COMPARISON OF PACLITAXEL AND DOCETAXEL ACTIVITY ON HUMAN OVARIAN-CARCINOMA XENOGRAFTS

被引:36
作者
NICOLETTI, MI
LUCCHINI, V
DINCALCI, M
GIAVAZZI, R
机构
[1] IST RIC FARMACOL MARIO NEGRI,I-24125 BERGAMO,ITALY
[2] OSPED SAN GERARDO,MONZA,ITALY
[3] IST RIC FARMACOL MARIO NEGRI,I-20157 MILAN,ITALY
来源
EUROPEAN JOURNAL OF CANCER | 1994年 / 30A卷 / 05期
关键词
HUMAN OVARIAN CARCINOMA; NUDE MICE; PACLITAXEL; DOCETAXEL;
D O I
10.1016/0959-8049(94)90547-9
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The antitumour activity of paclitaxel (NSC 125973) and docetaxel (RP 56976, NSC 628503) was evaluated and compared against human ovarian carcinoma (HOC) xenografts in nude mice. Paclitaxel and docetaxel were given intravenously (i.v.) at a dose range of 16.6-34.5 mg/kg, once every 4 days for three consecutive doses to nude mice with HOC xenografts, transplanted subcutaneously (s.c.) (HOC18 and HOC22-S) or intraperitoneally (i.p.) (HOC8 and HOC22). Paclitaxel and docetaxel, at the highest dosage, induced complete tumour regression in 80-100% and 67% of mice bearing HOC22-S and HOC18 s.c,, respectively, Both drugs cured 100% of mice bearing early stage HOC22 tumour in the peritoneal cavity, while treatment at an advanced stage significantly increased the survival time of all the mice. Both induced a 57% cure rate in mice bearing HOC8 in the peritoneal cavity. Paclitaxel and docetaxel were more effective than cisplatin (4 mg/kg, same dosing regime as above) used as a reference compound. These findings indicate that paclitaxel and docetaxel were highly active on four HOC xenograft models. No significant difference between them was detected in ovarian cancer xenografts.
引用
收藏
页码:691 / 696
页数:6
相关论文
共 43 条
  • [1] AAPRO M, 1992, P AM ASSOC CANC RES, V33, P3086
  • [2] AAPRO M, 1993, P AM SOC CLIN ONCOL, V12, P809
  • [3] BARASOAIN I, 1991, P AM ASSOC CANC RES, V32, P1952
  • [4] BISSERY MC, 1991, CANCER RES, V51, P4845
  • [5] SECONDARY SCREENING OF PLATINUM COMPOUNDS IN HUMAN OVARIAN-CANCER XENOGRAFTS IN NUDE-MICE
    BOVEN, E
    NAUTA, MM
    SCHLUPER, HMM
    ELFERINK, F
    VANDERVIJGH, WJF
    PINEDO, HM
    [J]. EUROPEAN JOURNAL OF CANCER & CLINICAL ONCOLOGY, 1985, 21 (10): : 1253 - 1260
  • [6] ANTITUMOR-ACTIVITY OF TAXOTERE (RP-56976, NSC-628503), A NEW TAXOL ANALOG, IN EXPERIMENTAL OVARIAN-CANCER
    BOVEN, E
    VENEMAGABERSCEK, E
    ERKELENS, CAM
    BISSERY, MC
    PINEDO, HM
    [J]. ANNALS OF ONCOLOGY, 1993, 4 (04) : 321 - 324
  • [7] A PHASE-I TRIAL OF TAXOL GIVEN BY A 6-HOUR INTRAVENOUS-INFUSION
    BROWN, T
    HAVLIN, K
    WEISS, G
    CAGNOLA, J
    KOELLER, J
    KUHN, J
    RIZZO, J
    CRAIG, J
    PHILLIPS, J
    VONHOFF, D
    [J]. JOURNAL OF CLINICAL ONCOLOGY, 1991, 9 (07) : 1261 - 1267
  • [8] PHASE-I CLINICAL-TRIAL OF TAXOTERE ADMINISTERED AS EITHER A 2-HOUR OR 6-HOUR INTRAVENOUS-INFUSION
    BURRIS, H
    IRVIN, R
    KUHN, J
    KALTER, S
    SMITH, L
    SHAFFER, D
    FIELDS, S
    WEISS, G
    ECKARDT, J
    RODRIGUEZ, G
    RINALDI, D
    WALL, J
    COOK, G
    SMITH, S
    VREELAND, F
    BAYSSAS, M
    LEBAIL, N
    VONHOFF, D
    [J]. JOURNAL OF CLINICAL ONCOLOGY, 1993, 11 (05) : 950 - 958
  • [9] BURRIS H, 1993, P AN M AM SOC CLIN, V12, pA1116
  • [10] CASAZZA AM, 1993, P AM ASSOC CANC RES, V34, P2267
12345