Phase I study of sequentially administered topoisomerase I inhibitor (irinotecan) and topoisomerase II inhibitor (etoposide) for metastatic non-small-cell lung cancer

被引：28

作者：

Ando, M

Eguchi, K

Shinkai, T

Tamura, T

Ohe, Y

Yamamoto, N

Kurata, T

Kasai, T

Ohmatsu, H

Kubota, K

Sekine, I

Hojo, N

Matsumoto, T

Kodama, T

Kakinuma, R

Nishiwaki, Y

Saijo, N

机构：

[1] NATL SHIKOLU CANC CTR HOSP,DEPT MED ONCOL,MATSUYAMA,EHIME 790,JAPAN

[2] NATL CANC CTR,DEPT MED ONCOL,CHUO KU,TOKYO 104,JAPAN

[3] NATL CANC CTR,DIV PHARMACOL,CHUO KU,TOKYO 104,JAPAN

[4] NATL CANC CTR HOSP,DEPT MED ONCOL,CHIBA 277,JAPAN

来源：

BRITISH JOURNAL OF CANCER | 1997年 / 76卷 / 11期

关键词：

irinotecan; Topo I and II inhibitors; sequential administration;

D O I：

10.1038/bjc.1997.584

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

We conducted a phase I study of irinotecan (CPT-11) and etoposide (VP-16) given sequentially to untreated patients with metastatic non-small-cell lung cancer. Arm A: CPT-11 was given over 90 min on days 1-3 and VP-16 was given over 60 min on days 4-6. Arm B: VP-16 was given on days 1-3 and CPT-11 on days 4-6. G-CSF was given to all patients daily on days 7-17. Twenty-seven patients were entered randomly at the two arms. The major dose-limiting toxicities in arms A and B were granulocytopenia and diarrhoea, Transient elevations of transaminases and bilirubin were observed in both arms. The degree of the toxicities did not differ between the two arms. The maximum tolerated doses (MTDs) were 60 mg m(-2) CPT-11 and 60 mg m(-2) VP-16 in both arms. Of the 13 patients who received more than two cycles, two out of five achieved partial response (PR) at the first level of arm A and one out of four achieved PR at the second level of arm B. We conclude that these schedules of sequential CPT-11 and VP-16 administration were inappropriate because of severe toxicities.

引用

页码：1494 / 1499

页数：6

共 19 条

[1] SEQUENTIAL ADMINISTRATION OF CAMPTOTHECIN AND ETOPOSIDE CIRCUMVENTS THE ANTAGONISTIC CYTOTOXICITY OF SIMULTANEOUS DRUG ADMINISTRATION IN SLOWLY GROWING HUMAN COLON-CARCINOMA HT-29 CELLS [J].

BERTRAND, R ;

OCONNOR, PM ;

KERRIGAN, D ;

POMMIER, Y .

EUROPEAN JOURNAL OF CANCER, 1992, 28A (4-5) :743-748

[2]

ECKARDT JR, 1993, P AN M AM SOC CLIN, V12, P137

[3] A PHASE-II STUDY OF CPT-11, A NEW DERIVATIVE OF CAMPTOTHECIN, FOR PREVIOUSLY UNTREATED NON-SMALL-CELL LUNG-CANCER [J].

FUKUOKA, M ;

NIITANI, H ;

SUZUKI, A ;

MOTOMIYA, M ;

HASEGAWA, K ;

NISHIWAKI, Y ;

KURIYAMA, T ;

ARIYOSHI, Y ;

NEGORO, S ;

MASUDA, N ;

NAKAJIMA, S ;

TAGUCHI, T ;

ASAKAWA, M ;

NAKABAYASI, T ;

NAKAI, T ;

KURITA, Y ;

KINAMERI, K ;

NOMURA, K ;

NAGAO, K ;

SAIJO, N ;

OHE, Y ;

SUGIURA, T ;

SHIMOKATA, K ;

SAKA, H ;

NEGORO, S ;

NAKAJIMA, S ;

TOHDA, Y ;

FUJII, M ;

OTA, M ;

HARA, N ;

HARA, Y ;

FUJISAWA, K ;

NAKANO, S ;

ARAKI, J ;

NIITANI, H ;

MIYATA, Y .

JOURNAL OF CLINICAL ONCOLOGY, 1992, 10 (01) :16-20

[4]

GOTO K, 1995, P AN M AM SOC CLIN, V14, P362

[5]

HANDE KR, 1990, SEMIN ONCOL, V19, P53

[6] A SENSITIVE HIGH-PERFORMANCE LIQUID-CHROMATOGRAPHIC METHOD FOR DETERMINATION OF THE ANTI-NEOPLASTIC AGENTS VP-16-213 AND VM-26 IN BIOLOGICAL-FLUIDS [J].

HOLTHUIS, JJM ;

VANOORT, WJ ;

PINEDO, HM .

ANALYTICA CHIMICA ACTA, 1981, 130 (01) :23-30

[7]

KANEDA N, 1990, CANCER RES, V50, P1721

[8] EFFECTS OF CPT-11 IN COMBINATION WITH OTHER ANTICANCER AGENTS IN CULTURE [J].

KANO, Y ;

SUZUKI, K ;

AKUTSU, M ;

SUDA, K ;

INOUE, Y ;

YOSHIDA, M ;

SAKAMOTO, S ;

MIURA, Y .

INTERNATIONAL JOURNAL OF CANCER, 1992, 50 (04) :604-610

[9] PHASE-I STUDY OF CPT-11 AND ETOPOSIDE IN PATIENTS WITH REFRACTORY SOLID TUMORS [J].

KARATO, A ;

SASAKI, Y ;

SHINKAI, T ;

EGUCHI, K ;

TAMURA, T ;

OHE, Y ;

OSHITA, F ;

NISHIO, M ;

KUNIKANE, H ;

ARIOKA, H ;

OHMATSU, H ;

NAKASHIMA, H ;

SHIRAISHI, J ;

SAIJO, N .

JOURNAL OF CLINICAL ONCOLOGY, 1993, 11 (10) :2030-2035

[10]

KAUFMANN SH, 1991, CANCER RES, V51, P1129

← 1 2 →