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携带白细胞介素-2基因的脂质体-DNA复合物在患有骨肉瘤肺转移的犬中的I期研究。

Phase I study of liposome-DNA complexes encoding the interleukin-2 gene in dogs with osteosarcoma lung metastases.

作者信息

Dow Steven, Elmslie Robyn, Kurzman Ilene, MacEwen Gregory, Pericle Federica, Liggitt Denny

机构信息

Department of Clinical Sciences, Colorado State University, Fort Collins, 80523, USA.

出版信息

Hum Gene Ther. 2005 Aug;16(8):937-46. doi: 10.1089/hum.2005.16.937.

DOI:10.1089/hum.2005.16.937
PMID:16076252
Abstract

Systemic gene delivery using cationic liposome-DNA complexes (LDCs) has been shown to elicit potent antitumor activity in mice with tumor metastases to the lungs. However, intravenous gene delivery for treatment of established cancer has not been evaluated previously in a spontaneous, large animal model. We therefore evaluated the safety, toxicity, and efficacy of intravenous gene delivery, using LDCs in dogs with established tumor metastases. Twenty dogs with chemotherapy-resistant osteosarcoma metastases to the lungs received a series of intravenous infusions of cationic liposomes and plasmid DNA encoding the canine interleukin-2 (IL-2) cDNA. Effects of intravenous gene delivery on immune activation, clinical and hematologic parameters, tumor responses, and survival times were assessed. We found that slow intravenous administration of IL-2 LDCs resulted in detectable IL-2 transgene expression in lung tissues of dogs. Repeated intravenous infusions of LDCs were well tolerated by dogs with lung tumor metastases and elicited systemic immune activation, as reflected by fever, leukogram changes, monocyte activation, and increased natural killer cell activity. Three of 20 dogs experienced partial or complete regression of lung metastases after infusion of IL-2 LDCs. Overall survival times were significantly increased in treated dogs compared with historical control animals with the same stage of disease. We conclude that repeated intravenous infusion of LDCs in cancerbearing dogs is safe and well tolerated at low doses and may be capable of eliciting antitumor activity in some animals with advanced tumor metastases.

摘要

使用阳离子脂质体 - DNA复合物(LDCs)进行全身基因递送已被证明在肺部有肿瘤转移的小鼠中能引发强大的抗肿瘤活性。然而,静脉内基因递送用于治疗已确诊的癌症此前尚未在自发的大型动物模型中进行评估。因此,我们评估了在患有已确诊肿瘤转移的犬中使用LDCs进行静脉内基因递送的安全性、毒性和疗效。二十只患有化疗耐药性骨肉瘤肺转移的犬接受了一系列阳离子脂质体和编码犬白细胞介素 - 2(IL - 2)cDNA的质粒DNA的静脉输注。评估了静脉内基因递送对免疫激活、临床和血液学参数、肿瘤反应及生存时间的影响。我们发现,缓慢静脉内给予IL - 2 LDCs可导致犬肺组织中可检测到IL - 2转基因表达。患有肺肿瘤转移的犬对重复静脉输注LDCs耐受性良好,并引发全身免疫激活,表现为发热、白细胞计数变化、单核细胞激活和自然杀伤细胞活性增加。20只犬中有3只在输注IL - 2 LDCs后肺转移灶出现部分或完全消退。与处于相同疾病阶段的历史对照动物相比,治疗犬的总体生存时间显著延长。我们得出结论,在患癌犬中重复静脉输注LDCs在低剂量时是安全且耐受性良好的,并且可能能够在一些患有晚期肿瘤转移的动物中引发抗肿瘤活性。

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