Zhang Xuefeng, Xu Jianfeng, Lawler Jack, Terwilliger Ernest, Parangi Sareh
Department of Surgery, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts 02215, USA.
Clin Cancer Res. 2007 Jul 1;13(13):3968-76. doi: 10.1158/1078-0432.CCR-07-0245.
Recombinant adeno-associated virus (rAAV)-mediated antiangiogenic gene therapy offers a powerful strategy for cancer treatment, maintaining sustained levels of antiangiogenic factors with coincident enhanced therapeutic efficacy. We aimed to develop rAAV-mediated antiangiogenic gene therapy delivering endostatin and 3TSR, the antiangiogenic domain of thrombospondin-1.
rAAV vectors were constructed to express endostatin (rAAV-endostatin) or 3TSR (rAAV-3TSR). The antiangiogenic efficacy of the vectors was characterized using a vascular endothelial growth factor (VEGF)-induced mouse ear angiogenesis model. To evaluate the antitumor effects of the vectors, immunodeficient mice were pretreated with rAAV-3TSR or rAAV-endostatin and received orthotopic implantation of cancer cells into the pancreas. To mimic clinical situations, mice bearing pancreatic tumors were treated with intratumoral injection of rAAV-3TSR or rAAV-endostatin.
rAAV-mediated i.m. gene delivery resulted in expression of the transgene in skeletal muscle with inhibition of VEGF-induced angiogenesis at a distant site (the ear). Local delivery of the vectors into the mouse ear also inhibited VEGF-induced ear angiogenesis. Pretreatment of mice with i.m. or intrasplenic injection of rAAV-endostatin or rAAV-3TSR significantly inhibited tumor growth. A single intratumoral injection of each vector also significantly decreased the volume of large established pancreatic tumors. Tumor microvessel density was significantly decreased in each treatment group and was well correlated with tumor volume reduction. Greater antiangiogenic and antitumor effects were achieved when rAAV-3TSR and rAAV-endostatin were combined.
rAAV-mediated 3TSR and endostatin gene therapy showed both localized and systemic therapeutic effects against angiogenesis and tumor growth and may provide promise for patients with pancreatic cancer.
重组腺相关病毒(rAAV)介导的抗血管生成基因治疗为癌症治疗提供了一种强大的策略,可维持抗血管生成因子的持续水平,同时提高治疗效果。我们旨在开发rAAV介导的抗血管生成基因治疗方法,递送内皮抑素和血小板反应蛋白-1的抗血管生成结构域3TSR。
构建rAAV载体以表达内皮抑素(rAAV-内皮抑素)或3TSR(rAAV-3TSR)。使用血管内皮生长因子(VEGF)诱导的小鼠耳血管生成模型来表征载体的抗血管生成功效。为了评估载体的抗肿瘤作用,对免疫缺陷小鼠进行rAAV-3TSR或rAAV-内皮抑素预处理,并将癌细胞原位植入胰腺。为模拟临床情况,对患有胰腺肿瘤的小鼠进行瘤内注射rAAV-3TSR或rAAV-内皮抑素治疗。
rAAV介导的肌肉内基因递送导致转基因在骨骼肌中表达,并抑制远处部位(耳朵)的VEGF诱导的血管生成。将载体局部递送至小鼠耳部也抑制了VEGF诱导的耳部血管生成。通过肌肉内或脾内注射rAAV-内皮抑素或rAAV-3TSR对小鼠进行预处理可显著抑制肿瘤生长。对每个载体进行单次瘤内注射也显著减小了已形成的大型胰腺肿瘤的体积。每个治疗组的肿瘤微血管密度均显著降低,且与肿瘤体积减小密切相关。当rAAV-3TSR和rAAV-内皮抑素联合使用时,可实现更强的抗血管生成和抗肿瘤作用。
rAAV介导的3TSR和内皮抑素基因治疗对血管生成和肿瘤生长显示出局部和全身治疗效果,可能为胰腺癌患者带来希望。
Zotero 插件