Eyol Ergül, Boleij Annemarie, Taylor Rachel R, Lewis Andrew L, Berger Martin R
Toxicology and Chemotherapy Unit, German Cancer Research Centre, Heidelberg, Germany.
Clin Exp Metastasis. 2008;25(3):273-82. doi: 10.1007/s10585-008-9142-x. Epub 2008 Feb 8.
Systemic chemotherapy has limited success in treating liver metastasis of colorectal cancer. Alternative approaches such as hepatic arterial infusion or trans arterial chemoembolisation aim to deliver the chemotherapy locally to address the predominant liver disease. Chemoembolisation with drug eluting beads (DEB) designed to deliver drug at the target over a protracted period of time is a new strategy to reduce the tumor burden of liver metastases. To test this hypothesis, DEB possessing anionic groups capable of ionically complexing with cationic drugs were synthesised by a suspension polymerisation method and were fractionated to produce an average size of 75 microm. The DEB were loaded with the desired concentration of either doxorubicin hydrochloride or irinotecan hydrochloride prior to administration by immersion in the drug solution, yielding essentially 100% loading efficiency. To determine their effect in vivo, a transplantable orthotopic and isogenic rat liver metastasis model was used which is based on intraportal injection of 4 x 10(6) beta-galactosidase transfected CC531 rat colorectal cancer cells into male WAG/Rij rats. By MTT assay, the cells were shown to be sensitive to both drugs in vitro with the IC(50) being by two orders of magnitude lower for doxorubicin (110 nM after 72 h) compared to irinotecan (25 microM after 72 h). For the in vivo phase, a differential expression of the ERK MAP kinase between tumor cells cultured in vitro and those inoculated in vivo was noted using Western blotting techniques. This was considered to be indicative of passage-induced cell senescence that reduced the sensitivity of the tumor cells to DEB chemoembolisation. This notwithstanding, administration of DEB loaded with irinotecan or doxorubicin by single injection into the hepatic artery showed significant anticancer activity, as measured by a reduction in the tumor burden of the liver and a corresponding reduction in liver weight. Comparing the two agents, irinotecan appears more advantageous because of its significant activity and excellent tolerability following administration at two dosages of either 20 or 30 mg/kg. Doxorubicin showed a narrower window of activity, being effective at 4 mg/kg but ineffective at the lower dose of 2 mg/kg. We conclude that chemoembolisation with DEB with either agent may have potential for treating patients with colorectal liver metastasis, although irinotecan DEB appeared to have a more favourable safety profile.
全身化疗在治疗结直肠癌肝转移方面成效有限。诸如肝动脉灌注或经动脉化疗栓塞等替代方法旨在将化疗药物局部输送,以应对主要的肝脏疾病。使用设计为在较长时间内在靶部位释放药物的载药微球(DEB)进行化疗栓塞是一种减轻肝转移瘤负担的新策略。为验证这一假设,通过悬浮聚合法合成了带有能够与阳离子药物发生离子络合的阴离子基团的DEB,并进行分级分离以产生平均粒径为75微米的微球。在通过浸入药物溶液进行给药之前,将DEB装载上所需浓度的盐酸多柔比星或盐酸伊立替康,装载效率基本达到100%。为确定它们在体内的效果,使用了一种可移植的原位同基因大鼠肝转移模型,该模型基于将4×10(6)个转染了β-半乳糖苷酶的CC531大鼠结直肠癌细胞经门静脉注射到雄性WAG/Rij大鼠体内。通过MTT试验表明,这些细胞在体外对两种药物均敏感,与伊立替康(72小时后IC(50)为25微摩尔)相比,多柔比星的IC(50)低两个数量级(72小时后为110纳摩尔)。在体内阶段,使用蛋白质印迹技术发现体外培养的肿瘤细胞与体内接种的肿瘤细胞之间ERK MAP激酶存在差异表达。这被认为表明传代诱导的细胞衰老降低了肿瘤细胞对DEB化疗栓塞的敏感性。尽管如此,通过单次肝动脉注射给予装载有伊立替康或多柔比星的DEB显示出显著的抗癌活性,这通过肝脏肿瘤负担的减轻和相应的肝脏重量减轻得以衡量。比较这两种药物,伊立替康似乎更具优势,因为在20或30毫克/千克这两种剂量给药后,它具有显著的活性和良好的耐受性。多柔比星的活性窗口较窄,在4毫克/千克时有效,但在2毫克/千克的较低剂量时无效。我们得出结论,使用这两种药物中的任何一种进行DEB化疗栓塞可能对治疗结直肠癌肝转移患者具有潜力,尽管伊立替康DEB似乎具有更有利的安全性。
