腺相关病毒载体介导的干扰素-β全身递送联合低剂量环磷酰胺对小鼠神经母细胞瘤模型中的肿瘤消退有影响。

Adeno-associated virus vector-mediated systemic delivery of IFN-beta combined with low-dose cyclophosphamide affects tumor regression in murine neuroblastoma models.

作者信息

Streck Christian J, Dickson Paxton V, Ng Catherine Y C, Zhou Junfang, Gray John T, Nathwani Amit C, Davidoff Andrew M

机构信息

Department of Surgery, St. Jude Children's Research Hospital, Memphis, TN, USA.

出版信息

Clin Cancer Res. 2005 Aug 15;11(16):6020-9. doi: 10.1158/1078-0432.CCR-05-0502.

DOI:10.1158/1078-0432.CCR-05-0502

PMID:16115947

Abstract

PURPOSE

Type I IFNs (IFN-alpha/beta) have shown significant antitumor activity in preclinical models but limited efficacy and significant toxicity in clinical trials. We hypothesized that the antitumor activity of type I IFNs could be enhanced by chronic, low-dose systemic delivery and sought to test this in murine neuroblastoma models.

EXPERIMENTAL DESIGN

Continuous liver-generated expression of human IFN-beta (hINF-beta) was achieved through a gene therapy-mediated approach using adeno-associated virus vectors encoding hIFN-beta (AAV hINF-beta). Orthotopic localized retroperitoneal and disseminated models of neuroblastoma were established using three different xenografts. Immunohistochemical analysis and ELISA were used to evaluate the antiangiogenic effect of therapy.

RESULTS

The development of both localized orthotopic (retroperitoneal) and disseminated neuroblastoma was prevented in all mice expressing hINF-beta. Continued growth of established retroperitoneal tumors, treated with AAV hINF-beta as monotherapy, was significantly restricted, and survival for mice with established, disseminated disease was significantly prolonged following administration of AAV hINF-beta. Analysis of treated tumors revealed a significant antiangiogenic effect. Mean intratumoral vessel density was diminished and expression of the angiogenic factors vascular endothelial growth factor and basic fibroblast growth factor were both decreased. Finally, combination therapy in which AAV hIFN-beta was used together with low-dose cyclophosphamide resulted in regression of both established retroperitoneal and disseminated disease.

CONCLUSIONS

AAV-mediated delivery of hIFN-beta when used as monotherapy was able to restrict neuroblastoma growth due in part to inhibition of angiogenesis. When used in combination with conventional chemotherapy, AAV hIFN-beta was able to effect complete tumor regression.

摘要

目的

I型干扰素（IFN-α/β）在临床前模型中已显示出显著的抗肿瘤活性，但在临床试验中的疗效有限且毒性显著。我们假设通过慢性、低剂量全身给药可增强I型干扰素的抗肿瘤活性，并试图在小鼠神经母细胞瘤模型中进行验证。

实验设计

通过使用编码人干扰素-β（hIFN-β）的腺相关病毒载体的基因治疗介导方法，实现人干扰素-β（hIFN-β）在肝脏的持续表达。使用三种不同的异种移植建立神经母细胞瘤的原位局部腹膜后和播散模型。采用免疫组织化学分析和酶联免疫吸附测定法评估治疗的抗血管生成作用。

结果

在所有表达hIFN-β的小鼠中，局部原位（腹膜后）和播散性神经母细胞瘤的发展均得到抑制。作为单一疗法用AAV hIFN-β治疗的已建立的腹膜后肿瘤的持续生长受到显著限制，并且在给予AAV hIFN-β后，患有已建立的播散性疾病的小鼠的生存期显著延长。对治疗肿瘤的分析显示出显著的抗血管生成作用。肿瘤内平均血管密度降低，血管生成因子血管内皮生长因子和碱性成纤维细胞生长因子的表达均降低。最后，AAV hIFN-β与低剂量环磷酰胺联合治疗导致已建立的腹膜后和播散性疾病均消退。