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新铜试剂,一种选择性铜(I)螯合剂,以及S-亚硝基硫醇对大鼠血管平滑肌的舒张作用。

Neocuproine, a selective Cu(I) chelator, and the relaxation of rat vascular smooth muscle by S-nitrosothiols.

作者信息

Al-Sa'doni H H, Megson I L, Bisland S, Butler A R, Flitney F W

机构信息

School of Chemistry, University of St Andrews, Fife.

出版信息

Br J Pharmacol. 1997 Jul;121(6):1047-50. doi: 10.1038/sj.bjp.0701218.

Abstract
  1. A study has been made of the effect of neocuproine, a specific Cu(I) chelator, on vasodilator responses of rat isolated perfused tail artery to two nitrosothiols: S-nitroso-N-acetyl-D,L-penicillamine (SNAP) and S-nitroso-glutathione (GSNO). 2. Bolus injections (10 microl) of SNAP or GSNO (10(-7)-10(-3) M) were delivered into the lumen of perfused vessels pre-contracted with sufficient phenylephrine (1-7 microM) to develop pressures of 100-120 mmHg. Two kinds of experiment were made: SNAP and GSNO were either (a) pre-mixed with neocuproine (10(-4) M) and then injected into arteries; or (b) vessels were continuously perfused with neocuproine (10(-5) M) and then injected with either pure SNAP or GSNO. 3. In each case, neocuproine significantly attenuated vasodilator responses to both nitrosothiols, although the nature of the inhibitory effect differed in the two types of experiment. We conclude that the ability of exogenous nitrosothiols to relax vascular smooth muscle in our ex vivo model is dependent upon a Cu(I) catalyzed process. Evidence is presented which suggests that a similar Cu(I)-dependent mechanism is responsible for the release of NO from endogenous nitrosothiols and that this process may assist in maintaining vasodilator tone in vivo.
摘要
  1. 已对一种特定的铜(I)螯合剂新亚铜试剂对大鼠离体灌注尾动脉对两种亚硝基硫醇:S-亚硝基-N-乙酰-D,L-青霉胺(SNAP)和S-亚硝基谷胱甘肽(GSNO)的血管舒张反应的影响进行了研究。2. 将SNAP或GSNO(10⁻⁷ - 10⁻³ M)以10微升的推注量注入预先用足够的去氧肾上腺素(1 - 7 microM)预收缩至压力达100 - 120 mmHg的灌注血管腔内。进行了两种实验:SNAP和GSNO要么(a)与新亚铜试剂(10⁻⁴ M)预混合后再注入动脉;要么(b)血管用新亚铜试剂(10⁻⁵ M)持续灌注,然后注入纯SNAP或GSNO。3. 在每种情况下,新亚铜试剂均显著减弱了对两种亚硝基硫醇的血管舒张反应,尽管在两种实验类型中抑制作用的性质有所不同。我们得出结论,在外源亚硝基硫醇使我们离体模型中的血管平滑肌舒张的能力取决于铜(I)催化的过程。有证据表明,类似的依赖铜(I)的机制负责内源性亚硝基硫醇释放一氧化氮,并且该过程可能有助于在体内维持血管舒张张力。

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