determined from multiple serum concentrations measured by enzyme-multiplied immunoassay (EMIT) during 10 h after each dose. A metaproterenol infusion study verified a high degree of beta-blockade during trials 2 and 3. Mean procainamide half-life during the three trials (1.9, 2.2, and 2.3 h, respectively) tended to show prolongation during beta-blocker treatment, but the overall difference was of borderline significance (0.05 less than p less than 0.1). Total procainamide clearance (16.2, 14.1, and 13.7 ml/min/kg) did not differ significantly between the three trials, nor was there a significant change in area under the serum concentration curve for N-acetylprocainamide, the major metabolite. Thus the kinetics of procainamide in healthy persons are not importantly altered by typical therapeutic doses of two beta-adrenergic blockers.

Published
1983

13. Trazodone kinetics: Effect of age, gender, and obesity

Author

H Friedman, Jerold S. Harmatz, Richard I. Shader, David J. Greenblatt, Ethan S. Burstein, Joseph M. Scavone, Hermann R. Ochs, Lawrence G Miller, and Gershwin T. Blyden

Subjects
Adult, Male, Aging, medicine.medical_specialty, Physiology, Body weight, Random Allocation, Pharmacokinetics, Oral administration, Internal medicine, medicine, Humans, Pharmacology (medical), Obesity, Biotransformation, Aged, Pharmacology, Volume of distribution, Sex Characteristics, business.industry, Trazodone, Half-life, Middle Aged, medicine.disease, Kinetics, Endocrinology, Female, business, Half-Life, medicine.drug, Sex characteristics
Abstract

Single 25 mg intravenous and 50 mg oral doses of trazodone were given to 43 healthy subjects, divided into young men and women (aged 18 to 40 years) and elderly men and women (aged 60 to 76 years). Among men, trazodone volume of distribution (Varea) was increased in elderly vs. young subjects (1.15 vs. 0.89 L/kg; P less than 0.05), and clearance decreased (1.65 vs. 2.31 ml/min/kg; P less than 0.05), thereby increasing elimination half-life (t1/2) in elderly men (8.2 vs. 4.7 hours; P less than 0.001). Varea in women was also increased in the elderly (1.5 vs. 1.27 L/kg; P less than 0.02), causing increased t1/2 (7.6 vs. 5.9 hours; P less than 0.05), but clearance was unrelated to age. Absolute bioavailability of oral trazodone averaged 70% to 90% and was unrelated to age or sex. In 23 obese subjects (mean weight 112 kg) vs. 23 matched control subjects of normal weight (mean 65 kg), Varea was greatly increased (162 vs. 67 L; 1.43 vs. 1.04 L/kg; P less than 0.001) and was highly correlated with body weight (r = 0.91). Clearance was unchanged between groups (146 vs. 136 ml/min), but the increased Varea caused prolonged t1/2 in obese subjects (13.3 vs. 5.9 hours; P less than 0.001). Reduced clearance of trazodone among elderly men may indicate a need for dosage reduction during chronic therapy. In obese individuals, choice of dosage during chronic treatment should be based on ideal rather than total body weight.

Published
1987

14. Single and multiple dose pharmacokinetics of oral quinidine sulfate and gluconate

Author

Hermann R. Ochs, Kate Franke, Henry J. Pfeifer, David J. Greenblatt, Thomas W. Smith, and Elaine Woo

Subjects
Adult, Male, Quinidine, medicine.medical_specialty, Administration, Oral, Absorption (skin), Pharmacology, Gluconates, chemistry.chemical_compound, Quinidine Sulfate, Pharmacokinetics, Internal medicine, Humans, Medicine, Sulfate, Sulfates, business.industry, Quinidine Gluconate, Crossover study, Kinetics, chemistry, Anesthesia, Cardiology, Female, Steady state (chemistry), Cardiology and Cardiovascular Medicine, business, Half-Life, medicine.drug
Abstract

The pharmacokinetics of oral quinidine sulfate and quinidine gluconate were compared in seven healthy volunteers In a two part pharmacokinetic study. Part I was a single dose crossover trial assessing absorption and elimination of quinidine sulfate (400 mg, equivalent to 331 mg of quinidine base) and quinidine gluconate (495 mg, equivalent to 309 mg of quinidine base). Mean kinetic values for the sulfate and gluconate preparations, respectively, were: peak serum quinidine level 2.07 versus 1.24 μg/ml (P Part II evaluated steady state kinetics of both preparations in a cross-over trial in the same subjects. Maintenance dosing schedules were 200 mg of quinidine sulfate every 6 hours versus 495 mg of quinidine gluconate every 12 hours. Systemic availability of the gluconate at the steady state level was 10 percent less (based upon area under the serum concentration curve) or 7 percent less (based upon urinary excretion of quinidine) than that of the sulfate, but the differences were not significant. Interdose fluctuation in serum quinidine concentrations during the gluconate trial averaged 70 percent, which was not significantly different from the average of 67 percent during the sulfate trial. However, variation within and between subjects in minimal steady state levels with quinidine gluconate (15.6 and 16.0 percent, respectively) was greater than with quinidine sulfate (7.2 and 9.9 percent, respectively). Steady state concentrations during the multiple dose trial were not accurately predicted from single dose pharmacokinetics, either for quinidine sulfate (r = 0.45) or quinidine gluconate (r = −0.12), but deviation of observed from predicted concentrations tended to be greater with quinidine gluconate. The slow absorption of quinidine from the gluconate preparation allows maintenance therapy on a 12 hourly dosage schedule with acceptable interdose fluctuation in serum levels. Variability within and between subjects in absorption kinetics tends to be greater with quinidine gluconate than with the more rapidly absorbed sulfate salt.

Published
1978

15. Cimetidine impairs nitrazepam clearance

Author

Roland Gugler, Hermann R. Ochs, David J. Greenblatt, Gerrit Müntefering, Ann Locniskar, and Darrell R. Abernethy

Subjects
Adult, Male, Pharmacology, Volume of distribution, Benzodiazepine, Adolescent, Nitrazepam, Chemistry, medicine.drug_class, Drug interaction, Guanidines, Kinetics, Liver, Pharmacokinetics, Histamine H2 receptor, Oral administration, medicine, Humans, Drug Interactions, Pharmacology (medical), Cimetidine, medicine.drug
Abstract

The effect of cimetidine on hepatic clearance of the benzodiazepine derivative nitrazepam was evaluated in healthy subjects. Six received a single 5- or 10-mg oral nitrazepam dose in the drug-free state and again with therapeutic cimetidine doses. Nitrazepam kinetics were determined from multiple serum concentrations measured during the 72 hr after each dose. Cimetidine had no effect on nitrazepam absorption kinetics, since peak serum nitrazepam concentration and time of peak concentration were not altered. Cimetidine did not alter nitrazepam volume of distribution, but cimetidine consistently reduced nitrazepam clearance, from a mean of 1.41 ml/min/kg in the control state to 1.17 ml/min/kg during cimetidine treatment. This resulted in prolongation of nitrazepam elimination t½ from 22.2 to 27.8 hr. Thus the ability of cimetidine to impair drug oxidation in man extends to the capacity for clearance of nitrazepam, a compound biotransformed mainly by nitroreduction. Clinical Pharmacology and Therapeutics (1983) 34, 227–230; doi:10.1038/clpt.1983.157

Published
1983

16. Comparative Single-Dose Kinetics of Oxazolam, Prazepam, and Clorazepate: Three Precursors of Desmethyldiazepam

Author

B S Ann Locniskar, Birgitt Verburg-Ochs, Hermann R. Ochs, and David J. Greenblatt

Subjects
Adult, Male, Nordazepam, Pharmacology, Benzodiazepines, Pharmacokinetics, Oral administration, medicine, Humans, Clorazepate, Pharmacology (medical), Volunteer, Clorazepate Dipotassium, Prazepam, Benzodiazepinones, Diazepam, Chemistry, Area under the curve, Molecular Weight, Kinetics, Anti-Anxiety Agents, Female, Oxazolam, medicine.drug
Abstract

Twelve healthy volunteers received a single 40-mg oral dose of the benzodiazepine derivative oxazolam, which serves primarily as a precursor of the active substance desmethyldiazepam (DMDZ). Concentrations of DMDZ were measured in multiple serum samples drawn for up to two weeks after the dose. Peak serum DMDZ concentrations averaged 115 ng/ml, measured at 8.6 hours after dosage. Mean DMDZ elimination half-life averaged 61 hours. Three of the subjects also received 40 mg each of prazepam and clorazepate, two other DMDZ precursors, on separate occasions. Although DMDZ elimination half-life was similar, total area under the curve (AUC) for DMDZ was larger for clorazepate, known to be completely transformed into DMDZ, than for oxazolam or prazepam the extent of whose conversion to DMDZ has not been previously established. After correcting for the different molar equivalent of DMDZ available from each preparation, the DMDZ ratio averaged 0.22 for oxazolam vs. clorazepate and 0.51 for prazepam vs. clorazepate. Thus, both oxazolam and prazepam lead to slow appearance of DMDZ in the systemic circulation. Furthermore the extent of DMDZ formation from oxazolam and prazepam is either incomplete or the drugs are incompletely absorbed. Equivalent doses of oxazolam, prazepam, and clorazepate should not be interchanged in clinical practice.

