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节律性伊立替康单药化疗以及联合司马沙尼的抗血管生成和抗结直肠癌作用

Antiangiogenic and anticolorectal cancer effects of metronomic irinotecan chemotherapy alone and in combination with semaxinib.

作者信息

Bocci G, Falcone A, Fioravanti A, Orlandi P, Di Paolo A, Fanelli G, Viacava P, Naccarato A G, Kerbel R S, Danesi R, Del Tacca M, Allegrini G

机构信息

Division of Pharmacology and Chemotherapy, Department of Internal Medicine, University of Pisa, Pisa, Italy.

出版信息

Br J Cancer. 2008 May 20;98(10):1619-29. doi: 10.1038/sj.bjc.6604352. Epub 2008 Apr 29.

DOI:10.1038/sj.bjc.6604352
PMID:18443598
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2391121/
Abstract

Metronomic chemotherapy refers to the administration of chemotherapy at low, nontoxic doses on a frequent schedule with no prolonged breaks. The aim of the study is to rationally develop a CPT-11 metronomic regimen in preclinical settings of colon cancer. In vitro cell proliferation, apoptosis and thrombospondin-1/vascular endothelial growth factor (TSP-1/VEGF) expression analyses were performed on endothelial (HUVEC, HMVEC-d) and colorectal cancer (HT-29, SW620) cells exposed for 144 h to metronomic concentrations of SN-38, the active metabolite of CPT-11. HT-29 human colorectal cancer xenograft model was used, and tumour growth, microvessel density and VEGF/TSP-1 quantification was performed in tumours. In vitro and in vivo combination studies with the tyrosine inhibitor semaxinib were also performed. SN-38 preferentially inhibited endothelial cell proliferation alone and interacted synergistically with semaxinib; it induced apoptosis and increased the expression and secretion of TSP-1. Metronomic CPT-11 alone and combined with semaxinib significantly inhibits tumour growth in the absence of toxicity, which was accompanied by decreases in microvessel density and increases in TSP-1 gene expression in tumour tissues. In vitro results show the antiangiogenic properties of low-concentration SN-38, suggesting a key role of TSP-1 in this effect. In vivo, the CPT-11 metronomic schedule is effective against tumour and microvessel growth without toxic effect on mice.

摘要

节拍化疗是指以低剂量、无毒的方式频繁给药化疗,且无长时间中断。本研究的目的是在结肠癌的临床前环境中合理开发一种伊立替康节拍方案。对暴露于伊立替康活性代谢物SN-38节拍浓度144小时的内皮细胞(人脐静脉内皮细胞、人微血管内皮细胞-d)和结肠癌细胞(HT-29、SW620)进行体外细胞增殖、凋亡和血小板反应蛋白-1/血管内皮生长因子(TSP-1/VEGF)表达分析。使用HT-29人结肠癌异种移植模型,对肿瘤进行肿瘤生长、微血管密度和VEGF/TSP-1定量分析。还进行了与酪氨酸抑制剂司马沙尼的体外和体内联合研究。SN-38单独优先抑制内皮细胞增殖,并与司马沙尼协同作用;它诱导凋亡并增加TSP-1的表达和分泌。单独使用节拍伊立替康并与司马沙尼联合使用可在无毒性的情况下显著抑制肿瘤生长,这伴随着肿瘤组织中微血管密度的降低和TSP-1基因表达的增加。体外结果显示低浓度SN-38具有抗血管生成特性,表明TSP-1在该效应中起关键作用。在体内,伊立替康节拍方案对肿瘤和微血管生长有效,且对小鼠无毒性作用。

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