Dalton Cardiovascular Research Center, University of Missouri-Columbia, Columbia, MO, 65211, USA.
Breast Cancer Res Treat. 2011 Jan;125(2):407-20. doi: 10.1007/s10549-010-0851-x. Epub 2010 Mar 27.
Breast cancer progression depends upon the elaboration of a vasculature sufficient for the nourishment of the developing tumor. Breast tumor cells frequently contain a mutant form of p53 (mtp53), a protein which promotes their survival. The aim of this study was to determine whether combination therapy targeting mtp53 and anionic phospholipids (AP) on tumor blood vessels might be an effective therapeutic strategy for suppressing advanced breast cancer. We examined the therapeutic effects, singly, or in combination, of p53 reactivation and induction of massive apoptosis (PRIMA-1), which reactivates mtp53 and induces tumor cell apoptosis, and 2aG4, a monoclonal antibody that disrupts tumor vasculature by targeting AP on the surface of tumor endothelial cells and causes antibody-dependent destruction of tumor blood vessels, leading to ischemia and tumor cell death. Xenografts from two tumor cell lines containing mtp53, BT-474 and HCC-1428, were grown in nude mice to provide models of advanced breast tumors. After treatment with PRIMA-1 and/or 2aG4, regressing tumors were analyzed for vascular endothelial growth factor (VEGF) expression, blood vessel loss, and apoptotic markers. Individual drug treatment led to partial suppression of breast cancer progression. In contrast, combined treatment with PRIMA-1 and 2aG4 was extremely effective in suppressing tumor growth in both models and completely eradicated approximately 30% of tumors in the BT-474 model. Importantly, no toxic effects were observed in any treatment group. Mechanistic studies determined that PRIMA-1 reactivated mtp53 and also exposed AP on the surface of tumor cells as determined by enhanced 2aG4 binding. Combination treatment led to significant induction of tumor cell apoptosis, loss of VEGF expression, as well as destruction of tumor blood vessels. Furthermore, combination treatment severely disrupted tumor blood vessel perfusion in both tumor models. The observed in vitro PRIMA-1-induced exposure of tumor epithelial cell AP might provide a target for 2aG4 and contribute to the increased effectiveness of such combination therapy in vivo. We conclude that the combined targeting of mtp53 and the tumor vasculature is a novel effective strategy for combating advanced breast tumors.
乳腺癌的进展取决于为肿瘤生长提供营养的血管的形成。乳腺癌细胞常含有突变型 p53(mtp53),这种蛋白促进其存活。本研究旨在确定针对肿瘤血管中的 mtp53 和阴离子磷脂(AP)的联合治疗是否可能是抑制晚期乳腺癌的有效治疗策略。我们分别或联合检查了 p53 再激活和大量细胞凋亡诱导(PRIMA-1)的治疗效果,PRIMA-1 再激活 mtp53 并诱导肿瘤细胞凋亡,以及 2aG4,这是一种通过靶向肿瘤内皮细胞表面的 AP 破坏肿瘤血管的单克隆抗体,并导致抗体依赖性肿瘤血管破坏,导致缺血和肿瘤细胞死亡。含有 mtp53 的两种肿瘤细胞系 BT-474 和 HCC-1428 的异种移植物在裸鼠中生长,提供晚期乳腺癌模型。在用 PRIMA-1 和/或 2aG4 治疗后,分析消退肿瘤的血管内皮生长因子(VEGF)表达、血管损失和凋亡标志物。单独药物治疗导致乳腺癌进展的部分抑制。相比之下,PRIMA-1 和 2aG4 的联合治疗在两种模型中都非常有效地抑制肿瘤生长,并完全消除 BT-474 模型中约 30%的肿瘤。重要的是,任何治疗组均未观察到毒性作用。机制研究确定 PRIMA-1 再激活 mtp53,并通过增强的 2aG4 结合来暴露肿瘤细胞表面的 AP。联合治疗导致肿瘤细胞凋亡显著诱导、VEGF 表达丧失以及肿瘤血管破坏。此外,联合治疗严重破坏了两种肿瘤模型中的肿瘤血管灌注。观察到的体外 PRIMA-1 诱导的肿瘤上皮细胞 AP 暴露可能为 2aG4 提供靶点,并有助于增加体内这种联合治疗的效果。我们得出结论,靶向 mtp53 和肿瘤血管是一种治疗晚期乳腺癌的新有效策略。
