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抗坏血酸通过氧化还原循环外源性/内源性铜离子和生成活性氧物种来实现癌症的催化治疗。

Catalytic therapy of cancer by ascorbic acid involves redox cycling of exogenous/endogenous copper ions and generation of reactive oxygen species.

机构信息

Department of Biochemistry, Faculty of Life Sciences, Aligarh Muslim University, Aligarh, India.

出版信息

Chemotherapy. 2010;56(4):280-4. doi: 10.1159/000319951. Epub 2010 Aug 11.

Abstract

Catalytic therapy is a cancer treatment modality based on the generation of reactive oxygen species (ROS) through administration of ascorbate/medicinal herbal extracts and copper. It is known that antioxidants such as ascorbate also exhibit prooxidant activity in the presence of transition metals such as copper. Based on our work and that in the literature, in this review we propose a mechanism for the cytotoxic action of ascorbate against cancer cells. It involves redox cycling of exogenous/endogenous copper ions and the consequent generation of ROS leading to oxidative DNA breakage. Using human peripheral lymphocytes and the Comet assay, we have shown that ascorbic acid is able to cause oxidative breakage in cellular DNA. Such DNA degradation is inhibited by neocuproine (a Cu(I) sequestering agent) and scavengers of ROS indicating that the cellular DNA breakage involves the generation of Cu(I) and formation of ROS. Similar results are also obtained with plant polyphenol antioxidants that are important constituents of medicinal herbal extracts. Copper is an essential component of chromatin and can take part in redox reactions. It is well established that tissue, cellular and serum copper levels are considerably elevated in various malignancies. Therefore, cancer cells may be more subject to electron transfer between copper ions and ascorbate/plant polyphenols to generate ROS. In this review we cite evidence to indicate that in catalytic therapy cytotoxic action against cancer cells involves redox cycling of exogenous/endogenous copper ions.

摘要

催化疗法是一种基于通过给予抗坏血酸/草药提取物和铜来产生活性氧物种 (ROS) 的癌症治疗方式。众所周知,抗氧化剂如抗坏血酸在存在过渡金属如铜的情况下也表现出促氧化剂活性。基于我们的工作和文献中的工作,在这篇综述中,我们提出了抗坏血酸对癌细胞的细胞毒性作用的机制。它涉及外源性/内源性铜离子的氧化还原循环,以及由此产生的导致氧化 DNA 断裂的 ROS。使用人外周淋巴细胞和彗星试验,我们已经表明抗坏血酸能够引起细胞 DNA 的氧化断裂。这种 DNA 降解被 neocuproine(一种 Cu(I) 螯合剂)和 ROS 的清除剂抑制,表明细胞 DNA 断裂涉及 Cu(I) 的生成和 ROS 的形成。植物多酚抗氧化剂也得到了类似的结果,它们是草药提取物的重要成分。铜是染色质的必需组成部分,并且可以参与氧化还原反应。已经证实,各种恶性肿瘤中的组织、细胞和血清铜水平显着升高。因此,癌细胞可能更容易发生铜离子和抗坏血酸/植物多酚之间的电子转移,以产生 ROS。在这篇综述中,我们引用了证据表明,在催化疗法中,对癌细胞的细胞毒性作用涉及外源性/内源性铜离子的氧化还原循环。

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