Published
1984

17. Effect of alprazolam on digoxin kinetics and creatinine clearance

Author

Hermann R. Ochs, Birgitt Verburg-Ochs, and David J. Greenblatt

Subjects
Adult, Male, Digoxin, medicine.medical_specialty, Adolescent, Metabolic Clearance Rate, Renal function, Digitalis, Excretion, Benzodiazepines, chemistry.chemical_compound, Pharmacokinetics, Internal medicine, medicine, Humans, Drug Interactions, Pharmacology (medical), Pharmacology, Volume of distribution, Creatinine, Alprazolam, biology, biology.organism_classification, Kinetics, Endocrinology, Anti-Anxiety Agents, chemistry, medicine.drug
Abstract

Eight healthy men received a single, 1.25 mg dose of digoxin on two occasions, once in an otherwise drug-free control state and again while concurrently receiving alprazolam, 1.5 mg/day. There was no significant difference between control and alprazolam conditions in digoxin volume of distribution (11.0 vs. 11.2 L/kg), elimination t1/2 (46 vs. 41 hours), or total clearance from serum (2.8 vs. 3.6 ml/min/kg). Alprazolam coadministration slightly reduced mean 96-hour urinary excretion of digoxin (37.6% vs. 30.9% of dose; P less than 0.01), but there was no significant difference between treatment conditions in projected total cumulative excretion of digoxin (45.2% vs. 40.9% of dose) or in renal clearance of digoxin (1.23 vs. 1.44 ml/min/kg). Creatinine clearance also did not differ between the control and alprazolam conditions (164 vs. 142 ml/min). Thus therapeutic doses of alprazolam do not significantly alter digoxin clearance in healthy man.

Published
1985

18. Impairment of Digoxin Clearance by Coadministration of Quinidine

Author

David J. Greenblatt, Hermann R. Ochs, and Gunther Bodem

Subjects
Adult, Male, Quinidine, Digoxin, Evening, Heart Diseases, Pharmacology, Random Allocation, Healthy volunteers, polycyclic compounds, medicine, Humans, Drug Interactions, Infusions, Parenteral, Pharmacology (medical), cardiovascular diseases, Biotransformation, Morning, Volume of distribution, Serum digoxin, business.industry, Middle Aged, carbohydrates (lipids), Kinetics, Anesthesia, Drug Therapy, Combination, Female, business, Site of action, Half-Life, medicine.drug
Abstract

Seven healthy volunteers received a single 1.0-mg dose of intravenous digoxin in a drug-free control trial and again during concurrent therapy with therapeutic doses of quinidine. Digoxin kinetics were determined from multiple serum digoxin concentrations measured during 72 hours after dosage. Compared to the control state, quinidine coadministration reduced mean digoxin volume of distribution (15.1 vs. 12.4 l./kg), prolonged its elimination half-life (47.7 vs. 75.7 hours), and significantly reduced total clearance (6.06 vs. 2.18 ml/min.kg). Both renal and extrarenal digoxin clearances were impaired by quinidine. In nine cardiac patients receiving long-term digoxin therapy (0.25 mg twice daily), quinidine coadministration elevated mean morning digoxin levels from 1.37 to 2.0 ng/ml (P less than 0.001) and evening levels from 1.44 to 1.97 ng/ml (N.S.). If digoxin concentrations at the site of action are increased by quinidine, the interaction is likely to be of clinical importance in many patients.

Published
1981

19. Clinical Pharmacokinetics of the Newer Benzodiazepines

Author

Richard I. Shader, David J. Greenblatt, Hermann R. Ochs, Marcia Divoll, and Darrell R. Abernethy

Subjects
Triazolam, medicine.drug_class, Midazolam, Pharmacology, Lorazepam, Halazepam, Hypnotic, Benzodiazepines, Temazepam, medicine, Humans, Pharmacology (medical), Clotiazepam, Benzodiazepinones, Benzodiazepine, Alprazolam, Chemistry, Brotizolam, Azepines, Lormetazepam, Kinetics, Anti-Anxiety Agents, Clobazam, medicine.drug
Abstract

New benzodiazepine derivatives continue to be developed and introduced into clinical use. The pharmacokinetic properties of these newer drugs can best be understood by their categorisation according to range of elimination half-life and pathway of metabolism (oxidation versus conjugation). Clobazam and halazepam are long half-life (and therefore accumulating) anxiolytics metabolised by oxidation. Alprazolam and clotiazepam also are oxidised compounds but have short to intermediate half-life values and therefore produce considerably less accumulation. Temazepam and lormetazepam are hypnotic agents with intermediate half-lives but metabolised by conjugation. The most unique of the newer benzodiazepines are the ultra-short half-life (oxidised) compounds midazolam, triazolam and brotizolam, which are essentially non-accumulating during multiple dosage.

Published
1983

20. Influence of propranolol coadministration or cigarette smoking on the kinetics of desmethyldiazepam following intravenous clorazepate

Author

David J. Greenblatt, Ann Locniskar, Hermann R. Ochs, and J. Weinbrenner

Subjects
Adult, Male, Metabolic Clearance Rate, Nordazepam, Kinetics, Propranolol, Cigarette smoking, Pharmacokinetics, Drug Discovery, medicine, Humans, Clorazepate, Drug Interactions, Infusions, Intravenous, Clorazepate Dipotassium, Genetics (clinical), Volume of distribution, Diazepam, Chemistry, Smoking, General Medicine, Anti-Anxiety Agents, Free fraction, Anesthesia, Molecular Medicine, Female, medicine.drug
Abstract

The influence of propranolol coadministration or of cigarette smoking on the kinetics of desmethyldiazepam following a single 20-mg intravenous dose of clorazepate dipotassium was evaluated in healthy volunteers. In Study One, intravenous clorazepate was given once in the control condition, and again during coadministration of propranolol, 80 mg twice daily. Compliance with the prescribed propranolol regimen was verified by measurement of serum propranolol concentrations (mean, 37 ng/ml). In control vs propranolol treatment conditions, there was no significant difference in desmethyldiazepam volume of distribution (1.27 vs 1.23 liters/kg) or in free fraction in serum (1.83 vs 1.80% unbound). There was a small although statistically significant prolongation of desmethyldiazepam half-life (55 vs 61 h, P less than 0.05) and reduction in clearance (0.281 vs 0.247 ml/min/kg, P less than 0.02) attributable to propranolol. In Study Two, desmethyldiazepam kinetics were compared in eight cigarette smokers (mean, 19 cigarettes/day) and in 11 nonsmoking controls matched for age, sex, and body weight. There was no significant difference between controls and cigarette smokers in desmethyldiazepam volume of distribution (1.29 vs 1.34 liters/kg), elimination half-life (55 vs 59 h), clearance (0.284 vs 0.276 ml/min/kg), or free fraction in serum (1.96 vs 1.92% unbound). Thus, propranolol slightly although significantly impairs the clearance of desmethyldiazepam and prolongs its half-life. Cigarette smoking has no apparent influence on desmethyldiazepam kinetics.

