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首页> 外文期刊>Biochemical Society Transactions >Structures and reaction pathways of the molybdenum centres of sulfite-oxidizing enzymes by pulsed EPR spectroscopy.
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Structures and reaction pathways of the molybdenum centres of sulfite-oxidizing enzymes by pulsed EPR spectroscopy.

机译:通过脉冲EPR光谱法,亚硫酸盐氧化酶的钼中心的结构和反应途径。

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摘要

SOEs (sulfite-oxidizing enzymes) are physiologically vital and occur in all forms of life. During the catalytic cycle, the five-co-ordinate square pyramidal oxo-molybdenum active site passes through the Mo(V) state, and intimate details of the structure can be obtained from variable frequency pulsed EPR spectroscopy through the hyperfine and nuclear quadrupole interactions of nearby magnetic nuclei. By employing variable spectrometer operational frequencies, it is possible to optimize the measurement conditions for difficult quadrupolar nuclei of interest (e.g. (17)O, (33)S, (35)Cl and (37)Cl) and to simplify the interpretation of the spectra. Isotopically labelled model Mo(V) compounds provide further insight into the electronic and geometric structures and chemical reactions of the enzymes. Recently, blocked forms of SOEs having co-ordinated sulfate, the reaction product, were detected using (33)S (I=3/2) labelling. This blocking of product release is a possible contributor to fatal human sulfite oxidase deficiency in young children.
机译:企业(亚硫酸盐氧化酶)在生理上至关重要,并且发生在各种形式的生命中。在催化循环中,五层级的正方形锥体氧气 - 氧化螺旋活性位点通过MO(v)状态,并且可以从可变的频率脉冲EPR光谱通过超精细和核精细的四螺杆相互作用获得结构的密切细节。附近的磁核。通过采用可变光谱仪的操作频率,可以优化引起的困难四极核的测量条件(例如(17)o,(33)s,(35)cl和(37)cl),并简化对解释的解释。光谱。同位素标记的模型MO(V)化合物提供了对酶的电子和几何结构以及化学反应的进一步见解。最近,使用(33)s(i = 3/2)标记检测到具有硫酸硫酸盐(硫酸盐)的阻塞形式。产品释放的这种阻断是幼儿致命的人硫酸盐氧化酶缺乏的可能性。

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