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监测肿瘤中实际一氧化氮浓度的必要性。

The need for monitoring the actual nitric oxide concentration in tumors.

作者信息

Heller Adam

机构信息

Department of Chemical Engineering, University of Texas, Austin, TX 78712 USA.

出版信息

Bioanal Rev. 2009 Dec;1(1):3-6. doi: 10.1007/s12566-009-0003-0. Epub 2009 Jun 3.

Abstract

The significance of the role of nitric oxide (NO) in cancer is evident from 1,100 publications on the subject; its triggering of apoptosis at high concentrations is documented in 300 publications. While aspects of the rate of generation of NO in tumors have been extensively studied, the rate of its removal from tumors has not been considered, even though it is the difference between the two rates that determines the all important steady-state NO concentration, and thus the likelihood of apoptosis-triggering. The rate of transport of NO scales with its concentration gradient at the interface between a neoplasm and the phase to which it diffuses, which can be air, fat, or blood. Diffusional loss of NO to air would explain the initial two-dimensionality of neoplasms of the skin and lung. The greater solubility of NO in lipids than in aqueous phases should cause its extraction by nearby fat, and would account for the positive correlation between obesity and the incidence of some cancers, such as cancers of the breast. And the rapid consumption of NO by red blood cells implies depletion of excess NO in tumors after they are vascularized: angiogenesis should blunt any apoptosis-triggering NO attack of the immune system. Thus, cancer research and the practice of oncology may benefit of in-tumor monitoring of the actual NO concentration. Miniature NO monitoring electrodes, that might serve the purpose, are reviewed.

摘要

一氧化氮(NO)在癌症中的作用的重要性从1100篇关于该主题的出版物中可见一斑;其在高浓度下引发细胞凋亡的现象在300篇出版物中有记载。虽然肿瘤中NO生成速率的各个方面已得到广泛研究,但尚未考虑其从肿瘤中清除的速率,尽管正是这两个速率之间的差异决定了至关重要的稳态NO浓度,进而决定了引发细胞凋亡的可能性。NO的传输速率与其在肿瘤与它扩散到的相(可以是空气、脂肪或血液)之间的界面处的浓度梯度成正比。NO向空气中的扩散损失可以解释皮肤和肺部肿瘤最初的二维特性。NO在脂质中的溶解度高于水相,这应使其被附近的脂肪提取,并可解释肥胖与某些癌症(如乳腺癌)发病率之间的正相关。红细胞对NO的快速消耗意味着肿瘤血管化后肿瘤中过量的NO会被耗尽:血管生成应会减弱免疫系统任何引发细胞凋亡的NO攻击。因此,癌症研究和肿瘤学实践可能会受益于对肿瘤内实际NO浓度的监测。本文综述了可能用于此目的的微型NO监测电极。

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