Published
1986

22. Diazepam kinetics in patients with renal insufficiency or hyperthyroidism

Author

HJ Kaschell, Marcia Divoll, Hermann R. Ochs, David J. Greenblatt, U. Klehr, and Abernethy

Subjects
Male, Drug, medicine.medical_specialty, Time Factors, media_common.quotation_subject, Age and sex, Hyperthyroidism, Pharmacotherapy, Internal medicine, medicine, Humans, Distribution (pharmacology), Pharmacology (medical), In patient, media_common, Pharmacology, Diazepam, business.industry, Maintenance haemodialysis, Middle Aged, Kinetics, Endocrinology, Female, Kidney Diseases, business, Research Article, medicine.drug, Blood sampling
Abstract

1 Eight patients with end-stage renal insufficiency on maintenance haemodialysis, and seven patients with newly diagnosed hyperthyroidism, received a single intravenous dose of diazepam, followed by blood sampling over the next 7 days. Fifteen healthy volunteer controls, matched with patients for age and sex, were similarly studied. 2 Diazepam half-life in renal failure patients (mean 37 h) was greatly reduced compared to controls (mean 92 h, P less than 0.05) and clearance of total (free plus bound) diazepam correspondingly increased (0.94 v 0.34 ml min-1 kg-1, P less than 0.01). 3 However, differences were largely related to disease-related changes in drug binding and distribution. Mean unbound fraction of diazepam in plasma of renal patients (7.0%) was greatly increased over controls (1.4%, P less than 0.01) and Vd of unbound diazepam greatly reduced (57 v 157 l/kg, P less than 0.01). 4 Clearance of pharmacologically active unbound diazepam (intrinsic clearance) was not significantly different between renal patients and controls (23 vs 30 ml min-1 kg-1). 5 None of the kinetic variables for total or unbound diazepam in thyrotoxic patients differed significantly from those in controls matched for age and sex. 6 End-stage renal failure (or its associated drug therapy) alters diazepam protein binding and distribution, but does not significantly change clearance of unbound drug. Thyrotoxicosis does not influence diazepam kinetics.

Published
1981

23. Reduction in Lidocaine Clearance during Continuous Infusion and by Coadministration of Propranolol

Author

Gerhard Carstens, Hermann R. Ochs, and David J. Greenblatt

Subjects
Adult, Male, Drug, Time Factors, Adolescent, Lidocaine, Continuous infusion, media_common.quotation_subject, medicine.medical_treatment, Propranolol, Pharmacology, medicine, Humans, Infusions, Parenteral, Reduction (orthopedic surgery), media_common, business.industry, General Medicine, Kinetics, Anesthesia, cardiovascular system, Female, business, medicine.drug
Abstract

LIDOCAINE is commonly administered parenterally for the treatment of cardiac arrhythmias. The use of this drug is complicated by its narrow therapeutic index.1 Any reduction in its metabolic cleara...

Published
1980

24. Disease-related Alterations in Cardiac Glycoside Disposition

Author

David J. Greenblatt, Hermann R. Ochs, Gunther Bodem, and Hans J. Dengler

Subjects
Digoxin, Gastrointestinal Diseases, Pharmacology toxicology, Disease, Biology, Pharmacology, Cardiac Glycosides, Pharmacotherapy, Digitoxin, medicine, Humans, Pharmacology (medical), Ouabain, Cardiac glycoside, Kidney, Gastrointestinal tract, Liver Diseases, Thyroid, Disposition, Thyroid Diseases, Kinetics, medicine.anatomical_structure, Intestinal Absorption, Cardiovascular Diseases, Kidney Diseases, Half-Life, Protein Binding, medicine.drug
Abstract

The effects of diseases involving the kidney, gastrointestinal tract, thyroid, and cardiovascular system on the disposition of cardiac glycosides are reviewed.

Published
1982

25. Benzodiazepine Kinetics: Implications for Therapeutics and Pharmacogeriatrics

Author

Marcia Divoll, David J. Greenblatt, Darrell R. Abernethy, Hermann R. Ochs, and Richard I. Shader

Subjects
Adult, Adolescent, medicine.drug_class, Nordazepam, Kinetics, Pharmacology, Flurazepam, Benzodiazepines, Biotransformation, medicine, Humans, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Child, Aged, Benzodiazepine, Diazepam, Chemistry, Age Factors, Oxidation reduction, Middle Aged, Oxidation-Reduction, Drug metabolism, Half-Life
Abstract

(1983). Benzodiazepine Kinetics: Implications for Therapeutics and Pharmacogeriatrics. Drug Metabolism Reviews: Vol. 14, No. 2, pp. 251-292.

Published
1983

26. Benzodiazepine drug-drug interactions commonly occurring in clinical practice

Author

Richard I. Shader, David J. Greenblatt, Hermann R. Ochs, and Darrell R. Abernethy

Subjects
Drug, medicine.medical_specialty, medicine.drug_class, media_common.quotation_subject, Propranolol, Pharmacology, Mixed Function Oxygenases, Benzodiazepines, chemistry.chemical_compound, Pharmacokinetics, Internal medicine, Disulfiram, Isoniazid, medicine, Humans, Ingestion, Drug Interactions, Cimetidine, media_common, Benzodiazepine, Ethanol, business.industry, General Medicine, Kinetics, Endocrinology, Anti-Anxiety Agents, Liver, chemistry, Enzyme Induction, business, Contraceptives, Oral, medicine.drug
Abstract

Pharmacokinetic drug-drug interactions which involve currently available benzodiazepines may be classified into two major categories: interactions which affect benzodiazepine rate of absorption, and interactions which affect clearance and, therefore, elimination half-life. Ethanol is the prototype for absorptive interactions. Concurrent ethanol use and oral ingestion of benzodiazepine derivatives uniformly slows the rate but does not change the extent of benzodiazepine absorption. Interactions which affect benzodiazepine clearance affect only those derivatives which are oxidatively metabolized or cleared as a function of hepatic blood flow (high first-pass clearance). Conjugated benzodiazepines are not implicated in such interactions. Rifampin and chronic ethanol use induce benzodiazepine oxidation, while cimetidine, oral contraceptives, ethanol (acute ingestion), disulfiram, isoniazid, and propranolol inhibit benzodiazepine oxidation. In addition, ethanol, cimetidine and isoniazid decrease first-pass hepatic extraction of triazolam, enhancing its systemic availability and decreasing oral clearance. The pharmacokinetic consequence of induction of benzodiazepine oxidation is higher clearance and decreased steady-state concentrations during chronic dosing. Conversely, inhibition of benzodiazepine oxidation decreases clearance and increases steady-state benzodiazepine concentrations during chronic dosing. Because a correlation of benzodiazepine plasma concentration and pharmacological effect is not established, the pharmacodynamic consequences of these interactions are not currently well characterized.Pharmacokinetic drug-drug interactions which involve currently available benzodiazepines may be classified into 2 major categories: interactions which affect benzodiazepine rate of absorption, and interactions which affect clearance and, therefore, elimination 1/2-life. Ethanol is the prototype for absorptive interactions. Concurrent ethanol use and oral ingestion of benzodiazepine derivatives uniformly slows the rate but does not change the extent of benzodiazepine absorption. Interactions which affect benzodiazepine clearance affect only those derivatives which are oxidatively metabolized or cleared as a function of hepatic blood flow (high 1st pass clearance). Conjugated benzodiazepines are not implicated in such interactions. Rifampicin and chronic ethanol use induce benzodiazepine oxidation, while cimetidine, oral contraceptives, ethanol (acute ingestion), disulfiram, isoniazid, and propranolol inhibit benzodiazepine oxidation. In addition, ethanol, cimetidine and isoniazid decrease 1st pass hepatic extraction of triazolam, enhancing its systemic availability and decreasing oral clearance. The pharmacokinetic consequence of induction of benzodiazepine oxidation is higher clearance and decreased steady state concentrations during chronnic dosing. Conversely, inhibition of benzodiazepine oxidation decreases clearance and increases steady state benzodiazepine plasma concentration and pharmacological effect is not established, the pharmacodynamic consequences of these interactions are not currently well characterized. (author's)

Published
1984

27. Desmethyldiazepam kinetics after intravenous, intramuscular, and oral administration of clorazepate dipotassium

Author

Martin Knüchel, Hermann R. Ochs, Ann Locniskar, Elke Steinhaus, and David J. Greenblatt

Subjects
Adult, Male, Metabolic Clearance Rate, Nordazepam, Administration, Oral, Absorption (skin), Pharmacology, Injections, Intramuscular, Pharmacokinetics, Oral administration, Drug Discovery, medicine, Humans, Clorazepate, Clorazepate Dipotassium, Genetics (clinical), Aged, Volume of distribution, Diazepam, business.industry, General Medicine, Middle Aged, Bioavailability, Kinetics, Anti-Anxiety Agents, Anesthesia, Injections, Intravenous, Molecular Medicine, Female, Intramuscular injection, business, Half-Life, medicine.drug
Abstract

The pharmacokinetics and bioavailability of desmethyldiazepam (DMDZ), formed from its precursor clorazepate (CZP) dipotassium, were assessed in a series of 17 healthy volunteers aged 21--66 years. After a single 20-mg intravenous dose of CZP, mean kinetic variables for DMDZ were: volume of distribution, 1.24 l/kg; elimination half-life, 65 h; total clearance, 0.24 ml/min/kg. Among males, DMDZ half-life tended to be prolonged and clearance reduced with age, but this was not true for females. After oral administration of 20 mg CZP, appearance of DMDZ in the circulation was rapid; the mean peak plasma level was 356 ng/ml, reached an average of 0.9 h after dosage. Based on comparison with IV dosage, systemic availability of DMDZ was complete (100% absorption). Ten of the subjects also received a single 20-mg intramuscular dose of CZP. Mean peak DMDZ levels were 290 ng/ml, reaching an average of 2.7 h after dosage. Systemic availability of DMDZ was complete. Elimination half-life of DMDZ for a given individual was highly replicable from trial to trial regardless of the route of CZP administration.

