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声孔介导的实体瘤免疫基因治疗。

Sonoporation mediated immunogene therapy of solid tumors.

机构信息

Cork Cancer Research Centre, Mercy University Hospital, University College Cork, Cork, Ireland.

出版信息

Ultrasound Med Biol. 2010 Mar;36(3):430-40. doi: 10.1016/j.ultrasmedbio.2009.11.005. Epub 2010 Feb 4.

DOI:10.1016/j.ultrasmedbio.2009.11.005
PMID:20133039
Abstract

Development of gene-based therapies for the treatment of inherited and acquired diseases, including cancer, has seen renewed interest in the use of nonviral vectors coupled to physical delivery modalities. Low-frequency ultrasound (US), with a well-established record in a clinical setting, has the potential to deliver DNA efficiently, accurately and safely. Optimal in vivo parameters for US-mediated delivery of naked plasmid DNA were established using the firefly luciferase reporter gene construct. Optimized parameters were used to administer a therapeutic gene construct, coding for granulocyte-macrophage colony-stimulating factor (GM-CSF) and B7-1 costimulatory molecule, to growing murine fibrosarcoma tumors. Tumor progression and animal survival was monitored throughout the study and the efficacy of the US-mediated gene therapy determined and compared with an electroporation-based approach. Optimal parameters for US-mediated delivery of plasmid DNA to tumors were deduced to be 1.0 W/cm(2) at 20% duty cycle for 5 min (60 J/cm(2)). In vivo US-mediated gene therapy resulted in a 55% cure rate in tumor-bearing animals. The immunological response invoked was cell mediated, conferring resistance against re-challenge and resistance to tumor challenge after transfer of splenocytes to naïve animals. US treatment was noninjurious to treated tissue, whereas therapeutic efficacy was comparable to an electroporation-based approach. US-mediated delivery of an immune-gene construct to growing tumors was therapeutically effective. Sonoporation has the potential to be a major factor in the development of nonviral gene delivery approaches.

摘要

基因治疗方法的发展可用于治疗遗传性和获得性疾病,包括癌症,人们对与物理传递方式相结合的非病毒载体的使用重新产生了兴趣。低频超声(US)在临床环境中有良好的记录,具有高效、准确和安全地传递 DNA 的潜力。使用萤火虫荧光素酶报告基因构建体,确定了用于 US 介导的裸质粒 DNA 传递的最佳体内参数。优化后的参数用于管理编码粒细胞-巨噬细胞集落刺激因子(GM-CSF)和 B7-1 共刺激分子的治疗基因构建体,用于生长中的鼠纤维肉瘤肿瘤。在整个研究过程中监测肿瘤进展和动物生存情况,并确定和比较 US 介导的基因治疗的疗效与电穿孔方法。推断出用于将质粒 DNA递送至肿瘤的 US 介导的最佳参数为 1.0 W/cm(2),占空比为 20%,持续 5 分钟(60 J/cm(2))。体内 US 介导的基因治疗导致荷瘤动物的治愈率达到 55%。引发的免疫反应是细胞介导的,赋予了对再挑战的抵抗力,并在将脾细胞转移到新生动物后抵抗肿瘤挑战。US 治疗对治疗组织没有伤害性,而治疗效果与电穿孔方法相当。US 介导的免疫基因构建体向生长中的肿瘤的传递具有治疗效果。声孔作用有可能成为非病毒基因传递方法发展的主要因素。

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