ETOPOSIDE PLUS CARBOPLATIN ADMIXTURE - PHASE-I STUDY OF 5-DAY OR 7-DAY CONTINUOUS INFUSION

被引：1

作者：

LOKICH, J

ANDERSON, N

BERN, M

ZIPOLI, T

GONSALVES, L

MOORE, C

机构：

[1] Cancer Center of Boston, Boston, MA 02120

来源：

AMERICAN JOURNAL OF CLINICAL ONCOLOGY-CANCER CLINICAL TRIALS | 1992年 / 15卷 / 04期

关键词：

CARBOPLATIN; CONTINUOUS INFUSION; ETOPOSIDE;

D O I：

10.1097/00000421-199208000-00008

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Thirty-five patients were entered in a Phase I trial of an admixture infusion of etoposide (VP-16) and carboplatin (CBDCA) administered continuously for 5 or 7 days. Because of the compatibility and solubility of the two agents, the treatment program could be administered on an outpatient basis. The dose rate of VP-16 was fixed at 30 mg/m2/day (total dose 150 mg/m2 for 5 days or 210 mg/m2 for seven days) for each cycle. Carboplatin was evaluated at three dose rates: 50, 60, and 75 mg/m2/day on the 5-day infusion and 40, 50, and 60 mg/m2/day on the 7-day infusion with cycles repeated at 28 to 42 days. The dose limiting toxicity was hematologic and followed a pattern typical for carboplatin, that is, delayed neutropenia and/or thrombocytopenia with a protracted leukocyte recovery. Renal toxicity was observed in three patients. The optimum total dose for the infusional carboplatin component was 300 mg/m2 (5-day) and 420 mg/m2 (7-day). The total etoposide dose was 150 mg/M2 and 210 mg/M2, which did not appear to contribute to the hematologic toxicity. Delivery of the admixture of VP-16 and CBDCA was feasible, although cumbersome, as a result of the portable delivery system. Extending the duration of infusion increases the total cumulative dose of carboplatin and etoposide that can be administered without increasing adverse effects.

引用

页码：314 / 318

页数：5

共 50 条

[31] PHASE-I STUDY OF TAXOL USING A 5-DAY INTERMITTENT SCHEDULE
LEGHA, SS
TENNEY, DM
KRAKOFF, IR
JOURNAL OF CLINICAL ONCOLOGY, 1986, 4 (05) : 762 - 766
[32] PHASE-I STUDY OF 5-DAY CONTINUOUS-INFUSION FLUORODEOXYURIDINE AND HIGH-DOSE FOLINIC ACID WITH ORAL HYDROXYUREA
RASCHKO, JW
AKMAN, SA
LEONG, LA
MARGOLIN, KA
MORGAN, RJ
NEWMAN, E
SOMLO, G
AHN, C
DOROSHOW, JH
CANCER CHEMOTHERAPY AND PHARMACOLOGY, 1994, 35 (02) : 161 - 164
[33] A PHASE-I-II STUDY OF CONTINUOUS 5-DAY INFUSION MITOMYCIN-C
YAP, HY
VALDIVIESO, M
BLUMENSCHEIN, G
HORTOBAGYI, G
BEDIKIAN, A
AMERICAN JOURNAL OF CLINICAL ONCOLOGY-CANCER CLINICAL TRIALS, 1983, 6 (01): : 109 - 112
[34] NEOCARZINOSTATIN - PHASE-I CLINICAL-TRIAL WITH 5-DAY INTERMITTENT AND CONTINUOUS INFUSIONS
MCKELVEY, EM
BURGESS, MA
MCCREDIE, KB
MURPHY, WK
BODEY, GP
CANCER, 1979, 44 (04) : 1182 - 1188
[35] A phase I study of 5-day continuous venous infusion of carboplatin at circadian rhythm-modulated rate compared with constant rate
Natoli, C
Salini, V
Irtelli, L
Martino, MT
Garufi, C
Grassadonia, A
Fiorentino, B
Iacobelli, S
ANTICANCER RESEARCH, 1996, 16 (3A) : 1275 - 1279
[36] PHASE-I TRIAL OF PCNU ADMINISTERED BY 5-DAY COURSES
EARHART, RH
KOELLER, JM
DAVIS, HL
CANCER TREATMENT REPORTS, 1981, 65 (9-10): : 835 - 840
[37] PHASE-I STUDY OF TRIMETREXATE (TMTX, TMQ, JB-11) GLUCURONATE IN A 5-DAY INFUSION SCHEDULE
ROSEN, M
OHNUMA, T
ZIMET, A
COFFEY, V
ZHANG, N
HOLLAND, JF
PROCEEDINGS OF THE AMERICAN ASSOCIATION FOR CANCER RESEARCH, 1986, 27 : 172 - 172
[38] Paclitaxel (P) as a 5-day continuous infusion in recurred head and neck cancer: A phase I study
Marmiroli, L
Ziccarelli, P
Nardone, L
Gentile, P
Salvi, G
Genovesi, D
Guidi, C
Niespolo, RM
Ausili-Cefaro, G
ANNALS OF ONCOLOGY, 1998, 9 : 104 - 104
[39] A PHASE-I AND PHARMACOKINETIC STUDY WITH 21-DAY CONTINUOUS INFUSION OF EPIRUBICIN
DEVRIES, EGE
GREIDANUS, J
MULDER, NH
NIEWEG, MB
POSTMUS, PE
SCHIPPER, DL
SLEIJFER, DT
UGES, DRA
WILLEMSE, PHB
JOURNAL OF CLINICAL ONCOLOGY, 1987, 5 (09) : 1445 - 1451
[40] A PHASE-I PHARMACOKINETIC STUDY OF 21-DAY CONTINUOUS INFUSION MITOXANTRONE
GREIDANUS, J
DEVRIES, EGE
MULDER, NH
SLEIJFER, DT
UGES, DRA
OOSTERHUIS, B
WILLEMSE, PHB
JOURNAL OF CLINICAL ONCOLOGY, 1989, 7 (06) : 790 - 797

← 1 2 3 4 5 →