Published
1982

28. Obesity effects on nitrazepam disposition

Author

Jerold S. Harmatz, David J. Greenblatt, Ann Locniskar, Hermann R. Ochs, Abernethy, and Richard I. Shader

Subjects
Adult, Male, medicine.medical_specialty, Nitrazepam, medicine.drug_class, Hypnotic, Pharmacokinetics, Oral administration, Internal medicine, medicine, Humans, Tissue Distribution, Pharmacology (medical), Obesity, Pharmacology, Volume of distribution, Chemistry, Half-life, Blood Proteins, medicine.disease, Blood proteins, Kinetics, Endocrinology, Female, Research Article, Half-Life, Protein Binding, medicine.drug
Abstract

Nitrazepam pharmacokinetics were studied in 14 obese (mean +/- s.e. mean body weight 107 +/- 9 kg; percent ideal body weight [IBW] 166 +/- 12%) and 14 normal body weight (63 +/- 3 kg; percent IBW 98 +/- 2%) subjects. After an overnight fast, each subject ingested 10 mg nitrazepam orally. Nitrazepam concentrations were determined in plasma samples obtained over the following 72 h. Comparison of peak nitrazepam plasma concentration (94.2 +/- 10.3-obese vs 119 +/- 14.6 ng ml-1; NS) and time required after drug administration to reach peak concentration (1.52 +/- 0.24-obese vs 1.59 +/- 0.36 h; NS) indicated no differences between obese and control subjects. Elimination half-life was markedly increased in obese subjects (33.5 +/- 2.2 vs 23.9 +/- 1.2 h; P less than 0.001) due to increased apparent volume of distribution (Vd) (290 +/- 45 vs 137 +/- 12 l; P less than 0.005). Oral clearance was also increased in the obese subjects (101 +/- 12.4 vs 66.8 +/- 12.4 ml min-1; P less than 0.02). Extent of nitrazepam binding to plasma proteins was slightly decreased in obese subjects (% unbound--19.7 +/- 0.4-obese vs 17.9 +/- 0.3%; P less than 0.005). Correction of both Vd (2.62 +/- 0.17-obese vs 2.22 +/- 0.19 l kg-1; NS) and clearance (0.93 +/- 0.06-obese +/- 1.07 +/- 0.07 ml min-1 kg-1; NS) for total body weight (TBW) suggested that increases in obese subjects of both of these parameters were a function of body weight.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1986

29. Absorption of digoxin from the distal parts of the intestine in man

Author

H. J. Dengler, Hermann R. Ochs, Kodrat G, Schäfer Pk, and G. Bodem

Subjects
Adult, Male, Blood level, Digoxin, medicine.medical_specialty, Adolescent, Colon, Biological Availability, Absorption (skin), Gastroenterology, Urinary excretion, Internal medicine, Humans, Medicine, Pharmacology (medical), Pharmacology, business.industry, Transverse colon, General Medicine, Middle Aged, medicine.disease, Ulcerative colitis, Bioavailability, Kinetics, Colonic mucosa, Intestinal Absorption, Colitis, Ulcerative, Female, business, medicine.drug
Abstract

In 12 patients undergoing coloscopy, 0.5 mg digoxin in aqueous alcoholic solution was injected into the transverse colon. The late maximum of the blood level curve at about 2 hours after the administration suggested delayed absorption of the glycoside. However, the 24 hour urinary excretion of 17 +/- 3.4% in 8 patients with normal colonic mucosa demonstrated extensive absorption in the distal part of the bowel. The results have been contrasted with the findings in 4 patients with ulcerative colitis who excreted only 1.66 +/- 0.6% of the given dose in 24 hours.

Published
1975

30. Reduced Distribution and Clearance of Acetaminophen in Patients with Congestive Heart Failure

Author

David J. Greenblatt, Hermann R. Ochs, Uta Schuppan, and Darrell R. Abernethy

Subjects
Adult, Male, medicine.medical_specialty, Metabolic Clearance Rate, Analgesic, Pharmacology, Pharmacokinetics, Internal medicine, Humans, Medicine, Distribution (pharmacology), Tissue Distribution, Antipyretic, Acetaminophen, Heart Failure, Volume of distribution, business.industry, Middle Aged, medicine.disease, Kinetics, Heart failure, Cardiology, Female, Cardiology and Cardiovascular Medicine, business, Glucuronide, medicine.drug
Abstract

Acetaminophen is a widely prescribed analgesic/antipyretic metabolized by hepatic glucuronide and sulfate conjugation. Twelve patients, 30-66 years of age, with stable Class III or IV congestive heart failure (CHF) and 12 healthy controls matched for age, sex, and weight received single 650-mg intravenous doses of acetaminophen. Pharmacokinetic variables were determined from multiple plasma acetaminophen concentrations measured by liquid chromatography during 12 h after the dose. Compared with controls, mean total clearance of acetaminophen was reduced in CHF patients (3.56 vs. 4.59 ml/min/kg, p less than 0.025), indicating reduced biotransformation capacity in this disease. Volume of distribution was also significantly reduced in CHF patients (0.85 vs. 1.02 L/kg, p less than 0.05). Since elimination half-life depends on both volume of distribution and clearance (both of which were reduced), the half-life was similar between groups (2.87 vs. 2.34 h, NS). Thus, hepatic conjugation of acetaminophen is impaired in CHF. The finding may also apply to other drugs biotransformed by conjugation.

Published
1983

31. Effect of cimetidine on digoxin kinetics and creatinine clearance

Author

Thomas Guthoff, David J. Greenblatt, Hermann R. Ochs, and Roland Gugler

Subjects
Adult, Male, Digoxin, medicine.medical_specialty, Metabolic Clearance Rate, Renal function, Infarction, QT interval, Bretylium, Internal medicine, medicine, Humans, Repolarization, cardiovascular diseases, Cimetidine, business.industry, Drug interaction, medicine.disease, Kinetics, Endocrinology, Creatinine, cardiovascular system, Cardiology, Cardiology and Cardiovascular Medicine, business, medicine.drug
Abstract

infarction is not known. Moreover, the diagnosis of this arrhythmia should not be restricted to instances where delayed repolarization or extreme bradyarrhythmias are present. The therapeutic implications of this finding are unclear. Antiarrhythmic agents which potentially prolong the QT interval may be relatively contraindicated in this setting and the use of bretylium or early ventricular pacing may be preferable.

Published
1984

32. Noninteraction of Digitoxin and Quinidine

Author

Hans J. Dengler, David J. Greenblatt, Joachim Pabst, and Hermann R. Ochs

Subjects
Adult, Male, Quinidine, Digoxin, Digitoxin, Administration, Oral, Pharmacology, polycyclic compounds, medicine, Humans, Distribution (pharmacology), Drug Interactions, Infusions, Parenteral, Cardiac glycoside, business.industry, General Medicine, carbohydrates (lipids), Clinical Practice, Kinetics, Anesthesia, Female, business, Pharmacokinetic interaction, Half-Life, medicine.drug
Abstract

A LARGE and clinically important interaction between digoxin and quinidine is now well documented.1 2 3 4 5 The cardiac glycoside digitoxin is extensively used in clinical practice, but its interaction with quinidine has not been definitively evaluated.6 , 7 In this study, which assessed the pharmacokinetic interaction of digitoxin with quinidine, we found that simultaneous administration of quinidine had no statistically significant effect on the distribution or clearance of intravenously administered digitoxin. Methods Ten healthy male and female volunteers participated after giving informed consent (Table 1). Their ages ranged from 23 to 32 years. None had evidence of medical disease, and none were taking medications . . .

