Ru Q, Li W, Wang X, Zhang S, Chen L, Zhang Y, Ge Y, Zu Y, Liu Y, Zheng D
Institute of Basic Medical Sciences, Chinese Academy of Medical Sciences, Beijing, China.
National Institutes for Food and Drug Control, National Center for Safety Evaluation of Drugs, Beijing, China.
Cancer Gene Ther. 2017 Jun;24(6):251-258. doi: 10.1038/cgt.2017.12. Epub 2017 Apr 21.
The recombinant sTRAIL has been in clinical trial for various human malignancies. However, the half-life time of sTRAIL is very short, which might be an important factor influencing its clinical efficacy for cancer therapy. We previously reported the recombinant adeno-associated virus (AAV)-encoding sTRAIL-mediated sTRAIL expression in vivo up to 8 months and suppressed tumor growth markedly in mouse xenografts. In the present study, we further evaluated the clinical potency for cancer gene therapy and the safety in mouse and non-human primates. The mouse models with HCT-116, NCI-H460 and BEL-7402 cancers were injected intraperitoneally with a single dose of 1.0 × 10, 1.0 × 10 and 1.0 × 10 vg of rAAV2-sTRAIL virus, respectively. The cynomolgus monkeys were injected (i.m.) with a single dose of rAAV2-sTRAIL of 1 × 10, 3 × 10 and 1 × 10 vg, corresponding to 6-, 20- and 60-fold of intended use dosage for humans, respectively. The efficacy, pharmacology and toxicity of rAAV-sTRAIL in the animals were analyzed accordingly. The tumor inhibitory rates reached 44-76%, 48-52% and 55-74% in the three tumor models, respectively, and they had no influence on mouse spontaneous activity. Administration (s.c.) of a single dose of rAAV2-sTRAIL virus of 1.0 × 10 or 1.0 × 10 vg in mice with implanted tumor led to mainly distribution in the spleen, liver, implanted tumor, blood, injected site of muscle and bone marrow. Two weeks later, there was no rAAV2-sTRAIL detected in blood and bone marrow, and it significantly decreased in other tissues and organs and then gradually cleared away in 4-12 weeks after administration. There was no rAAV2-sTRAIL accumulation in the animal's body and no influence on the body weights. Administration (i.v.) did not cause animal death, and no dose-related abnormal clinical symptoms were found in the mice. There were no abnormal tissue and organ found in all animals. Long-term toxicity test in cynomolgus monkeys did not cause rAAV2-sTRAIL-related toxic and side effects, except that anti-AAV and anti-sTRAIL antibodies were generated. In conclusion, these data demonstrated that administration of rAAV2-sTRAIL in mice and in cynomolgus monkeys is safe without obvious toxic and side effects to the animals, and throw light on pharmacokinetics and safety in human clinical trials for cancer gene therapy.
重组sTRAIL已用于多种人类恶性肿瘤的临床试验。然而,sTRAIL的半衰期很短,这可能是影响其癌症治疗临床疗效的一个重要因素。我们之前报道了编码sTRAIL的重组腺相关病毒(AAV)在体内介导sTRAIL表达长达8个月,并显著抑制小鼠异种移植瘤的生长。在本研究中,我们进一步评估了其在癌症基因治疗中的临床潜力以及在小鼠和非人灵长类动物中的安全性。分别给患有HCT-116、NCI-H460和BEL-7402癌症的小鼠模型腹腔注射单剂量1.0×10、1.0×10和1.0×10 vg的rAAV2-sTRAIL病毒。给食蟹猴肌肉注射单剂量1×10、3×10和1×10 vg的rAAV2-sTRAIL,分别相当于人类预期使用剂量的6倍、20倍和60倍。相应地分析了rAAV-sTRAIL在动物体内的疗效、药理学和毒性。在三种肿瘤模型中,肿瘤抑制率分别达到44%-76%、48%-52%和
