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人结肠腺癌细胞短期和持续暴露于氟尿嘧啶之间的协同作用及交叉耐药性缺失。

Synergism and lack of cross-resistance between short-term and continuous exposure to fluorouracil in human colon adenocarcinoma cells.

作者信息

Sobrero A F, Aschele C, Guglielmi A P, Mori A M, Melioli G G, Rosso R, Bertino J R

机构信息

Department of Medical Oncology, Istituto Nazionale per la Ricerca sul Cancro, Genova, Italy.

出版信息

J Natl Cancer Inst. 1993 Dec 1;85(23):1937-44. doi: 10.1093/jnci/85.23.1937.

Abstract

BACKGROUND

Our recent findings in vitro in the human colon adenocarcinoma cell line HCT-8 suggest that resistance to fluorouracil (5-FU) in patients with advanced colorectal cancer might be overcome by use of a different treatment schedule.

PURPOSE

We tested the hypothesis that HCT-8 cells resistant to short-term 5-FU exposure retain sensitivity to continuous exposure and studied interactions between the two schedules.

METHODS

HCT-8 cell lines resistant to short-term (pulse) treatment with 5-FU or to continuous exposure were obtained by six exposures to different concentrations of 5-FU for 4 hours or 7 days. We used a monolayer clonogenic assay to determine 5-FU-induced cell kill in resistant HCT-8 cells and sensitive parent cells. Parent cells were exposed to different concentrations of 5-FU for 1, 4, or 24 hours (short term), for 7 days (continuous exposure), or in a combination of both types of schedules. In a study of the mechanism of interaction between short-term and continuous exposure in parent cells, we performed flow cytometric DNA analysis to determine the percentage of cells in S phase and assays of thymidylate synthase inhibition in intact cells and of incorporation of [6-3H)]5-FU nucleotides into nucleic acids.

RESULTS

Sensitive HCT-8 cells became fully resistant to 5-FU within five or six treatments, and low-dose continuous exposure almost immediately produced resistant clones. HCT-8 cells resistant to 5-FU given every 4 hours retained full sensitivity to continuous exposure, suggesting lack of cross-resistance between the two schedules, but cells resistant to continuous exposure were cross-resistant to short-term treatment. Parent cells showed a statistically significant (synergistic) enhancement of the cytotoxic activity for 5-FU exposure for 1 hour (100, 300, or 500 microM) followed by continuous exposure (0.5, 1, or 2 microM) or 4 hours (10, 30, or 60 microM) followed by continuous exposure (1 or 2 microM). Short-term plus continuous exposure produced a marked increase in percentage of S-phase cells, compared with the percentage for each schedule alone. The combination of 1-hour exposure and continuous exposure (1000 and 2 microM, respectively) produced a marked accumulation of cells in S phase at 24 hours (59%), which lasted up to 96 hours (53%). The combination of the two schedules produced only additive enhancement of thymidylate synthase inhibition as well as incorporation of [6-3H]5-FU nucleotides into nucleic acids of HCT-8 cells.

CONCLUSIONS

Our findings provide a rationale for the use of bolus 5-FU and continuous infusion 5-FU in sequence.

IMPLICATION

We are conducting a clinical trial of bolus methotrexate followed by continuous-infusion 5-FU plus leucovorin.

摘要

背景

我们最近在人结肠腺癌细胞系HCT - 8中的体外研究结果表明,晚期结直肠癌患者对氟尿嘧啶(5 - FU)的耐药性可能通过采用不同的治疗方案来克服。

目的

我们验证了以下假设,即对短期5 - FU暴露耐药的HCT - 8细胞对持续暴露仍保持敏感性,并研究了两种方案之间的相互作用。

方法

通过对不同浓度的5 - FU进行6次4小时或7天的暴露,获得对短期(脉冲)5 - FU治疗或持续暴露耐药的HCT - 8细胞系。我们使用单层克隆形成试验来确定5 - FU对耐药HCT - 8细胞和敏感亲本细胞的杀伤作用。亲本细胞分别暴露于不同浓度的5 - FU 1小时、4小时或24小时(短期)、7天(持续暴露)或两种方案的组合。在一项关于亲本细胞短期和持续暴露之间相互作用机制的研究中,我们进行了流式细胞术DNA分析以确定S期细胞的百分比,并检测完整细胞中胸苷酸合成酶的抑制情况以及[6 - ³H]5 - FU核苷酸掺入核酸的情况。

结果

敏感的HCT - 8细胞在5或6次治疗后对5 - FU完全耐药,低剂量持续暴露几乎立即产生耐药克隆。每4小时给予5 - FU耐药的HCT - 8细胞对持续暴露仍保持完全敏感性,表明两种方案之间不存在交叉耐药性,但对持续暴露耐药的细胞对短期治疗存在交叉耐药性。亲本细胞在暴露于1小时(100、300或500微摩尔)的5 - FU后接着持续暴露(0.5、1或2微摩尔)或4小时(10、30或60微摩尔)后接着持续暴露(1或2微摩尔)时,5 - FU的细胞毒性活性有统计学意义的(协同)增强。与单独每种方案相比,短期加持续暴露使S期细胞百分比显著增加。1小时暴露和持续暴露(分别为1000和2微摩尔)的组合在24小时时使S期细胞显著积累(59%),持续至96小时(53%)。两种方案的组合在抑制胸苷酸合成酶以及[6 - ³H]5 - FU核苷酸掺入HCT - 8细胞核酸方面仅产生相加增强作用。

结论

我们的研究结果为序贯使用大剂量5 - FU和持续输注5 - FU提供了理论依据。

启示

我们正在进行一项先给予大剂量甲氨蝶呤接着持续输注5 - FU加亚叶酸钙的临床试验。

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