Published
1980

33. Interaction of ibuprofen with the H-2 receptor antagonists ranitidine and cimetidine

Author

David J. Greenblatt, Rita Matlis, Jutta Weinbrenner, and Hermann R. Ochs

Subjects
Adult, Male, Biological Availability, Ibuprofen, Pharmacology, Ranitidine, Histamine H2 receptor, medicine, Humans, Pharmacology (medical), Drug Interactions, Dosing, Cimetidine, Receptor, Chromatography, High Pressure Liquid, Analysis of Variance, Chemistry, organic chemicals, Significant difference, Drug interaction, Kinetics, Female, medicine.drug
Abstract

The influences of cimetidine and ranitidine on single-dose ibuprofen kinetics were evaluated. Thirteen healthy subjects took a single, 600 mg oral dose of ibuprofen on three occasions: in the control state without drug coadministration; during concurrent dosing with cimetidine, 1.2 gm/day; and during concurrent dosing with ranitidine, 150 mg twice daily. Compared with the control state, cimetidine increased the peak serum ibuprofen concentration (64 vs. 56 micrograms/ml), but the value during ranitidine dosing (57 micrograms/ml) was indistinguishable from the control value. There were no significant differences between control, cimetidine, and ranitidine conditions in ibuprofen elimination t1/2 (2.1, 2.1, and 2.0 hours, respectively). Overall there was a significant difference among the control, cimetidine, and ranitidine conditions in ibuprofen oral clearance (52.8, 48.3, and 54.1 ml/min, respectively), but individual differences in cimetidine vs. control and between ranitidine vs. control were not statistically significant. The impairment of ibuprofen clearance by cimetidine is small, and ranitidine had no detectable effect on ibuprofen kinetics. These findings should be further validated during chronic dosing with ibuprofen.

Published
1985

34. Diazepam kinetics in relation to age and sex

Author

Helmut Feyerabend, Hans J. Dengler, Hermann R. Ochs, Marcia Divoll, David J. Greenblatt, and Darrell R. Abernethy

Subjects
Adult, Male, medicine.medical_specialty, Age and sex, Sex Factors, Pharmacokinetics, Internal medicine, Medicine, Distribution (pharmacology), Humans, Young male, Aged, Pharmacology, Volume of distribution, Diazepam, business.industry, Age Factors, General Medicine, Middle Aged, Blood proteins, Kinetics, Endocrinology, Free fraction, Female, business, medicine.drug
Abstract

27 male volunteers aged 20 to 91 years, and 13 female volunteers aged 21 to 33 years, received single 5 to 10 mg doses of diazepam intravenously. Diazepam pharmacokinetics were determined from concentrations measured in multiple plasma samples drawn during 7 days after each dose. Diazepam elimination half-life among males (mean: 66 h) increased significantly with age (r = 0.53, p less than 0.005). Volume of distribution (mean: 1.39 liters/kg) also increased significantly with age (r = 0.67, p less than 0.001). Clearance of total diazepam in males (mean: 0.42 ml/min/kg) tended to decline with age (r = 0.32), but the association was of borderline significance (p = 0.1). Diazepam was extensively bound to plasma protein, with a mean free fraction among male subjects of 1.34%. Free fraction tended to increase with age (r = 0.14). Correction of volume of distribution and clearance for individual differences in binding did not alter the conclusions. Compared to young males, young females had larger volumes of distribution (1.87 vs. 1.34 liters/kg) and higher total clearance (0.63 vs. 0.49 ml/min/kg). These differences were even greater after correction for sex-related changes in protein binding. Elimination half-life did not differ between sexes. Since both age and sex can influence diazepam disposition, both should be considered as independent variables in studies of diazepam pharmacokinetics.

Published
1981

35. Single- and multiple-dose kinetics of intravenous digoxin

Author

Gunther Bodem, Hermann R. Ochs, and David J. Greenblatt

Subjects
Pharmacology, Volume of distribution, Adult, Male, Digoxin, Time Factors, Chemistry, Kinetics, Washout, Multiple dose, Drug accumulation, Washout period, Urinary excretion, Injections, Intravenous, medicine, Humans, Pharmacology (medical), Infusions, Parenteral, medicine.drug, Half-Life
Abstract

Nine healthy men received 0.5, 1.0, and 1.5 mg digoxin intravenously in random sequence on occasions separated by at least 4 wk. Digoxin concentrations were measured in serum samples drawn during 36 hr after each dose, and a mean across-dose kinetic profile was determined for each subject. After a 6-mo washout period, the same subjects received 0.25 mg digoxin intravenously every 24 hr for 10 consecutive days. Samples were drawn every 12 hr during the first 9 days and at multiple points during 72 hr after the last dose. Mean kinetic variables for the single- and multiple-dose trials were as follows: elimination half-life (t½), 27.9 and 38.0 hr (r = 0.62); volume of distribution, 5.5 and 7.4 l/kg (r = −0.56); total clearance, 2.50 and 2.49 ml/min/kg (r = 0.19); urinary excretion t½, 40.9 and 37.9 hr (r = −0.14). Mean observed and predicted predose steady-state serum concentrations were 0.59 and 0.79 ng/ml (r = −0.02). Mean values of accumulation and elimination t½ were nearly identical (27.8 and 27.9 hr), but were not positively correlated (r = −0.64). Multiple-dose digoxin therapy leads to no systematic change in digoxin clearance. Single-dose kinetics is poorly predictive of the rate and extent of drug accumulation and of washout kinetics during and after multiple-dose therapy. Clinical Pharmacology and Therapeutics (1980) 28, 340–345; doi:10.1038/clpt.1980.171

Published
1980

36. Intravenous quinidine: pharmacokinetic properties and effects on left ventricular performance in humans

Author

Hermann R. Ochs, Eberhard Grube, David J. Greenblatt, Elaine Woo, and Gunther Bodem

Subjects
Quinidine, Adult, Male, medicine.medical_specialty, Heart Ventricles, Blood Pressure, QRS complex, Electrocardiography, Pharmacokinetics, Heart Rate, Internal medicine, Heart rate, medicine, Humans, Volume of distribution, Ejection fraction, medicine.diagnostic_test, business.industry, Myocardial Contraction, Kinetics, Nasal Mucosa, Blood pressure, Echocardiography, Anesthesia, Injections, Intravenous, Cardiology, Female, Cardiology and Cardiovascular Medicine, business, medicine.drug
Abstract

Ten healthy volunteers received 300 mg. of quinidine base as the gluconate salt by 15-minute intravenous infusion. Physiologic variables monitored before, during, and for 24 hours after the infusion were: electrocardiogram, systolic and diastolic blood pressure, echocardiogram, and carotid pulse tracing. During quinidine infusion, mean ventricular rate increased by 18% (67.1 to 79.5 beats per minute) and corrected QT interval increased by 54% (0.44 to 0.68 sec.). QRS duration did not change significantly, nor did systolic or diastolic blood pressure. Ejection fraction (EF) measured by echocardiography did not decrease during quinidine infusion, but rather increased by 12% (0.58 to 0.65). Mean rate of circumferential fiber shortening (Vcf) likewise increased by 22%, from 1.15 to 1.40 per second. Over the 24-hours post-infusion, all monitored physiologic variables fluctuated considerably; in the case of EF and Vcf, apparently random variations over time were as great as those attributable to quinidine infusion. Mean (and range) kinetic variables for quinidine were: volume of distribution, 2.03 (1.47 to 3.00) liter/Kg.; elimination half-life, 6.3 (4.8 to 7.9) hours; total clearance, 3.8 (2.8 to 5.2) ml./min./Kg. Neither total nor unbound serum quinidine concentrations were significantly correlated with physiologic changes. Thus, intravenous quinidine in the doses studied did not have negative inotropic effects in a series of healthy humans.

