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Is S-Nitrosocysteine a True Surrogate for Nitric Oxide?

机译:S-亚硝基半胱氨酸是否是一氧化氮的真正替代物?

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摘要

S-Nitrosothiol (RSNO) formation is one manner by which nitric oxide (•NO) exerts its biological effects. There are several proposed mechanisms of formation of RSNO in vivo: auto-oxidation of •NO, transnitrosation, oxidative nitrosylation, and from dinitrosyliron complexes (DNIC). Both free •NO, generated by •NO donors, and S-nitrosocysteine (CysNO) are widely used to study •NO biology and signaling, including protein S-nitrosation. It is assumed that the cellular effects of both compounds are analogous and indicative of in vivo •NO biology. A quantitative comparison was made of formation of DNIC and RSNO, the major •NO-derived cellular products. In RAW 264.7 cells, both •NO and CysNO were metabolized, leading to rapid intracellular RSNO and DNIC formation. DNIC were the dominant products formed from physiologic •NO concentrations, however, and RSNO were the major product from CysNO treatment. Chelatable iron was necessary for DNIC assembly from either •NO or CysNO, but not for RSNO formation. These profound differences in RSNO and DNIC formation from •NO and CysNO question the use of CysNO as a surrogate for physiologic •NO. Researchers designing experiments intended to elucidate the biological signaling mechanisms of •NO should be aware of these differences and should consider the biological relevance of the use of exogenous CysNO. Antioxid. Redox Signal. 17, 962–968.
机译:S-亚硝基硫醇(RSNO)的形成是一氧化氮(•NO)发挥其生物学效应的一种方式。体内存在几种形成RSNO的机制:NO的自动氧化,反硝化,氧化性亚硝基化以及由二亚硝基铁络合物(DNIC)形成。由•NO供体产生的游离•NO和S-亚硝基半胱氨酸(CysNO)都广泛用于研究•NO生物学和信号传导,包括蛋白质S-亚硝化。假定这两种化合物的细胞效应是相似的,并指示体内NO生物学。对主要来源于•NO的细胞产物DNIC和RSNO的形成进行了定量比较。在RAW 264.7细胞中,•NO和CysNO均被代谢,导致快速的细胞内RSNO和DNIC形成。 DNIC是由生理浓度•NO形成的主要产物,而RSNO是CysNO处理的主要产物。从•NO或CysNO进行DNIC组装需要螯合铁,但对于形成RSNO则不需要。 •NO和CysNO在RSNO和DNIC形成方面的这些深远差异,使人们将CysNO用作生理•NO的替代品。设计用于阐明•NO的生物信号传导机制的实验的研究人员应意识到这些差异,并应考虑使用外源CysNO的生物学相关性。抗氧化。氧化还原信号。 17,962-968。

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