Your search keyword '"Triethylenephosphoramide pharmacokinetics"' showing total 5 results

1. Pharmacokinetics of thio-TEPA and TEPA in the conventional dose-range and its correlation to myelosuppressive effects.

Author

Hagen B

Subjects

Aged, Aged, 80 and over, Bilirubin blood, Creatinine blood, Female, Humans, Leukocyte Count drug effects, Middle Aged, Ovarian Neoplasms blood, Platelet Count drug effects, Regression Analysis, Thiotepa administration & dosage, Triethylenephosphoramide administration & dosage, Bone Marrow Diseases chemically induced, Ovarian Neoplasms drug therapy, Thiotepa adverse effects, Thiotepa pharmacokinetics, Triethylenephosphoramide adverse effects, Triethylenephosphoramide pharmacokinetics

Abstract

A total of 13 patients with ovarian cancer were studied during the initial two courses of i.v. thio-TEPA treatment they underwent after primary surgery. Following an increase in the dose from 60 to 80 mg for the second course, no sign of saturation of thio-TEPA elimination processes or of formation of the metabolite TEPA occurred, indicating dose-independent pharmacokinetics. Myelosuppression after courses was registered by serial measurements of platelets and leukocytes. The time to platelet nadir was quite uniformly 3 weeks and tended to be longer than that of leukocytes, which averaged 2 weeks but showed greater interindividual variation. Linear regression analyses of pharmacokinetic parameters versus myelosuppression revealed statistically significant correlations between thio-TEPA pharmacokinetics and the percentage of reductions in leukocytes and platelets at their mean nadirs. In contrast, no such correlation could be demonstrated for TEPA despite its greater exposure to the body in terms of AUC. We advocate further investigation of this pharmacokinetic-pharmacodynamic relationship so as to establish individualized dosing of thio-TEPA.

Published

1991

2. Metabolism and alkylating activity of thio-TEPA in rat liver slice incubation.

Author

Hagen B, Dale O, Neverdal G, Azri S, and Nilsen OG

Subjects

Alkylation, Allylisopropylacetamide pharmacology, Animals, Dose-Response Relationship, Drug, In Vitro Techniques, Liver drug effects, Male, Phenobarbital pharmacology, Rats, Rats, Inbred Strains, Thiotepa analysis, Time Factors, Tissue Survival drug effects, Triethylenephosphoramide analysis, Triethylenephosphoramide pharmacokinetics, Liver enzymology, Thiotepa pharmacokinetics

Abstract

Precision-cut rat-liver slices were used to study the metabolism of the alkylating agent N,N',N''-triethylenethiophosphoramide (thio-TEPA). Exposure to high concentrations (1-10 mM) of thio-TEPA for 6 h did not prove to be toxic to the liver slices as indicated by insignificant leakage of potassium from the cells. The time course of the disappearance of thio-TEPA (initial concentration, 5.2 microM) from the buffer during incubation followed first-order kinetics. Formation of N,N'N''-triethylenephosphoramide (TEPA) apparently accounted for the elimination of thio-TEPA. Pretreatment of the rats with phenobarbital significantly increased the reaction rate. Conversely, pretreatment with the cytochrome P-450 inhibitor allylisopropylacetamide significantly reduced the metabolic rate. The elimination of thio-TEPA and formation of TEPA occurred independently of thio-TEPA concentration, which ranged from 5.2 to 104 microM. Thio-TEPA's oxo-analogue TEPA, which was not further metabolized, was the only metabolite identified. However, a significantly time-related increase in 4-(nitrobenzyl)-pyridine (NBP) alkylating activity was observed following incubation of liver slices with thio-TEPA but not after their incubation with TEPA. This may possibly indicate the formation of unknown active metabolites.

Published

1991

3. ThioTEPA pharmacokinetics during intravesical chemotherapy and the influence of Tween 80.

Author

Masters JR, McDermott BJ, Jenkins WE, Fenwick E, Shah PJ, Mundy AR, Loadman PM, and Bibby MC

Subjects

Absorption, Administration, Intravesical, Aged, Female, Humans, Hydrogen-Ion Concentration, Leukocyte Count drug effects, Male, Middle Aged, Osmolar Concentration, Random Allocation, Thiotepa administration & dosage, Triethylenephosphoramide pharmacokinetics, Carcinoma, Transitional Cell drug therapy, Polysorbates pharmacology, Thiotepa pharmacokinetics, Urinary Bladder Neoplasms drug therapy

Abstract

A pharmacokinetic study of randomised crossover design was carried out in which eight patients with recurrent stage pTa or pT1 transitional cell carcinoma of the bladder were given thioTEPA (30 mg) in distilled water or in 10% (v/v) Tween 80 (30 ml) intravesically for 2 h, followed 3 months later by the alternative treatment. ThioTEPA and its primary metabolite, TEPA, were measured in plasma and urine using a sensitive and specific chromatographic assay. Large differences between patients were observed in the proportion of thioTEPA absorbed, ranging from 20%-78%. Peak plasma levels of thioTEPA were observed within 1 h of intravesical administration. By 2 h after administration the plasma levels of TEPA were similar to those of thioTEPA and, in contrast to those of the parent compound, remained at a similar level over the next 4 h. The rate of absorption of thioTEPA was not influenced by Tween 80, but it did cause statistically significant increases in mean peak plasma levels (from 101 to 154 ng/ml) and mean AUC values (from 0.376 to 0.496 micrograms h per ml) and a decrease in the mean half-life (from 1.83 to 1.25 h). To obtain plasma levels similar to those achieved after instillation with thioTEPA alone, the dose should be reduced with Tween 80.

