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Literature DB >> 8070004

Phase I and pharmacokinetics studies of prochlorperazine 2-h i.v. infusion as a doxorubicin-efflux blocker.

K S Sridhar¹, A Krishan, T S Samy, R C Duncan, A Sauerteig, G V McPhee, M E Auguste, P W Benedetto.

Abstract

In an earlier phase I study, we reported that the maximal tolerated dose (MTD) of prochlorperazine (PCZ) given as a 15-min i.v. infusion was 75 mg/m2. The highest peak plasma PCZ concentration achieved was 1100 ng/ml. The present study was conducted to determine if PCZ levels high enough to block doxorubicin (DOX) efflux in vitro could be achieved and sustained in vivo by increasing the duration of i.v. infusion from 15 min to 2 h. The treatment schedule consisted of i.v. prehydration with at least 500 ml normal saline (NS) and administration of a fixed standard dose of 60 mg/m2 DOX as an i.v. bolus over 15 min followed by i.v. doses of 75, 105, 135, or 180 mg/m2 PCZ in 250 ml NS over 2 h. The hematologic toxicities attributable to DOX were as expected and independent of the PCZ dose. Toxicities attributable to PCZ were sedation, dryness of mouth, anxiety, akathisia, hypotension, cramps, and confusion. The MTD of PCZ was 180 mg/m2. Large interpatient variation in peak PCZ plasma levels (91-3215 ng/ml) was seen, with the plasma half-life (t1/2 alpha) being approximately 57 min in patients given 135-180 mg/m2 PCZ. The volume of distribution (Vd), total clearance (ClT), and area under the curve (AUC) were 350.1 +/- 183.8 1/m2, 260.7 +/- 142.7 l m2 h-1 and 1539 +/- 922 ng ml h-1, respectively, in patients given 180 mg/m2 PCZ and the respective values for patients receiving 135 mg/m2 were 48.9 +/- 23.76 l/m2, 33.2 +/- 2.62 l m2 h-1, and 4117 +/- 302 ng ml h-1. High PCZ plasma levels (> 600 ng/ml) were sustained in all patients treated with 135 mg/m2 PCZ for up to 24 h. DOX plasma elimination was biphasic at 135 and 180 mg/m2 PCZ, and a > 10-ng/ml DOX plasma level was maintained for 24 h. Partial responses were seen in three of six patients with malignant mesothelioma, in two of ten patients with non-small-cell lung carcinoma, and in the single patient with hepatoma. Our data show that PCZ can be safely given as a 2-h infusion at 135 mg/m2 with clinically manageable toxicities. The antitumor activity of the combination of DOX and PCZ needs to be confirmed in phase II trials.

Entities: Chemical Disease Gene Species

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Year: 1994 PMID： 8070004 DOI： 10.1007/bf00685561

Source DB: PubMed Journal: Cancer Chemother Pharmacol ISSN： 0344-5704 Impact factor: 3.333

34 in total

1. Clinical modulation of doxorubicin resistance by the calmodulin-inhibitor, trifluoperazine: a phase I/II trial.

Authors: R L Miller; R M Bukowski; G T Budd; J Purvis; J K Weick; K Shepard; K K Midha; R Ganapathi
Journal: J Clin Oncol Date: 1988-05 Impact factor: 44.544

2. Circumvention of vincristine and Adriamycin resistance in vitro and in vivo by calcium influx blockers.

Authors: T Tsuruo; H Iida; M Nojiri; S Tsukagoshi; Y Sakurai
Journal: Cancer Res Date: 1983-06 Impact factor: 12.701

3. A dose finding study of prochlorperazine as an antiemetic for cancer chemotherapy.

Authors: I N Olver; L K Webster; J F Bishop; J Clarke; B L Hillcoat
Journal: Eur J Cancer Clin Oncol Date: 1989-10

4. Verapamil and adriamycin in the treatment of drug-resistant ovarian cancer patients.

Authors: R F Ozols; R E Cunnion; R W Klecker; T C Hamilton; Y Ostchega; J E Parrillo; R C Young
Journal: J Clin Oncol Date: 1987-04 Impact factor: 44.544

5. Thaliblastine, a plant alkaloid, circumvents multidrug resistance by direct binding to P-glycoprotein.

Authors: G Chen; C Ramachandran; A Krishan
Journal: Cancer Res Date: 1993-06-01 Impact factor: 12.701

6. Active efflux of daunorubicin and adriamycin in sensitive and resistant sublines of P388 leukemia.

Authors: M Inaba; H Kobayashi; Y Sakurai; R K Johnson
Journal: Cancer Res Date: 1979-06 Impact factor: 12.701

7. Differential effect of the calmodulin inhibitor trifluoperazine on cellular accumulation, retention, and cytotoxicity of anthracyclines in doxorubicin (adriamycin)-resistant P388 mouse leukemia cells.

Authors: R Ganapathi; D Grabowski; W Rouse; F Riegler
Journal: Cancer Res Date: 1984-11 Impact factor: 12.701

Phase I and pharmacokinetics studies of prochlorperazine 2-h i.v. infusion as a doxorubicin-efflux blocker.

1. Clinical modulation of doxorubicin resistance by the calmodulin-inhibitor, trifluoperazine: a phase I/II trial.

2. Circumvention of vincristine and Adriamycin resistance in vitro and in vivo by calcium influx blockers.

3. A dose finding study of prochlorperazine as an antiemetic for cancer chemotherapy.

4. Verapamil and adriamycin in the treatment of drug-resistant ovarian cancer patients.

5. Thaliblastine, a plant alkaloid, circumvents multidrug resistance by direct binding to P-glycoprotein.

6. Active efflux of daunorubicin and adriamycin in sensitive and resistant sublines of P388 leukemia.

7. Differential effect of the calmodulin inhibitor trifluoperazine on cellular accumulation, retention, and cytotoxicity of anthracyclines in doxorubicin (adriamycin)-resistant P388 mouse leukemia cells.

8. Prochlorperazine as a doxorubicin-efflux blocker: phase I clinical and pharmacokinetics studies.

Review 9. Biological basis for cancer treatment.

10. Flow cytometric studies on modulation of cellular adriamycin retention by phenothiazines.

1. Phenothiazines and thioxanthenes inhibit multidrug efflux pump activity in Staphylococcus aureus.