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顺反-[Re(II)(CO)2Br2L2]n 配合物的 CO 释放性能和细胞保护作用。

CO releasing properties and cytoprotective effect of cis-trans-[Re(II)(CO)2Br2L2]n complexes.

机构信息

Institute of Inorganic Chemistry, University of Zürich, Winterthurerstrasse 190, CH-8057 Zürich, Switzerland.

出版信息

Inorg Chem. 2010 Aug 16;49(16):7313-22. doi: 10.1021/ic100458j.

Abstract

The carbon monoxide (CO) releasing properties of a series of rhenium(II)-based complexes of general formula cis-trans-Re(II)(CO)(2)Br(2)L(2) and cis-trans-[Re(II)(CO)(2)Br(2)N[intersection]N] (where L = monodentate and N[intersection]N = bidentate ligand) are reported. Complexes evaluated in this study were obtained from direct ligand substitution reactions of the cis-Re(II)(CO)(2)Br(4) synthon (2) recently described. (1) All molecules have been fully characterized. The solid-state structures of the cis-trans-[Re(II)(CO)(2)Br(2)L(2)] (with L = N-methylimidazole (3), benzimidazole (4) and 4-picoline (5)) and the cis-trans-[Re(II)(CO)(2)Br(2)N[intersection]N] (with N[intersection]N = 4,4'-dimethyl-2,2'-bipyridine (8) and 2,2'-dipyridylamine (11)) adducts are presented. The release of CO from the cis-trans-Re(II)(CO)(2)Br(2)L(2) complexes was assessed spectrophotometrically by measuring the conversion of deoxymyoglobin (Mb) to carbonmonoxy myoglobin (MbCO). Only compounds bearing monodentate ligands were found to liberate CO. The rate of CO release was found to be pH dependent with half-lives (t(1/2)) under physiological conditions (25 degrees C, 0.1 M phosphate buffer, and pH 7.4) varying from ca. 6-43 min. At lower pH values, the time required to fully saturate Mb with CO liberated from the metal complexes gradually decreased. Complex 2 and the cis-trans-[Re(II)(CO)(2)Br(2)(Im)(2)] adduct (with Im = imidazole (6)) show a protective action against "ischemia-reperfusion" stress of neonatal rat ventricular cardiomyocytes in culture.

摘要

报告了一系列基于铼(II)的配合物的一氧化碳(CO)释放性质,这些配合物的通式为顺式-反式-[Re(II)(CO)(2)Br(2)L(2)](n)和顺式-反式-[Re(II)(CO)(2)Br(2)N [intersection] N](其中 L = 单齿配体和 N [intersection] N = 双齿配体)。在这项研究中评估的配合物是通过最近描述的顺式-[Re(II)(CO)(2)Br(4)](2-)前体(2)的直接配体取代反应获得的。(1)所有分子都经过了充分的表征。顺式-反式-[Re(II)(CO)(2)Br(2)L(2)](其中 L = N-甲基咪唑(3)、苯并咪唑(4)和 4-吡啶(5))和顺式-反式-[Re(II)(CO)(2)Br(2)N [intersection] N](其中 N [intersection] N = 4,4'-二甲基-2,2'-联吡啶(8)和 2,2'-联吡啶胺(11))加合物的固态结构被呈现。通过测量脱氧肌红蛋白(Mb)向碳氧肌红蛋白(MbCO)的转化,分光光度法评估了顺式-反式-[Re(II)(CO)(2)Br(2)L(2)](n)配合物释放 CO 的情况。仅发现带有单齿配体的化合物能够释放 CO。发现 CO 释放的速度随 pH 值而变化,在生理条件下(25°C、0.1 M 磷酸盐缓冲液、pH 值 7.4)半衰期(t(1/2))约为 6-43 分钟。在较低的 pH 值下,从金属配合物中释放的 CO 完全饱和 Mb 所需的时间逐渐减少。配合物 2 和顺式-反式-[Re(II)(CO)(2)Br(2)(Im)(2)]加合物(其中 Im = 咪唑(6))显示出对培养的新生大鼠心室心肌细胞“缺血再灌注”应激的保护作用。

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