Published
1980

37. Nifedipine: kinetics and dynamics after single oral doses

Author

Hermann R. Ochs, K. D. Rämsch, Birgitt Verburg-Ochs, J. Gerloff, and David J. Greenblatt

Subjects
Oral dose, Adult, Male, Nifedipine, Kinetics, Hemodynamics, Administration, Oral, Blood Pressure, Absorption (skin), Pharmacology, Placebo, Eating, Pharmacokinetics, Heart Rate, Drug Discovery, Medicine, Humans, Genetics (clinical), Clinical Trials as Topic, business.industry, General Medicine, Fasting, Myocardial Contraction, Blood pressure, Molecular Medicine, Female, business, medicine.drug
Abstract

Serum nifedipine concentrations and hemodynamic changes were evaluated in ten healthy volunteers after a single 40-mg oral dose of nifedipine. Peak serum concentrations averaged 45 micrograms/l, attained 2.7 h after dosage. The mean elimination half-life was 5.9 h (range: 3-12 h). Blood pressure, ventricular rate, and echocardiographically-determined rate of circumferential fiber shortening did not differ between placebo and nifedipine trials. Five additional subjects ingested nifedipine once in the control state and on a second occasion with a standard breakfast. Coingestion of food delayed the peak serum nifedipine concentration but did not alter the area under the serum concentration curve. Thus the pharmacokinetic profile of nifedipine indicates that a three- or four-times-daily dose is, in general, appropriate in clinical practice. Completeness of absorption is not altered by coadministration with food. Adverse hemodynamic effects of single oral doses in healthy persons are not evident.

Published
1984

38. Clorazepate dipotassium and diazepam in renal insufficiency: serum concentrations and protein binding of diazepam and desmethyldiazepam

Author

David J. Greenblatt, Hans J. Kaschell, Hermann R. Ochs, and Hans Werner Rauh

Subjects
Adult, Male, medicine.medical_specialty, Resuscitation, Nordazepam, Pharmacokinetics, Internal medicine, medicine, Clorazepate, Distribution (pharmacology), Humans, Clorazepate Dipotassium, Aged, Diazepam, Dose-Response Relationship, Drug, business.industry, Middle Aged, Dose–response relationship, Kinetics, Endocrinology, Anti-Anxiety Agents, Free fraction, Kidney Failure, Chronic, Female, business, medicine.drug, Protein Binding
Abstract

5 patients with chronic renal failure on maintenance hemodialysis and 5 healthy matched controls received single 20-mg intravenous doses of clorazepate dipotassium. Clearance of pharmacologically active unbound desmethyldiazepam was reduced in renal failure patients as opposed to controls, and free fraction in serum was greater. Since desmethyldiazepam distribution was reduced in renal patients, elimination half-life was actually shorter than in controls (36 vs. 57 h). In 10 dialysis patients receiving chronic diazepam treatment (5-15 mg/day), steady-state concentrations of diazepam (56 ng/ml) and desmethyldiazepam (77 ng/ml) were significantly lower than in age- and weight-matched controls receiving similar doses (189 and 216 ng/ml, respectively). However after correction for the higher free fractions of both compounds in renal patients as opposed to controls, steady-state concentrations of unbound drug were found to be similar between groups. Interpretation of kinetic variables and steady-state serum concentrations of extensively protein-bound drugs requires consideration of alterations in protein binding that may occur in disease states.

Published
1984

39. The interactions of propranolol and ketanserin

Author

L Labedzky, Michael Höller, Hermann R. Ochs, and David J. Greenblatt

Subjects
Pharmacology, Volume of distribution, Adult, Male, medicine.medical_specialty, Ketanserin, Chemistry, Antagonist, Propranolol, Excretion, Kinetics, Endocrinology, Propranolol Hydrochloride, Pharmacokinetics, Oral administration, Internal medicine, medicine, Humans, Pharmacology (medical), Drug Interactions, medicine.drug
Abstract

Ten healthy volunteers received a single 10 mg intravenous dose of the 5-hydroxytryptamine-2 serotonin antagonist ketanserin in the control state and again during coadministration of propranolol, 80 mg b.i.d. There were no differences between control and propranolol treatment conditions in ketanserin volume of distribution (5.2 vs. 3.8 L/kg), elimination half-life (6.6 vs. 4.7 hours), clearance (9.7 vs. 10.0 ml/min/kg), or 72-hour excretion of intact ketanserin (0.7% vs. 0.7% of dose) or ketanserinol (21.8% vs. 24.9% of dose). In a second study, eight volunteers received a 160 mg oral dose of propranolol hydrochloride in the control state and again during treatment with ketanserin, 40 mg b.i.d. There were no significant differences between control and ketanserin conditions in the time of peak serum propranolol concentration (2.1 vs. 1.5 hours after dosage) or elimination half-life (3.8 vs. 4.1 hours). However, ketanserin increased peak serum propranolol concentrations (169 vs. 233 ng/ml) and reduced oral clearance (39 vs. 27 ml/min/kg); the differences were not statistically significant (0.05 less than P less than 0.1) with a sample size of eight. Thus therapeutic doses of propranolol in healthy volunteers do not alter the kinetics of a single dose of ketanserin. Therapeutic doses of ketanserin may impair oral clearance of propranolol, leading to increased area under the serum concentration curve and higher peak serum levels.

Published
1987

40. Clinical pharmacokinetics of quinidine

Author

Hermann R. Ochs, Elaine Woo, and David J. Greenblatt

Subjects
Quinidine, Adult, Adolescent, Metabolic Clearance Rate, Administration, Oral, Pharmacology, Injections, Intramuscular, Specimen Handling, chemistry.chemical_compound, Pharmacokinetics, Quinidine Sulfate, medicine, Humans, Pharmacology (medical), Drug Interactions, Dihydroquinidine, Biotransformation, Aged, Volume of distribution, Heart Failure, Chromatography, Liver Diseases, Albumin, Age Factors, Middle Aged, Blood proteins, Kinetics, Spectrometry, Fluorescence, chemistry, Renal physiology, Injections, Intravenous, Kidney Diseases, medicine.drug, Protein Binding
Abstract

The elimination of quinidine is accomplished by a combination of renal excretion of the intact drug (15 to 40% of total clearance) and hepatic biotransformation to a variety of metabolites (60 to 85% of total clearance). Many of the metabolites appear to be pharmacologically active. Typical ranges for kinetic properites of quinidine in healthy persons are: apparent volume of distribution 2.0 to 3.5 litres/kg; elimination half-life 5 to 12 hours; clearance, 2.5 to 5.0 ml/min/kg. Quinidine clearance is reduced in the elderly, in patients with cirrhosis, and in those with congestive heart failure. Oral quinidine is available either as relatively rapidly absorbed conventional tablets (usually quinidine sulphate) or as a variety of slowly absorbed sustained release preparations. Absolute systemic availability generally is 70% or greater. Quinidine is 70 to 95% bound to plasma protein, primarily to albumin but also to a number of other plasma constituents. Binding is reduced in patients with cirrhosis, partly because of hypoalbuminaemia, but is not influenced by renal insufficiency. Clinical interpretation of total serum or plasma quinidine concentrations must be altered in patients with reduced or increased binding, since it is the unbound fraction which is pharmacologically active.

Published
1980

41. Disposition of oxazepam in relation to age, sex, and cigarette smoking

Author

David J. Greenblatt, Hermann R. Ochs, and H. Otten

Subjects
Adult, Male, medicine.medical_specialty, Aging, Smoking habit, Metabolic Clearance Rate, Sex Factors, Pharmacokinetics, Cigarette smoking, Internal medicine, Drug Discovery, medicine, Humans, Genetics (clinical), Aged, Volume of distribution, Plasma samples, Chemistry, Oxazepam, Smoking, General Medicine, Middle Aged, Kinetics, Endocrinology, Intestinal Absorption, Anesthesia, Plasma concentration, Molecular Medicine, Female, medicine.drug
Abstract

The kinetics of single 30-mg oral doses of oxazepam were determined in 22 male and nine female volunteers aged 20-86 years. Oxazepam plasma concentrations were measured in multiple plasma samples drawn during 36 h after each dose. Mean kinetic variables in males and females, respectively, were: elimination half-life, 7.5 and 8.5 h; volume of distribution, 0.96 and 1.17 l/kg; clearance, 1.48 and 1.70 ml/min/kg. Sex differences were not significant, nor were any of the kinetic variables significantly related to age. However, oxazepam clearance increased significantly with heavier cigarette smoking (r = 0.48, p less than 0.01). Mean clearance in smokers (1.98 ml/min/kg) was significantly higher than in nonsmokers (1.23 ml/min/kg, p less than 0.01). Thus, smoking is a more important determinant of oxazepam clearance than age or sex.