Published

1990

4. Long-term pharmacokinetics of thio-TEPA, TEPA and total alkylating activity following i.v. bolus administration of thio-TEPA in ovarian cancer patients.

Author

Hagen B, Neverdal G, Walstad RA, and Nilsen OG

Subjects

Adult, Aged, Aged, 80 and over, Alkylation, Female, Half-Life, Humans, Injections, Intravenous, Middle Aged, Ovarian Neoplasms metabolism, Thiotepa administration & dosage, Triethylenephosphoramide pharmacokinetics, Urine analysis, Ovarian Neoplasms drug therapy, Thiotepa pharmacokinetics

Abstract

The serum pharmacokinetics of unchanged thio-TEPA and the active metabolite TEPA and the urinary excretion of thio-TEPA, TEPA and total alkylating activity were studied after a single i.v. bolus injection of thio-TEPA in six ovarian cancer patients. TEPA was present in serum as of 5 min after drug administration, and its concentration rapidly reached a plateau in the range of 50-100 ng/ml. After about 3 h the serum concentration of TEPA exceeded that of thio-TEPA, and in five of the six patients the metabolite persisted longer than the parent drug in serum. AUCs of thio-TEPA and TEPA were 822 +/- 83 and 1,084 +/- 234 ng h/ml, respectively. The great interindividual variation encountered in the serum pharmacokinetics of TEPA may be of clinical importance and represents a further indication that pharmacokinetically guided dosing of thio-TEPA could be valuable. Urinary recoveries of both thio-TEPA and TEPA were low, together constituting less than 2% of the delivered dose. A substantial gap existed between this and the total urinary alkylating activity, which averaged 13% of the dose in terms of thio-TEPA equivalents. This gap strongly indicates the presence of other unknown metabolites.

Published

1990

5. Influence of the tissue distribution of ThioTEPA and its metabolite, TEPA, on the response of murine colon tumours.

Author

Bibby MC, McDermott BJ, Double JA, Phillips RM, Loadman PM, and Burgess L

Subjects

Adenocarcinoma metabolism, Adenocarcinoma pathology, Animals, Colonic Neoplasms metabolism, Colonic Neoplasms pathology, Female, Male, Mice, Mice, Inbred Strains, Sex Factors, Thiotepa blood, Thiotepa therapeutic use, Tissue Distribution, Triethylenephosphoramide blood, Adenocarcinoma drug therapy, Azirines pharmacokinetics, Colonic Neoplasms drug therapy, Thiotepa pharmacokinetics, Triethylenephosphoramide pharmacokinetics

Abstract

Disposition studies in the same animals as those used for assessment of antitumor and toxic effects could increase understanding of the variation in response to cytotoxic drugs. Tissue and plasma levels of ThioTEPA and triethylenephosphoramide (TEPA) were measured to see if any correlation existed between them and the effects of the drug on a series of mouse colon tumours (MAC). The tumour panel included an ascitic form (MAC 15A), an anaplastic (MAC 13) and a well-differentiated (MAC 26) solid tumour, all grown subcutaneously. The maximum tolerated dose of ThioTEPA was 20 mg kg-1 in females bearing MAC 13 and 15 mg kg-1 in males having MAC 15A or 26. The diverse growth characteristics of the tumour cell lines necessitated the use of different methods for assessment of response. After administration of the maximum tolerated dose, the greatest response was observed in MAC 26, in which a growth delay of 15 days-twice the doubling time of the tumour volume-occurred. ThioTEPA produced 58% inhibition of MAC 13 tumour weight, but MAC 15A was unresponsive. One hour after intraperitoneal administration of Thio-TEPA (20 mg kg-1), ratios of tissue to plasma concentration were 1.13, 0.87 and 1.17 in tumours and 0.80, 0.75 and 0.73 in spleens of mice bearing MAC 13, 15A and 26 respectively. These data show greater accumulation of drug in neoplastic than in normal tissues. The pattern of distribution of the metabolite was similar, but there was a lesser degree of tissue accumulation than by the drug. Concentrations of drug and metabolite in neoplastic tissues related to their protein content were 116.0, 126.3 and 183.3 micrograms ThioTEPA/g and 57.5, 83.1 and 78.6 micrograms TEPA/g in MAC 13, 15A and 26 respectively. Combination of these chemosensitivity and pharmacokinetic data indicates that differences in response of these tumours to ThioTEPA cannot be explained by the availability of the drug and metabolite. The therapeutic effects of ThioTEPA cannot be predicted purely from a knowledge of drug and metabolite disposition.

Published

1987