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利用氧化还原调节小分子,这些小分子在癌细胞中选择性地作为促氧化剂发挥作用,为改善癌症治疗打开一个治疗窗口。

Utilization of redox modulating small molecules that selectively act as pro-oxidants in cancer cells to open a therapeutic window for improving cancer therapy.

机构信息

Department of Radiation Oncology, University of Iowa, Iowa City, IA, USA.

Department of Cancer Biology, University of Iowa, Iowa City, IA, USA.

出版信息

Redox Biol. 2021 Jun;42:101864. doi: 10.1016/j.redox.2021.101864. Epub 2021 Jan 16.

Abstract

There is a rapidly growing body of literature supporting the notion that differential oxidative metabolism in cancer versus normal cells represents a metabolic frailty that can be exploited to open a therapeutic window into cancer therapy. These cancer cell-specific metabolic frailties may be amenable to manipulation with non-toxic small molecule redox active compounds traditionally thought to be antioxidants. In this review we describe the potential mechanisms and clinical applicability in cancer therapy of four small molecule redox active agents: melatonin, vitamin E, selenium, and vitamin C. Each has shown the potential to have pro-oxidant effects in cancer cells while retaining antioxidant activity in normal cells. This dichotomy can be exploited to improve responses to radiation and chemotherapy by opening a therapeutic window based on a testable biochemical rationale amenable to confirmation with biomarker studies during clinical trials. Thus, the unique pro-oxidant/antioxidant properties of melatonin, vitamin E, selenium, and vitamin C have the potential to act as effective adjuvants to traditional cancer therapies, thereby improving cancer patient outcomes.

摘要

越来越多的文献支持这样一种观点,即癌症与正常细胞之间的代谢差异代表了一种代谢脆弱性,可以利用这种脆弱性为癌症治疗开辟一个治疗窗口。这些癌细胞特有的代谢脆弱性可能可以通过使用传统上被认为是抗氧化剂的无毒小分子氧化还原活性化合物来进行操纵。在这篇综述中,我们描述了四种小分子氧化还原活性化合物在癌症治疗中的潜在机制和临床适用性:褪黑素、维生素 E、硒和维生素 C。它们都显示出在癌细胞中具有促氧化作用,而在正常细胞中保持抗氧化活性的潜力。这种二分法可以通过打开一个基于可测试的生化原理的治疗窗口来提高对辐射和化疗的反应,这种原理在临床试验中可以通过生物标志物研究进行确认。因此,褪黑素、维生素 E、硒和维生素 C 的独特的促氧化/抗氧化特性有可能作为传统癌症治疗的有效辅助手段,从而改善癌症患者的预后。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d1b5/8113052/32ddf8fc71d9/gr1.jpg

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