Published
1981

42. Kinetics of high-dose i.v. diazepam

Author

H. Stoeckel, Kuno Rommelsheim, Hermann R. Ochs, Lauven Pm, and David J. Greenblatt

Subjects
Adult, Male, Critical Care, Metabolite, Nordazepam, Pharmacology, law.invention, chemistry.chemical_compound, law, medicine, Humans, Diazepam, business.industry, Half-life, Washout, Middle Aged, Intensive care unit, Kinetics, Anesthesiology and Pain Medicine, chemistry, Underlying disease, Anesthesia, Plasma concentration, Injections, Intravenous, business, medicine.drug, Half-Life
Abstract

The pharmacokinetics of high-dose i.v. diazepam were studied in two patients in an intensive care unit. The first patient received up to 240 mg of diazepam daily for 21 days while the second received 60 mg daily for 30 days. Plasma concentrations of diazepam and its major metabolite, desmethyldiazepam, were very large but, despite severe underlying disease and simultaneous administration of several other drugs, the half-lives of diazepam and desmethyldiazepam washout were consistent with those found in healthy persons. Washout half-lives in the first patient were, if anything, shorter than expected, possibly caused by simultaneous administration of phenobarbitone. Thus the kinetics of diazepam are apparently not altered by administration of large doses.

Published
1982

43. Kinetics of 1,2-dinitroglycerin following sustained release nitroglycerin: influence of propranolol and metoprolol

Author

Hermann R. Ochs, Birgitt Verburg-Ochs, and David J. Greenblatt

Subjects
Adult, Metabolic Clearance Rate, Metabolite, Kinetics, Propranolol, Pharmacology, chemistry.chemical_compound, Nitroglycerin, Pharmacokinetics, Drug Discovery, medicine, Humans, Drug Interactions, Metaproterenol, Genetics (clinical), Biotransformation, Metoprolol, Area under the curve, General Medicine, chemistry, Pharmacodynamics, Delayed-Action Preparations, Molecular Medicine, medicine.drug
Abstract

Ten healthy volunteers ingested a single 18-mg oral dose of sustained release nitroglycerin (TNG) (Giulini-Pharma) on three occasions: once in the control state, once during coadministration of propranolol (80-mg three times daily), and once during coadministration of metoprolol (100-mg twice daily). The degree of beta adrenergic blockade was evaluated by the metaproterenol infusion test. Plasma concentration of TNG and its major metabolite, 1,2-dinitroglycerin (DNG), during 12 h after each dose were measured by gas chromatography-mass spectrometry. Intact TNG was not detected in the plasma of any patient. The major metabolite, DNG, was easily measurable in blood, and had a biphasic plasma concentration profile. Coadministration of the beta-blockers had no influence on any of the kinetic variables for DNG. The mean values during control, propranolol, and metoprolol trials of DNG elimination half-life were: 1.35, 1.10, and 1.09 h; total area under the curve: 42, 38, and 42 ng/ml × h; oral clearance: 6.6, 7.2, and 6.4 liters/min. Thus TNG when administered as a sustained release oral preparation is rapidly and completely transformed to DNG. There was no pharmacokinetic interaction between sustained release TNG and two commonly used beta-blocking agents, suggesting that any clinical interaction that may-occur between sustained release nitroglycerin and beta-blocking agents is pharmacodynamic rather than pharmacokinetic in nature.

Published
1985

44. Pharmacokinetics and dynamics of penbutolol in humans: evidence for pathway-specific stereoselective clearance

Author

P. Hajdú, Hermann R. Ochs, and David J. Greenblatt

Subjects
Cardiac function curve, Adult, Male, Metabolic Clearance Rate, Metabolite, Administration, Oral, Pharmacology, Placebo, Propanolamines, chemistry.chemical_compound, Pharmacokinetics, Penbutolol, Oral administration, Drug Discovery, medicine, Humans, Genetics (clinical), Biotransformation, Chromatography, High Pressure Liquid, Stereoisomerism, General Medicine, Kinetics, Blood pressure, chemistry, Pharmacodynamics, Molecular Medicine, Female, medicine.drug, Half-Life
Abstract

The pharmacokinetics and dynamics of the D- and L-isomers of the beta-adrenergic blocking agent penbutolol were investigated in healthy human volunteers. In Study One, subjects received a single 40-mg oral dose of L-penbutolol (the pharmacologically active stereoisomer), and matching placebo on two occasions. A mean peak serum penbutolol concentration of 268 ng/ml was reached at 0.9 h after dosing. Elimination half-life averaged 1.6 h, and total clearance 16.6 ml/min per kg body weight. Changes in blood pressure, ventricular rate, and rate of circumferential fiber shortening (Vcf) did not differ between L-penbutolol and placebo. In Study Two, subjects received 40 mg D-penbutolol, L-penbutolol, and placebo on three occasions. Total clearance of D-penbutolol was higher than for the L-isomer (43.7 vs 15.9 ml/min/kg; P less than 0.01); this was reflected in correspondingly increased area under the serum concentration curve for conjugates of the oxidized metabolite 4-hydroxy penbutolol (2.25 vs 0.66 micrograms/ml X h; P less than 0.005). In contrast, direct conjugates of L-penbutolol achieved higher serum concentrations than conjugates of D-penbutolol. Alterations in blood pressure, ventricular rate, and Vcf for D-penbutolol, L-penbutolol, and placebo were quantitatively small. Thus the clearance of penbutolol after oral administration in humans is stereoselective, but the oxidative pathway is more stereosensitive than the parallel conjugative pathway. Penbutolol causes minimal alterations in parameters of cardiac function after single 40-mg doses in healthy humans.

Published
1986

45. Bromazepam pharmacokinetics: influence of age, gender, oral contraceptives, cimetidine, and propranolol

Author

Ethan S. Burstein, Hylar L Friedman, David J. Greenblatt, Hermann R. Ochs, Ann Locniskar, Jerold S. Harmatz, and Richard I. Shader

Subjects
Adult, Male, medicine.medical_specialty, Aging, Population, Administration, Oral, Contraceptives, Oral, Hormonal, Pharmacokinetics, Oral administration, Internal medicine, medicine, Humans, Pharmacology (medical), Drug Interactions, Cimetidine, education, Volunteer, Bromazepam, Aged, Pharmacology, Volume of distribution, education.field_of_study, Sex Characteristics, business.industry, Propranolol, Kinetics, Endocrinology, Anti-Anxiety Agents, Anesthesia, Female, business, Blood sampling, medicine.drug
Abstract

Pharmacokinetics of the benzodiazepine bromazepam were evaluated in volunteer subjects who received single 6 mg oral doses followed by blood sampling during the next 48 hours. Age and gender effects were studied in 32 subjects, divided into young (aged 21 to 29 years) and elderly (aged 60 to 81 years) groups. Compared with young subjects, the elderly had significantly higher peak serum bromazepam concentrations (132 vs. 82 ng/ml), smaller volume of distribution (0.88 vs. 1.44 L/kg), lower oral clearance (0.41 vs. 0.76 ml/min/kg), and increased serum free fraction (34.8% vs. 28.8% unbound). However, gender had no significant influence on bromazepam kinetics. In 11 young female users of oral contraceptive steroids, compared with seven age- and weight-matched control women not using oral contraceptives, no differences in bromazepam kinetics were observed. Coadministration of cimetidine (1.2 gm daily) significantly reduced bromazepam clearance (0.41 vs. 0.82 ml/min/kg) and prolonged elimination half-life (29 vs. 23 hours). Propranolol (160 mg daily) significantly prolonged bromazepam half-life (28 vs. 23 hours), but the reduction in clearance associated with propranolol (0.65 vs. 0.82 ml/min/kg) did not reach significance. Bromazepam has the pharmacokinetic characteristics of benzodiazepines with half-life values between 20 and 30 hours. Consistent with its biotransformation pathway by hepatic microsomal oxidation, bromazepam clearance is significantly impaired in elderly individuals, by coadministration of cimetidine and possibly propranolol.

