Zweiri Jehad, Christmas Stephen E
1Department of Molecular Medicine, King's College London, The Rayne Institute, 123 Coldharbour Lane, London, SE5 9NU UK.
2Department of Clinical Infection & Immunology, Institute of Infection & Global Health, University of Liverpool, Ronald Ross Building, 8, West Derby St, Liverpool, L69 7BE UK.
Cancer Cell Int. 2020 Jan 28;20:26. doi: 10.1186/s12935-020-1115-4. eCollection 2020.
Therapeutic approaches for cancer rely on careful consideration of finding the optimal way of delivering the pro-drug for cellular-based cancer treatment. Cell lines and cell cultures have been used in these studies to compare the in vitro and in vivo efficacy of autologous vs. allogeneic tumour cellular gene therapy. Here we have investigated and are reporting for the first time the effect of prodrug ganciclovir (GCV)-preloading (pre-treatment) in suicide gene therapy of cancer.
This study examines the effect of GCV-preloading (pre-treatment) on a range of tumour cell lines in conjunction with suicide gene therapy of cancer. To determine the efficacy of this modality, a series of in vitro and in vivo experiments were conducted using genetically modified and unmodified tumour cell lines.
Following co-culture of herpes simplex virus thymidine kinase (HSV-TK) modified tumour cells and unmodified tumour cells both in vitro and in vivo, GCV-preloading (pre-treatment) of TK-modified human and mouse mesothelioma cells and ovarian tumour cells allowed them to mediate efficiently bystander killing of neighbouring unmodified tumour cells in vitro. In contrast, GCV-preloading of TK-modified human and mouse mesothelioma cells and ovarian tumour cells abolished their in vivo ability to induce bystander killing of unmodified tumour cells, although there was some tumour regression compared to control groups but this was not statistically significant. These results suggest that preloading TK modified tumour cells with GCV needs further study to define the most effective strategy for an in vivo application to retain their bystander killing potential after exposure to lethal doses of GCV in vitro.
This study highlights the promising possibility of improving the efficacy of pro-drug system to prevent any damage to the immune system and enhancing this type of suicide gene therapy of cancer, as well as the need for further studies to explore the discrepancies between in vitro and in vivo results.
癌症治疗方法依赖于仔细考虑找到将前药递送至细胞以进行基于细胞的癌症治疗的最佳方式。细胞系和细胞培养物已用于这些研究,以比较自体与异体肿瘤细胞基因治疗的体外和体内疗效。在此,我们首次研究并报告了前药更昔洛韦(GCV)预加载(预处理)在癌症自杀基因治疗中的作用。
本研究考察了GCV预加载(预处理)联合癌症自杀基因治疗对一系列肿瘤细胞系的影响。为了确定这种治疗方式的疗效,使用基因修饰和未修饰的肿瘤细胞系进行了一系列体外和体内实验。
在体外和体内将单纯疱疹病毒胸苷激酶(HSV-TK)修饰的肿瘤细胞与未修饰的肿瘤细胞共培养后,GCV预加载(预处理)TK修饰的人及小鼠间皮瘤细胞和卵巢肿瘤细胞,使其在体外能够有效地介导对邻近未修饰肿瘤细胞的旁观者杀伤。相比之下,GCV预加载TK修饰的人及小鼠间皮瘤细胞和卵巢肿瘤细胞消除了它们在体内诱导未修饰肿瘤细胞旁观者杀伤的能力,尽管与对照组相比有一些肿瘤消退,但这在统计学上并不显著。这些结果表明,用GCV预加载TK修饰的肿瘤细胞需要进一步研究,以确定在体内应用的最有效策略,使其在体外暴露于致死剂量的GCV后仍保留旁观者杀伤潜力。
本研究突出了提高前药系统疗效以防止对免疫系统造成任何损害并增强这类癌症自杀基因治疗的前景,以及进一步研究以探索体外和体内结果差异的必要性。
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