Freytag Svend O, Paielli Dell, Wing Mark, Rogulski Ken, Brown Steve, Kolozsvary Andy, Seely John, Barton Ken, Dragovic Alek, Kim Jae Ho
Department of Radiation Oncology, Henry Ford Health Systems, Detroit, MI 48202, USA.
Int J Radiat Oncol Biol Phys. 2002 Nov 1;54(3):873-85. doi: 10.1016/s0360-3016(02)03005-5.
The purpose of this study was to evaluate the efficacy and toxicity of replication-competent adenovirus-mediated double suicide gene therapy in an adjuvant setting with external beam radiation therapy (EBRT) in an experimental prostate cancer model in preparation for a Phase I clinical study in humans.
For efficacy studies, i.m. DU145 and intraprostatic LNCaP C4-2 tumors were established in immune-deficient mice. Tumors were injected with the lytic, replication-competent Ad5-CD/TKrep adenovirus containing a cytosine deaminase (CD)/herpes simplex virus thymidine kinase (HSV-1 TK) fusion gene. Two days later, mice were administered 1 week of 5-fluorocytosine + ganciclovir (GCV) prodrug therapy and fractionated doses of EBRT (trimodal therapy). Tumor control rate of trimodal therapy was compared to that of EBRT alone. For toxicology studies, immune-competent male mice received a single intraprostatic injection (10(10) vp) of the replication-competent Ad5-CD/TKrep adenovirus. Two days later, mice were administered 4 weeks of 5-fluorocytosine + GCV prodrug therapy and 56 Gy EBRT to the pelvic region. The toxicity of trimodal therapy was assessed by histopathologic analysis of major organs and clinical chemistries.
In both the i.m. DU145 and intraprostatic LNCaP C4-2 tumor models, trimodal therapy significantly improved primary tumor control beyond that of EBRT alone. In the DU145 model, trimodal therapy resulted in a tumor growth delay (70 days) that was more than twice that (32 days) of EBRT alone. Whereas EBRT failed to eradicate DU145 tumors, trimodal therapy resulted in 25% tumor cure. In the LNCaP C4-2 tumor model, EBRT slowed the growth of intraprostatic tumors, but resulted in no tumor cures, and 57% of the mice developed retroperitoneal lymph node metastases at 3 months. By contrast, trimodal therapy resulted in 44% tumor cure and reduced significantly the percentage (13%) of lymph node metastases relative to EBRT alone. Overall, trimodal therapy was associated with little toxicity. A comparison of the major histopathologic findings among the treatment groups indicated that most of the locoregional (prostate, seminal vesicles, urinary bladder) pathology was attributable to the combined effects of the Ad5-CD/TKrep vector and EBRT and that the prodrugs contributed little to this effect. Importantly, trimodal therapy did not exacerbate inflammation of the rectum and intestines beyond that of EBRT alone.
Together, the results support the thesis that replication-competent adenovirus-mediated double suicide gene therapy may be a safe and effective adjuvant to EBRT and provide a sound scientific rationale for human trials.
本研究旨在评估在实验性前列腺癌模型中,具有复制能力的腺病毒介导的双自杀基因疗法联合外照射放疗(EBRT)作为辅助治疗的疗效和毒性,为开展人体I期临床研究做准备。
为进行疗效研究,在免疫缺陷小鼠中建立了皮下DU145肿瘤和前列腺内LNCaP C4-2肿瘤。将含有胞嘧啶脱氨酶(CD)/单纯疱疹病毒胸苷激酶(HSV-1 TK)融合基因的具有裂解能力、可复制的Ad5-CD/TKrep腺病毒注射到肿瘤内。两天后,给小鼠进行为期1周的5-氟胞嘧啶+更昔洛韦(GCV)前药治疗以及分次剂量的EBRT(三联疗法)。将三联疗法的肿瘤控制率与单纯EBRT的控制率进行比较。为进行毒理学研究,免疫健全的雄性小鼠接受一次前列腺内注射(10¹⁰病毒粒子)具有复制能力的Ad5-CD/TKrep腺病毒。两天后,给小鼠进行为期4周的5-氟胞嘧啶+GCV前药治疗以及对盆腔区域进行56 Gy的EBRT。通过对主要器官的组织病理学分析和临床化学检测来评估三联疗法的毒性。
在皮下DU145肿瘤模型和前列腺内LNCaP C4-2肿瘤模型中,三联疗法均显著提高了对原发肿瘤的控制,效果优于单纯EBRT。在DU145模型中,三联疗法使肿瘤生长延迟(70天),这是单纯EBRT(32天)的两倍多。单纯EBRT未能根除DU145肿瘤,而三联疗法使25%的肿瘤得到治愈。在LNCaP C4-2肿瘤模型中,EBRT减缓了前列腺内肿瘤的生长,但未实现肿瘤治愈,并且57%的小鼠在3个月时出现了腹膜后淋巴结转移。相比之下,三联疗法使44%的肿瘤得到治愈,并且相对于单纯EBRT,显著降低了淋巴结转移的比例(13%)。总体而言,三联疗法的毒性较小。各治疗组主要组织病理学结果的比较表明,大多数局部区域(前列腺、精囊、膀胱)的病理改变归因于Ad5-CD/TKrep载体和EBRT的联合作用,前药对此作用的贡献较小。重要的是,三联疗法并未使直肠和肠道的炎症比单纯EBRT更严重。
总之,这些结果支持以下论点,即具有复制能力的腺病毒介导的双自杀基因疗法可能是EBRT的一种安全有效的辅助疗法,并为人体试验提供了可靠的科学依据。
Zotero 插件