Published
1987

46. Dose-independent pharmacokinetics of digoxin in humans

Author

Gunther Bodem, Hermann R. Ochs, David J. Greenblatt, and Jerold S. Harmatz

Subjects
Adult, Male, medicine.medical_specialty, Digoxin, Urology, Renal function, Urine, Pharmacokinetics, Medicine, Humans, Infusions, Parenteral, Volume of distribution, Clinical Trials as Topic, Dose-Response Relationship, Drug, business.industry, Radioimmunoassay, Venous blood, Crossover study, Kinetics, Anesthesia, Cardiology and Cardiovascular Medicine, business, medicine.drug, Half-Life
Abstract

Nine healthy male volunteers received single 0.5, 1.0, and 1.5 mg. doses of intravenous digoxin in a randomized three-way crossover study. Multiple venous blood samples were drawn during 35 hours after each dose, and all urine was collected for 6 consecutive days. Concentrations of digoxin in serum and urine were determined by radioimmunoassay. Over-all mean values for kinetic variables were: distribution half-life, 0.35 hours; elimination half-life, 27.9 hours; volume of distribution, 5.46 liters/Kg; total clearance, 2.51 ml./min./Kg. The mean projected cumulative urinary excretion of digoxin was 70.1% of the dose; mean renal clearance of digoxin was 1.71 ml./min./Kg., not significantly different from creatinine clearance (1.50 ml./min./Kg.). None of the identifiable pharmacokinetic variables was significantly influenced by dose, suggesting that digoxin disposition is dose-independent in healthy individuals.

Published
1978

47. Repeated diazepam dosing in cirrhotic patients: cumulation and sedation

Author

Jerold S. Harmatz, Bernd Eckardt, Richard I. Shader, David J. Greenblatt, and Hermann R. Ochs

Subjects
Adult, Liver Cirrhosis, Male, Cirrhosis, Sedation, Metabolite, Nordazepam, law.invention, chemistry.chemical_compound, law, Mood state, Medicine, Humans, Hypnotics and Sedatives, Pharmacology (medical), Dosing, Pharmacology, Clinical pharmacology, Diazepam, business.industry, Middle Aged, medicine.disease, Psychiatry and Mental health, Kinetics, chemistry, Anesthesia, Sedative Effects, medicine.symptom, business, medicine.drug, Half-Life
Abstract

Five medically stable male patients with cirrhosis and four healthy age- and sex-matched controls received single 5-mg oral doses of diazepam (DZ) daily for 22 consecutive days. Plasma concentrations of DZ and its major metabolite desmethyldiazepam (DMDZ) were measured daily during the period of dosing and in the 7-day washout period that followed. Clinical self-ratings of sedation, fatigue, mood state, and sleep patterns were obtained daily during the period of dosage with the use of visual analogue scales. Steady-state plasma DZ concentrations were higher (165 and 98 ng/ml), and DMDZ concentrations tended to be higher (399 and 206 ng/ml), in cirrhotics than in controls. Increases in self-rated daytime sedation also were greater in cirrhotics than in controls and correlated strongly with total DZ and DMDZ plasma concentration during the first 2 wk of diazepam dosing. Thus, reduced clearance of DZ in cirrhotics leads to increased cumulation during long-term dosing. This in turn is associated with increased clinical sedation. Sedative effects are partly offset as treatment proceeds because of adaptation or tolerance. Based on kinetic findings, diazepam can be given safely to cirrhotic patients provided daily dosage is reduced by approximately 50%. Clinical Pharmacology and Therapeutics (1983) 33, 471–476; doi:10.1038/clpt.1983.64

Published
1983

48. Pharmacokinetics and CSF entry of flurazepam in dogs

Author

Hermann R. Ochs, Wolfgang Eichelkraut, Norbert Hahn, Ethan S. Burstein, and David J. Greenblatt

Subjects
Pharmacology, Volume of distribution, Flurazepam, Metabolite, Area under the curve, Half-life, General Medicine, Flurazepam Hydrochloride, chemistry.chemical_compound, Kinetics, Cerebrospinal fluid, Dogs, chemistry, Pharmacokinetics, medicine, Animals, medicine.drug, Half-Life
Abstract

Anesthetized dogs received a single 1.0-mg/kg intravenous dose of flurazepam hydrochloride, following which multiple blood and cerebrospinal fluid (CSF) samples were taken over the next 8 h. Concentrations of flurazepam and its metabolite, desalkylflurazepam, were determined by gas chromatography with electron-capture detection. Mean kinetic variables for flurazepam were: volume of distribution 7.9 l/kg, elimination half-life 2.3 h, clearance 37 ml/min/kg, serum free fraction 25% unbound. The metabolic product desalkylflurazepam appeared in serum in low concentrations, and was eliminated with a half-life of 4.9 h. Flurazepam rapidly entered CSF, then was eliminated in parallel with flurazepam in serum. However, the extent of entry into CSF was limited, with the mean ratio of area under the curve for CSF versus serum (0.24) nearly identical to the serum free fraction. Thus, intravenous flurazepam in dogs is characterized by extensive distribution, high clearance, and short half-life. Entry into CSF is rapid, and appears governed by passive diffusion. The extent of CSF entry is limited by protein binding in serum.

Published
1988

49. Is temazepam an accumulating hypnotic?

Author

David J. Greenblatt, Heinz Heuer, and Hermann R. Ochs

Subjects
Pharmacology, Volume of distribution, Adult, Male, Benzodiazepine, medicine.drug_class, Temazepam, Chemistry, Half-life, Liter, Absorption, Hypnotic, Kinetics, Pharmacokinetics, Anti-Anxiety Agents, Anesthesia, medicine, Humans, Hypnotics and Sedatives, Pharmacology (medical), Female, Volunteer, medicine.drug, Half-Life
Abstract

Ten healthy volunteers aged 22 to 30 years received a single 20-mg oral dose of temazepam. Serum temazepam concentrations were measured by gas chromatography at multiple times during the next 48 hours. Mean kinetic variables were: volume of distribution, 1.45 liter/kg; elimination half-life, 8.6 hours; total clearance, 2.33 ml/min/kg. The subjects then received 20 mg temazepam once daily for seven consecutive days. Serum concentrations were measured just prior to each dose and at multiple time points after the last dose. Predose serum levels increased during the first three days of dosage, then increased no further. Mean values measured 24 hours after doses 1 through 6, respectively, were 33, 43, 55, 47, 53, and 51 ng/ml. Based on the area under the serum concentration curve after the last dose compared with that after the first dose, the mean accumulation ratio was 1.32, which was significantly greater than unity. The extent of accumulation was consistent with that predicted from the single-dose study. Postdosage washout half-life averaged 10.2 hours. Thus, temazepam has a pharmacokinetic profile of an intermediate half-life benzodiazepine that produces an intermediate degree of accumulation with multiple dosage.

Published
1984

50. Influence of age, gender, and obesity on salicylate kinetics following single doses of aspirin

Author

Richard I. Shader, Hermann R. Ochs, Jerold S. Harmatz, Harold Boxenbaum, Darrell R. Abernethy, Rita Matlis, and David J. Greenblatt

Subjects
Adult, Male, medicine.medical_specialty, Immunology, Administration, Oral, Multiple dosing, chemistry.chemical_compound, Sex Factors, Rheumatology, Internal medicine, medicine, Immunology and Allergy, Humans, Pharmacology (medical), Infusions, Parenteral, Obesity, Young female, Aged, Volume of distribution, Aspirin, business.industry, Body Weight, Age Factors, medicine.disease, Salicylates, Kinetics, Endocrinology, Peak plasma, chemistry, Free fraction, Female, business, Salicylic Acid, Salicylic acid, medicine.drug
Abstract

Salicylate kinetics following single, 650-mg intravenous and oral doses of aspirin were evaluated in humans in 2 studies. Complete conversion of aspirin to salicylate was assumed. The first study involved 25 young (25-40 years) and 21 elderly (66-89 years) healthy male and female volunteers. Mean salicylate clearance was lower in elderly females compared with that in young females; however, the difference between young men and elderly men was not significant. Salicylate free fraction in plasma increased significantly with age in men and women. After correction for free fraction, unbound mean clearance was reduced in elderly men compared with young men, and in elderly women compared with young women. Peak plasma salicylate concentrations after taking oral aspirin were not significantly influenced by age, and systemic availability of salicylate in all groups was complete. The second study compared 20 obese subjects (mean weight 113 kg) with 20 normal weight controls (mean weight 67 kg) matched for age, sex, height, and smoking habits. Small differences between obese and control groups were observed in total salicylate volume of distribution (Vd), unbound Vd, and mean clearance of total or unbound salicylate. Following normalization for total weight, however, values of total Vd and mean clearance were significantly smaller in obese subjects than in normal weight subjects. Rate and completeness of salicylate absorption were not influenced by obesity when aspirin was ingested, although peak levels were lower in obese subjects. If applied to multiple doses, the reduced unbound clearance of salicylate in the elderly would imply increased accumulation unless doses are appropriately adjusted downward. During long-term therapy, salicylate dosage for obese individuals should not be adjusted upward in proportion to total weight.

Published
1986

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