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一氧化碳在生理温度下从肌红蛋白释放到溶液中的过程。

The escape process of carbon monoxide from myoglobin to solution at physiological temperature.

作者信息

Nishihara Yasutaka, Sakakura Masaaki, Kimura Yoshifumi, Terazima Masahide

机构信息

Department of Chemistry, Graduate School of Science, Kyoto University, Kyoto, 606-8502, Japan.

出版信息

J Am Chem Soc. 2004 Sep 29;126(38):11877-88. doi: 10.1021/ja038877w.

Abstract

The carbon monoxide (CO) docking sites involved in the ligand escape process from the iron atom in hem of myoglobin (Mb) to solution at physiological temperature were studied on the basis of the effect of xenon (Xe) on the ligand escape rate by the transient grating (TG) technique. The TG method provides a direct measurement of the changes in molecular volume. The apparent CO escaping rate and the volume contraction increase with increasing Xe pressure. The pressure dependence of the rate is consistent with that of the Xe population at the Xe(1) site. This result clearly shows that CO is trapped at the Xe(1) site before escaping to solvent in a Xe-free solution at room temperature. It is shown that only CO but not the trapped Xe is released by the photoexcitation of the Xe-trapped MbCO. A dissociation scheme is proposed to explain the enhancement of the escaping rate by the presence of Xe(1). There are two branches for the CO escaping pathway. The dominant part of the dissociated CO escapes to the solvent through the Xe(1) trapping site under the Xe-free condition, and there are at least three intermediate states along this pathway. When a Xe atom blocks the Xe(1) site, the CO escapes through another route.

摘要

基于氙(Xe)对配体逸出速率的影响,采用瞬态光栅(TG)技术研究了在生理温度下,一氧化碳(CO)从肌红蛋白(Mb)血红素中的铁原子逸出到溶液中的对接位点。TG方法可直接测量分子体积的变化。随着Xe压力的增加,表观CO逸出速率和体积收缩也增加。速率的压力依赖性与Xe(1)位点处Xe原子的数量的压力依赖性一致。该结果清楚地表明,在室温下,CO在无Xe溶液中逸出到溶剂之前被困在Xe(1)位点。结果表明,通过光激发Xe捕获的MbCO,只有CO而不是被困的Xe被释放。提出了一个解离方案来解释Xe(1)的存在对逸出速率的增强作用。CO逸出途径有两个分支。在无Xe条件下,解离的CO的主要部分通过Xe(1)捕获位点逸出到溶剂中,沿此途径至少有三个中间状态。当一个Xe原子阻断Xe(1)位点时,CO通过另一条途径逸出。

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