紫杉醇不增加乳腺癌患者外周血胸苷磷酸化酶的表达。

Rupert Bartsch, Guenther G Steger, Birgit Forstner, Catharina Wenzel, Ursula Pluschnig, Blanka Rizovski, Gabriela Altorjai, Christoph C Zielinski, Robert M Mader
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引用次数: 7

摘要

背景:紫杉烷和卡培他滨(5-氟尿嘧啶的前药)可能存在协同细胞毒作用。基于临床前研究,这种协同作用归因于胸苷磷酸化酶(TP)的上调。除肿瘤组织外,当紫杉烷与卡培他滨联合使用时,TP在白细胞中高度表达,可能导致血液毒性增加。到目前为止,这一假设还没有在人类身上进行过研究。方法:对8例接受紫杉醇治疗的晚期乳腺癌患者连续采集128份血样,每周剂量为80mg /m2。为了评估TP在血细胞中的表达,在第一次治疗前、输注结束时和15天后收集样本。在紫杉醇第六次应用时重复此过程。分离外周血单核细胞后,采用ELISA法检测TP的表达。同时,在三个选择的时间点评估血浆中紫杉醇水平作为药代动力学控制参数。结果:输注结束时紫杉醇浓度从第1周到第6周无显著变化。注射后外周血单核细胞TP的表达明显低于治疗前水平(p = 0.023;n = 8)。在第3天降至最低点后,TP的表达适度增加,一周内恢复到基线水平。第6周的整体情况与第1周相似。使用趋势分析,既没有观察到短期也没有观察到长期诱发TP。结论:紫杉醇对外周血单核细胞TP的调节作用不大。因此,预计紫杉烷和卡培他滨联合使用不会导致TP上调而增加血液毒性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Expression of thymidine phosphorylase in peripheral blood cells of breast cancer patients is not increased by paclitaxel.

Expression of thymidine phosphorylase in peripheral blood cells of breast cancer patients is not increased by paclitaxel.

Expression of thymidine phosphorylase in peripheral blood cells of breast cancer patients is not increased by paclitaxel.

Background: A synergistic cytotoxic effect has been hypothesized for taxanes and capecitabine, a prodrug of 5-fluorouracil. Based on preclinical studies, this synergism has been attributed to an up-regulation of the enzyme thymidine phosphorylase (TP). Beside tumour tissue, TP is highly expressed in white blood cells, possibly causing increased hematotoxicity, when taxanes are combined with capecitabine. So far, this hypothesis has not been investigated in humans.

Methods: A total of 128 consecutive blood samples were collected from eight patients with advanced breast cancer receiving paclitaxel weekly at a dose of 80 mg/m2. To assess the expression of TP in blood cells, samples were collected prior to first therapy, at the end of infusion, and up to 15 days thereafter. This procedure was repeated during the sixth application of paclitaxel. After isolation of the peripheral mononuclear blood cells, the expression of TP was assessed by ELISA. In parallel, paclitaxel level in plasma was evaluated at three selected time points as pharmacokinetic control parameter.

Results: Paclitaxel concentrations at the end of infusion did not change significantly from week 1 to week 6. The expression of TP in peripheral mononuclear blood cells decreased significantly after infusion below pretherapeutic values (p = 0.023; n = 8). After the nadir on day 3, the expression of TP increased moderately returning to baseline levels within one week. The overall picture in week 6 was similar to week 1. Using a trend analysis, neither a short-term nor a long-term induction of TP was observed.

Conclusion: TP in peripheral mononuclear blood cells was hardly regulated under therapy with paclitaxel. Therefore, no increased haematotoxicity due to TP upregulation is expected from the combination of taxanes and capecitabine.

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