Tortora Giampaolo, Caputo Rosa, Damiano Vincenzo, Melisi Davide, Bianco Roberto, Fontanini Gabriella, Veneziani Bianca Maria, De Placido Sabino, Bianco A Raffaele, Ciardiello Fortunato
Dipartimento di Endocrinologia e Oncologia Molecolare e Clinica, Università di Napoli Federico II, 80131 Napoli, Italy.
Clin Cancer Res. 2003 Apr;9(4):1566-72.
Epidermal growth factor receptor (EGFR) and protein kinase A type I(PKAI) play an important role in the control of cancer cell growth and angiogenesis. Inhibitors of EGFR and PKAI have antitumor activity in vitro and in vivo in a variety of tumor types, and some of these agents are active after oral administration. Increasing evidence shows that cyclooxygenase (COX)-2 also plays a role in promoting cancer cell proliferation and angiogenesis. COX-2 expression can be induced by EGFR activation and is regulated by cAMP and PKA. Combination of an EGFR inhibitor with a nonselective COX-1/COX-2 inhibitor prevents the development of intestinal cancer in nude mice. Therefore, we investigated whether any cooperative antitumor effect can be obtained by the combined blockade of COX-2, EGFR, and PKAI.
The COX-2 inhibitor SC-236 was combined with the selective EGFR tyrosine kinase inhibitor ZD1839 (Iressa) and the DNA/RNA-mixed backbone oligonucleotide AS-PKAI to study their effect on human cancer growth and angiogenesis, measuring vascular endothelial growth factor (VEGF) and basic fibroblast growth factor expression and vessel formation, in vitro and after oral administration of these agents in mice.
A cooperative effect was observed with SC-236 in combination with either ZD1839 or AS-PKAI, as well as with all three agents together, on the proliferation of human colon and breast cancer cells in soft agar at doses that were ineffective for each agent alone. The antiproliferative effect was accompanied by inhibition of COX-2 expression. Moreover, combination of SC-236 with either agent or the triple combination markedly reduced VEGF secretion in the conditioned medium and completely suppressed VEGF and basic fibroblast growth factor expression. In nude mice bearing human colon cancer xenografts, a low, noninhibitory dose of SC-236 with ZD1839 and AS-PKAI, all given p.o., caused a dramatic cooperative antitumor effect, with no histological evidence of tumor in 60% of mice 5 weeks after treatment withdrawal, at which time all mice were alive. Moreover, analysis of tumor specimens revealed inhibition of vessel formation and expression of COX-2 and VEGF.
This is the first demonstration that three novel agents blocking multiple signaling pathways, in absence of cytotoxic drugs, may have a potent antitumor and antiangiogenic activity after oral administration. Because all agents are under clinical evaluation, our results provide a rationale to translate this feasible therapeutic strategy into a clinical setting.
表皮生长因子受体(EGFR)和蛋白激酶A I型(PKAI)在癌细胞生长和血管生成的调控中发挥重要作用。EGFR和PKAI的抑制剂在多种肿瘤类型的体外和体内均具有抗肿瘤活性,其中一些药物口服后也具有活性。越来越多的证据表明,环氧合酶(COX)-2在促进癌细胞增殖和血管生成中也发挥作用。COX-2的表达可由EGFR激活诱导,并受cAMP和PKA调控。EGFR抑制剂与非选择性COX-1/COX-2抑制剂联合使用可预防裸鼠肠道癌的发生。因此,我们研究了联合阻断COX-2、EGFR和PKAI是否能产生协同抗肿瘤作用。
将COX-2抑制剂SC-236与选择性EGFR酪氨酸激酶抑制剂ZD1839(易瑞沙)和DNA/RNA混合骨架寡核苷酸AS-PKAI联合使用,研究它们对人类癌症生长和血管生成的影响,检测血管内皮生长因子(VEGF)和碱性成纤维细胞生长因子的表达以及血管形成,分别在体外和给小鼠口服这些药物后进行观察。
观察到SC-236与ZD1839或AS-PKAI联合使用,以及三者共同使用时,在软琼脂中对人结肠癌细胞和乳腺癌细胞增殖具有协同作用,而单独使用每种药物时在相应剂量下均无效。这种抗增殖作用伴随着COX-2表达的抑制。此外,SC-236与任何一种药物联合或三联组合均显著降低了条件培养基中VEGF的分泌,并完全抑制了VEGF和碱性成纤维细胞生长因子的表达。在携带人结肠癌异种移植瘤的裸鼠中,低剂量、无抑制作用的SC-236与ZD1839和AS-PKAI口服给药后,产生了显著的协同抗肿瘤作用,停药5周后,60%的小鼠未发现肿瘤组织学证据,此时所有小鼠均存活。此外,对肿瘤标本的分析显示血管形成以及COX-2和VEGF的表达均受到抑制。
这是首次证明在无细胞毒性药物的情况下,三种新型药物阻断多个信号通路,口服给药后可能具有强大的抗肿瘤和抗血管生成活性。由于所有药物均处于临床评估阶段,我们的结果为将这种可行的治疗策略转化为临床应用提供了理论依据。
