LEUCOVORIN RESCUE OF HUMAN CANCER AND BONE-MARROW CELLS FOLLOWING EDATREXATE OR METHOTREXATE

被引:11
|
作者
JOLIVET, J
JANSEN, G
PETERS, GJ
PINARD, MF
SCHORNAGEL, JH
机构
[1] FREE UNIV AMSTERDAM HOSP, DEPT ONCOL, 1081 HV AMSTERDAM, NETHERLANDS
[2] NETHERLANDS CANC INST, DEPT INTERNAL MED, 1066 CX AMSTERDAM, NETHERLANDS
来源
BIOCHEMICAL PHARMACOLOGY | 1994年 / 47卷 / 04期
关键词
EDATREXATE; METHOTREXATE; LEUCOVORIN; HUMAN CANCER CELLS; HUMAN BONE MARROW CELLS;
D O I
10.1016/0006-2952(94)90128-7
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
We have examined the cytotoxic activities of edatrexate (EDX) and methotrexate (MTX) and their reversal by leucovorin in nine human cancer cell lines and in human bone marrow CFU-GM cells. EDX was 3.7- to 123-fold more toxic than MTX against the cancer cell lines and 25-fold against the bone marrow cells. Lower EDX concentrates generally were needed to inhibit cancer cell growth relative to bone marrow cells, however, whereas bone marrow and cancer cell growth were more often susceptible to the same MTX concentrations. The new antifolate was metabolized to long-chain polyglutamates to a greater extent than MTX in seven cell lines. Leucovorin at 0.2 mu M rescued two breast cancer and two non-small cell lung cancer cell lines to a lesser extent following EDX than MTX, but significant rescue was observed in two head and neck cancer cell lines that formed large amounts of polyglutamates. These cell lines also accumulated reduced folates to a greater extent than the other cell lines following leucovorin exposure. Leucovorin rescued bone marrow cells following MTX but only partially following the highest EDX concentrations. EDX may enjoy a better therapeutic index than MTX against some cancer cell lines relative to bone marrow precursor cells, especially after leucovorin rescue.
引用
收藏
页码:659 / 665
页数:7
相关论文
共 50 条
  • [21] T-CELLS IN HUMAN BONE-MARROW
    GALE, RP
    OPELZ, G
    GOLDE, DW
    KIUCHI, M
    CLINICAL RESEARCH, 1975, 23 (03): : A290 - A290
  • [22] ELIMINATION OF MALIGNANT-CELLS FROM BONE-MARROW IN AUTOLOGOUS RESCUE
    BUCKMAN, R
    COOMBES, RC
    FORESTER, AJ
    SHEPHERD, V
    MCILHINNEY, RAJ
    NEVILLE, AM
    PROCEEDINGS OF THE AMERICAN ASSOCIATION FOR CANCER RESEARCH, 1984, 25 (MAR): : 156 - 156
  • [23] GENETIC-TRANSFORMATION OF MURINE BONE-MARROW CELLS TO METHOTREXATE RESISTANCE
    CARR, F
    MEDINA, WD
    DUBE, S
    BERTINO, JR
    BLOOD, 1983, 62 (01) : 180 - 185
  • [24] THERAPEUTIC USEFULNESS OF HOME AND ERYTHROPOIETIN ON HEMATOPOIETIC RESCUE FOLLOWING BONE-MARROW SUPPRESSION
    LUTTON, JD
    JIANG, SL
    ABRAHAM, NG
    EXPERIMENTAL HEMATOLOGY, 1993, 21 (05) : 724 - 724
  • [25] PROTECTION OF BONE-MARROW TRANSPLANT RECIPIENTS FROM LETHAL DOSES OF METHOTREXATE BY THE GENERATION OF METHOTREXATE-RESISTANT BONE-MARROW
    WILLIAMS, DA
    HSIEH, K
    DESILVA, A
    MULLIGAN, RC
    JOURNAL OF EXPERIMENTAL MEDICINE, 1987, 166 (01): : 210 - 218
  • [26] NONSPECIFIC SUPPRESSOR CELLS FOLLOWING BONE-MARROW TRANSPLANTATION
    HESS, AD
    TUTSCHKA, PJ
    SARAL, R
    SANTOS, GW
    EXPERIMENTAL HEMATOLOGY, 1982, 10 : 64 - 64
  • [27] RESCUE OF METHOTREXATE TOXICITY TO MOUSE BONE-MARROW - COMPARISON BETWEEN CITROVORUM FACTOR (CF) AND NUCLEOSIDES
    PINEDO, HM
    CHABNER, BA
    CLINICAL RESEARCH, 1976, 24 (03): : A380 - A380
  • [28] CALCITONIN AND SOMATOSTATIN IMMUNOREACTIVE CELLS ARE PRESENT IN HUMAN BONE-MARROW AND BONE-MARROW CELLS ARE RESPONSIVE TO CALCITONIN AND SOMATOSTATIN
    GODLEWSKI, A
    EXPERIMENTAL AND CLINICAL ENDOCRINOLOGY, 1990, 96 (02): : 219 - 233
  • [29] MR APPEARANCES OF BONE-MARROW IN CHILDREN FOLLOWING BONE-MARROW TRANSPLANTATION
    BOOTHROYD, AE
    SEBAG, G
    BRUNELLE, F
    PEDIATRIC RADIOLOGY, 1991, 21 (04) : 291 - 292
  • [30] METHOTREXATE-INDUCED BONE-MARROW SUPPRESSION
    COSTELLO, C
    MIR, N
    HUGHES, RA
    RILEY, B
    CLINICAL AND LABORATORY HAEMATOLOGY, 1991, 13 (03): : 322 - 323
12345