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Oxidation therapy: the use of a reactive oxygen species-generating enzyme system for tumour treatment.

机译:氧化疗法:使用产生活性氧的酶系统进行肿瘤治疗。

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摘要

Oxygen radicals induce cytotoxicity via a variety of mechanisms, including DNA damage, lipid peroxidation and protein oxidation. Here, we explore the use of a polyethylene glycol (PEG)-stabilised enzyme capable of producing reactive oxygen species (ROS), glucose oxidase (GO), for the purpose of harnessing the cytotoxic potential of ROS for treating solid tumours. PEG-GO (200 U), administered by two intratumoral injections 3 h apart, produced a significant growth delay in subcutaneous rat 9L gliomas as compared with control animals receiving heat-denatured PEG-GO. Rats were protected from systemic toxicity by subsequent i.v. administration of PEG-superoxide dismutase (PEG-SOD) and PEG-catalase. In vivo tumour metabolic changes, monitored using 31P magnetic resonance spectroscopy (31P-MRS) 6 h following initial administration of PEG-GO, revealed a 96 +/- 2% reduction in the ATP/Pi ratio and a 0.72 +/- 0.10 unit decline in intracellular pH. A 3-fold sensitisation of 9L glioma cells in vitro to hydrogen peroxide could be achieved by a 24 h preincubation with buthionine sulphoximine (BSO). This study suggests that oxidation therapy, the use of an intratumoral ROS-generating enzyme system for the treatment of solid tumours, is a promising area which warrants further exploration.
机译:氧自由基通过多种机制诱导细胞毒性,包括DNA损伤,脂质过氧化和蛋白质氧化。在这里,我们探索使用能够产生活性氧(ROS)的聚乙二醇(PEG)稳定酶,葡萄糖氧化酶(GO),以利用ROS的细胞毒性潜力来治疗实体瘤。与接受热变性PEG-GO的对照动物相比,通过两次瘤内注射间隔3小时进行的PEG-GO(200 U)在皮下大鼠9L胶质瘤中产生了显着的生长延迟。随后的静脉注射保护大鼠免受全身毒性。 PEG超氧化物歧化酶(PEG-SOD)和PEG过氧化氢酶的管理。首次施用PEG-GO后6小时,使用31P磁共振波谱(31P-MRS)监测的体内肿瘤代谢变化显示,ATP / Pi比降低了96 +/- 2%,单位为0.72 +/- 0.10单位细胞内pH下降。通过用丁硫氨酸磺胺嘧啶(BSO)进行24小时预孵育,可以使9L胶质瘤细胞在体外对过氧化氢的敏感性提高3倍。这项研究表明,氧化疗法(使用瘤内产生ROS的酶系统治疗实体瘤)是一个有前途的领域,值得进一步探索。

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