ESTABLISHMENT OF AN IN-VITRO MODEL FOR CISPLATIN RESISTANCE IN HUMAN NEUROBLASTOMA CELL-LINES

被引：0

作者：

IRELAND, CM

PITTMAN, SM

JONES, SL

HARNETT, PR

机构：

[1] UNIV NEW S WALES, PRINCE WALES CHILDRENS HOSP, CHILDRENS LEUKAEMIA & CANC RES CTR, SYDNEY, NSW, AUSTRALIA

[2] WESTMEAD HOSP, DEPT MED ONCOL & PALLIAT CARE, SYDNEY, NSW, AUSTRALIA

来源：

ANTICANCER RESEARCH | 1994年 / 14卷 / 6B期

关键词：

DRUG RESISTANCE; CISPLATIN; NEUROBLASTOMA; DNA REPAIR;

D O I：

暂无

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Two unique cisplatin-resistant neuroblastoma (NB) cell lines have been derived fi om the established lines IMR-32 and: SK-N-SH by treatment with escalating doses of cisplatin. IMR/CP.20 was 6.6-fold and SK/CP.15 was 3.8-fold more resistant to the cytotoxic effects of cisplatin than the parent lines. The parent SK-N-SH cells were 16.6-fold more resistant to the effects of cisplatin than IMR-32 cells. The cisplatin-resistant cell lines demonstrated alterations to their morphology, bus there was no change in the cell growth characteristics of the resistant compared to the sensitive lines. Cytogenetic analysis revealed that clonal selection of parental subclones had occurred with additional chromosomal changes in both resistant lines. Both IMR/CP.20 and SK/CP.15 fines were cross-resistant to aphidicolin and tb L-phenylalanine mustard. The IMR/CP.20 line was 7.3-fold more resistant to mitomycin C than the parent line. Neither cisplatin-resistant NE line was crass-resistant to 5-fluorouracil, etoposide or doxorubicin. All NE lines had low levels of DNA repair compared to HeLa or CHO-K1 cells. However, the IMR/CP.20 cell line showed a significantly higher ability to effect DNA repair than the parent IMR-32 line indicating that the increased resistance to cisplatin observed in this line may, in part be due to an enhanced DNA repair capacity.

引用

页码：2397 / 2403

页数：7

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