An optimal promoter regulating cytokine transgene expression is crucial for safe and effective oncolytic virus immunotherapy

IF 6.4 2区 医学 Q1 MEDICAL LABORATORY TECHNOLOGY
Hirotaka Kawakami , Nobuhiro Ijichi , Yuki Obama , Eriko Matsuda , Kaoru Mitsui , Yuya Nishikawaji , Maki Watanabe , Satoshi Nagano , Noboru Taniguchi , Setsuro Komiya , Ken-ichiro Kosai
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Abstract

In general, ensuring safety is the top priority of a new modality. Although oncolytic virus armed with an immune stimulatory transgene (OVI) showed some promise, the strategic concept of simultaneously achieving maximum effectiveness and minimizing side effects has not been fully explored. We generated a variety of survivin-responsive “conditionally replicating adenoviruses that can target and treat cancer cells with multiple factors (m-CRAs)” (Surv.m-CRAs) armed with the granulocyte-macrophage colony-stimulating factor (GM-CSF) transgene downstream of various promoters using our m-CRA platform technology. We carefully analyzed both therapeutic and adverse effects of them in the in vivo syngeneic Syrian hamster cancer models. Surprisingly, an intratumor injection of a conventional OVI, which expresses the GM-CSF gene under the constitutively and strongly active “cytomegalovirus enhancer and β-actin promoter”, provoked systemic and lethal GM-CSF circulation and shortened overall survival (OS). In contrast, a new conceptual type of OVI, which expressed GM-CSF under the cancer-predominant and mildly active E2F promoter or the moderately active “Rous sarcoma virus long terminal repeat”, not only abolished lethal adverse events but also prolonged OS and systemic anti-cancer immunity. Our study revealed a novel concept that optimal expression levels of an immune stimulatory transgene regulated by a suitable upstream promoter is crucial for achieving high safety and maximal therapeutic effects simultaneously in OVI therapy. These results pave the way for successful development of the next-generation OVI and alert researchers about possible problems with ongoing clinical trials.

调节细胞因子转基因表达的最佳启动子对于安全有效的溶瘤病毒免疫疗法至关重要。
一般来说,确保安全是新方法的首要任务。虽然带有免疫刺激转基因(OVI)的溶瘤病毒显示出一定的前景,但同时实现最大疗效和最小副作用的战略概念尚未得到充分探索。我们利用 m-CRA 平台技术,在不同启动子的下游生成了多种具有存活素响应的 "条件复制腺病毒,可通过多种因子(m-CRAs)靶向治疗癌细胞"(Surv.m-CRAs),这些病毒带有粒细胞-巨噬细胞集落刺激因子(GM-CSF)转基因。我们仔细分析了它们在体内叙利亚仓鼠癌症模型中的治疗效果和不良反应。令人惊讶的是,在组成型强活性 "巨细胞病毒增强子和β-肌动蛋白启动子 "下表达GM-CSF基因的传统OVI的瘤内注射会引起全身性致命的GM-CSF循环,并缩短总生存期(OS)。与此相反,一种新概念的 OVI,即在以癌症为主的轻度活跃的 E2F 启动子或中度活跃的 "Rous 肉瘤病毒长末端重复 "下表达 GM-CSF,不仅消除了致死性不良事件,而且延长了 OS 和全身抗癌免疫。我们的研究揭示了一个新的概念,即由合适的上游启动子调控的免疫刺激转基因的最佳表达水平,是同时获得高安全性和最大治疗效果的关键。这些结果为成功开发下一代 OVI 铺平了道路,并提醒研究人员注意正在进行的临床试验中可能出现的问题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Translational Research
Translational Research 医学-医学:内科
CiteScore
15.70
自引率
0.00%
发文量
195
审稿时长
14 days
期刊介绍: Translational Research (formerly The Journal of Laboratory and Clinical Medicine) delivers original investigations in the broad fields of laboratory, clinical, and public health research. Published monthly since 1915, it keeps readers up-to-date on significant biomedical research from all subspecialties of medicine.
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