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设计铁羰基配合物作为一氧化碳(CO)释放分子:在水性缓冲液中快速释放和传递 CO 至肌红蛋白,以及舒张小鼠主动脉。

Designed iron carbonyls as carbon monoxide (CO) releasing molecules: rapid CO release and delivery to myoglobin in aqueous buffer, and vasorelaxation of mouse aorta.

机构信息

Department of Chemistry and Biochemistry, University of California, Santa Cruz, California 95064, USA.

出版信息

Inorg Chem. 2011 Apr 4;50(7):3127-34. doi: 10.1021/ic2000848. Epub 2011 Mar 8.

Abstract

The physiological roles of CO in neurotransmission, vasorelaxation, and cytoprotective activities have raised interest in the design and syntheses of CO-releasing materials (CORMs) that could be employed to modulate such biological pathways. Three iron-based CORMs, namely, (PaPy(3))Fe(CO) (1), (SBPy(3))Fe(CO)(2) (2), and (Tpmen)Fe(CO)(2) (3), derived from designed polypyridyl ligands have been synthesized and characterized by spectroscopy and X-ray crystallography. In these three Fe(II) carbonyls, the CO is trans to a carboxamido-N (in 1), an imine-N (in 2), and a tertiary amine-N (in 3), respectively. This structural feature has been correlated to the strength of the Fe-CO bond. The CO-releasing properties of all three carbonyls have been studied in various solvents under different experimental conditions. Rapid release of CO is observed with 2 and 3 upon dissolution in both aqueous and nonaqueous media in the presence and absence of dioxygen. With 1, CO release is observed only under aerobic conditions, and the final product is an oxo-bridged diiron species while with 2 and 3, the solvent bound (L)Fe(CO) (where L = SBPy(3) or Tpmen) results upon loss of CO under both aerobic and anaerobic conditions. The apparent rates of CO loss by these CORMs are comparable to other CORMs such as [Ru(glycine)(CO)(3)Cl] reported recently. Facile delivery of CO to reduced myoglobin has been observed with both 2 and 3. In tissue bath experiments, 2 and 3 exhibit rapid vasorelaxation of mouse aorta muscle rings. Although the relaxation effect is not inhibited by the soluble guanylate cyclase inhibitor ODQ, significant inhibition is observed with the BK(Ca) channel blocker iberiotoxin.

摘要

CO 在神经递质传递、血管舒张和细胞保护活性中的生理作用引起了人们对设计和合成 CO 释放材料 (CORMs) 的兴趣,这些材料可以用于调节这些生物途径。三种基于铁的 CORMs,即 (PaPy(3))Fe(CO) (1)、(SBPy(3))Fe(CO)(2) (2) 和 (Tpmen)Fe(CO)(2) (3),源自设计的多吡啶配体,已通过光谱和 X 射线晶体学进行了合成和表征。在这三种 Fe(II)羰基化合物中,CO 分别处于羧酰胺-N(在 1 中)、亚胺-N(在 2 中)和叔胺-N(在 3 中)的反位。这种结构特征与 Fe-CO 键的强度有关。已经在不同的实验条件下在各种溶剂中研究了所有三种羰基化合物的 CO 释放性质。在有氧和无氧存在的情况下,2 和 3 在水相和非水相介质中的溶解都会迅速释放 CO。对于 1,只有在有氧条件下才能观察到 CO 的释放,最终产物是氧桥接的双核铁物种,而对于 2 和 3,在有氧和无氧条件下,CO 损失后都会得到溶剂结合的 (L)Fe(CO)(其中 L = SBPy(3) 或 Tpmen)。这些 CORMs 的 CO 损失的表观速率与最近报道的其他 CORMs(如 [Ru(glycine)(CO)(3)Cl])相当。已经观察到 2 和 3 可以将 CO 轻松递送到还原肌红蛋白。在组织浴实验中,2 和 3 可以迅速松弛小鼠主动脉肌肉环。尽管松弛作用不受可溶性鸟苷酸环化酶抑制剂 ODQ 的抑制,但 BK(Ca)通道阻滞剂 Iberiotoxin 观察到明显的抑制作用。

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