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溶瘤痘苗病毒编码的抗VEGF单链抗体GLAF-1显著增强抗肿瘤治疗效果。

Anti-VEGF single-chain antibody GLAF-1 encoded by oncolytic vaccinia virus significantly enhances antitumor therapy.

作者信息

Frentzen Alexa, Yu Yong A, Chen Nanhai, Zhang Qian, Weibel Stephanie, Raab Viktoria, Szalay Aladar A

机构信息

Genelux Corporation, San Diego Science Center, San Diego, CA 92109, USA.

出版信息

Proc Natl Acad Sci U S A. 2009 Aug 4;106(31):12915-20. doi: 10.1073/pnas.0900660106. Epub 2009 Jul 15.

Abstract

We previously reported that the replication-competent vaccinia virus (VACV) GLV-1h68 shows remarkable oncolytic activity and efficacy in different animal models as a single treatment modality and also in combination with chemotherapy [Yu YA, et al. (2009) Mol Cancer Ther 8:141-151]. Here, we report the construction of 3 VACV strains encoding GLAF-1, a previously undescribed engineered single-chain antibody (scAb). This unique scAb is transcribed from 3 vaccinia promoters (synthetic early, early/late, and late) and directed against both human and murine VEGFs. The expression of GLAF-1 was demonstrated in cell cultures. Also, the replication efficiency of all GLAF-1-expressing VACV strains in cell culture was similar to that of the parental GLV-1h68 virus. Successful tumor-specific delivery and continued production of functional scAb derived from individual VACV strains were obtained in tumor xenografts following a single intravenous injection of the virus. The VACV strains expressing the scAb exhibited significantly enhanced therapeutic efficacy in comparison to treatment of human tumor xenografts with the parental virus GLV-1h68. This enhanced efficacy was comparable to the concomitant treatment of tumors with a one-time i.v. injection of GLV-1h68 and multiple i.p. injections of Avastin. Taken together, the VACV-mediated delivery and production of immunotherapeutic anti-VEGF scAb in colonized tumors may open the way for a unique therapy concept: tumor-specific, locally amplified drug therapy in humans.

摘要

我们之前报道过,具有复制能力的痘苗病毒(VACV)GLV-1h68作为单一治疗方式以及与化疗联合使用时,在不同动物模型中均显示出显著的溶瘤活性和疗效[Yu YA等人,(2009年)《分子癌症治疗》8:141 - 151]。在此,我们报告了3种编码GLAF-1的痘苗病毒株的构建,GLAF-1是一种先前未描述的工程化单链抗体(scAb)。这种独特的单链抗体由3个痘苗启动子(合成早期、早期/晚期和晚期)转录,并针对人和鼠的血管内皮生长因子(VEGF)。GLAF-1在细胞培养物中的表达得到了证实。此外,所有表达GLAF-1的痘苗病毒株在细胞培养中的复制效率与亲本GLV-1h68病毒相似。在单次静脉注射病毒后,在肿瘤异种移植模型中成功实现了源自单个痘苗病毒株的功能性单链抗体的肿瘤特异性递送和持续产生。与用亲本病毒GLV-1h68治疗人肿瘤异种移植模型相比,表达单链抗体的痘苗病毒株表现出显著增强的治疗效果。这种增强的疗效与一次性静脉注射GLV-1h68和多次腹腔注射阿瓦斯汀联合治疗肿瘤的效果相当。综上所述,痘苗病毒介导的免疫治疗性抗VEGF单链抗体在定植肿瘤中的递送和产生可能为一种独特的治疗理念开辟道路:人类肿瘤特异性、局部扩增的药物治疗。

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