bcl-2和c-myc反义寡核苷酸联合顺铂对人黑色素瘤异种移植瘤的抗肿瘤疗效：给药顺序的相关性

Antitumor efficacy of bcl-2 and c-myc antisense oligonucleotides in combination with cisplatin in human melanoma xenografts: relevance of the administration sequence.

作者信息

Zupi Gabriella, Scarsella Marco, Semple Sean C, Mottolese Marcella, Natali Pier G, Leonetti Carlo

机构信息

Experimental Chemotherapy Laboratory, Pathology Department, and Immunology Laboratory, Regina Elena Cancer Institute, Via delle Messi d'Oro 156, 00158 Rome, Italy.

出版信息

Clin Cancer Res. 2005 Mar 1;11(5):1990-8. doi: 10.1158/1078-0432.CCR-04-1284.

DOI:10.1158/1078-0432.CCR-04-1284

PMID:15756025

Abstract

PURPOSE

bcl-2 and c-myc oncogenes are frequently overexpressed in different human tumors, including melanoma. Here, we evaluate the combined efficacy of two antisense oligonucleotides targeting bcl-2 mRNA (ODN bcl-2) and c-myc mRNA (ODN c-myc) in combination with cis-diammine dichloroplatinum (cisplatin, DDP) on three human melanoma lines (LM, NG, and M20).

EXPERIMENTAL DESIGN

Two different sequences were designed to treat tumor-bearing mice: in the first one, ODN bcl-2 at a dose of 0.2 mg/day x4, followed by DDP given i.p. at a dose of 3.3 mg/kg/day x3 and ODN c-myc i.v. at 0.5 mg/day x7, whereas the other sequence consisted of ODN c-myc given as first agent followed by DDP and ODN bcl-2 at the same doses. Mice received three complete cycles of treatment in 1-week intervals.

RESULTS

The treatment sequence with ODN bcl-2/DDP/ODN c-myc combination completely inhibited growth in NG tumor and induced a 35-day delay in LM tumor growth. In contrast, the M20 tumor growth was unaffected by the combination. A discrete amount of c-Myc and bcl-2 protein expression in both LM and NG tumors was detected, whereas no detectable levels of the two proteins were observed in M20 tumors. Compared with the other combination, the sequence (ODN bcl-2/DDP/ODN c-myc) produced the most effective results, producing a significant decrease in bcl-2 and c-Myc protein expression, which in turn significantly increased the survival of NG- and LM-bearing mice, with 4 mice out of 11 and 1 out of 7 mice being cured, respectively. Finally, this combination increased the apoptotic rate and produced an antiangiogenetic effect.

CONCLUSIONS

These results show that an antisense approach to the treatment of melanoma xenografts overexpressing either bcl-2 or c-myc oncogenes represents a successful strategy to improve the response to chemotherapy in melanoma, with particular attention to the treatment sequence.

摘要

目的

bcl-2和c-myc癌基因在包括黑色素瘤在内的不同人类肿瘤中经常过度表达。在此，我们评估了两种分别靶向bcl-2 mRNA（ODN bcl-2）和c-myc mRNA（ODN c-myc）的反义寡核苷酸与顺二氨二氯铂（顺铂，DDP）联合使用对三种人类黑色素瘤细胞系（LM、NG和M20）的综合疗效。

实验设计

设计了两种不同的序列来治疗荷瘤小鼠：第一种序列中，ODN bcl-2以0.2 mg/天×4的剂量给药，随后腹腔注射DDP，剂量为3.3 mg/kg/天×3，ODN c-myc静脉注射，剂量为0.5 mg/天×7；而另一种序列则是先给予ODN c-myc，随后给予相同剂量的DDP和ODN bcl-2。小鼠每隔1周接受三个完整的治疗周期。

结果

ODN bcl-2/DDP/ODN c-myc联合治疗序列完全抑制了NG肿瘤的生长，并使LM肿瘤的生长延迟了35天。相比之下，M20肿瘤的生长不受该联合治疗的影响。在LM和NG肿瘤中均检测到了少量的c-Myc和bcl-2蛋白表达，而在M20肿瘤中未观察到这两种蛋白的可检测水平。与其他联合治疗相比，（ODN bcl-2/DDP/ODN c-myc）序列产生了最有效的结果，使bcl-2和c-Myc蛋白表达显著降低，进而显著提高了荷NG和LM肿瘤小鼠的存活率，分别有11只小鼠中的4只和7只小鼠中的1只被治愈。最后，这种联合治疗提高了凋亡率并产生了抗血管生成作用。