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血红素加氧酶-1/一氧化碳:从基础科学到治疗应用

Heme oxygenase-1/carbon monoxide: from basic science to therapeutic applications.

作者信息

Ryter Stefan W, Alam Jawed, Choi Augustine M K

机构信息

Department of Medicine, Division of Pulmonary, Allergy, and Critical Care Medicine, The University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.

出版信息

Physiol Rev. 2006 Apr;86(2):583-650. doi: 10.1152/physrev.00011.2005.

Abstract

The heme oxygenases, which consist of constitutive and inducible isozymes (HO-1, HO-2), catalyze the rate-limiting step in the metabolic conversion of heme to the bile pigments (i.e., biliverdin and bilirubin) and thus constitute a major intracellular source of iron and carbon monoxide (CO). In recent years, endogenously produced CO has been shown to possess intriguing signaling properties affecting numerous critical cellular functions including but not limited to inflammation, cellular proliferation, and apoptotic cell death. The era of gaseous molecules in biomedical research and human diseases initiated with the discovery that the endothelial cell-derived relaxing factor was identical to the gaseous molecule nitric oxide (NO). The discovery that endogenously produced gaseous molecules such as NO and now CO can impart potent physiological and biological effector functions truly represented a paradigm shift and unraveled new avenues of intense investigations. This review covers the molecular and biochemical characterization of HOs, with a discussion on the mechanisms of signal transduction and gene regulation that mediate the induction of HO-1 by environmental stress. Furthermore, the current understanding of the functional significance of HO shall be discussed from the perspective of each of the metabolic by-products, with a special emphasis on CO. Finally, this presentation aspires to lay a foundation for potential future clinical applications of these systems.

摘要

血红素加氧酶由组成型和诱导型同工酶(HO-1、HO-2)构成,催化血红素代谢转化为胆汁色素(即胆绿素和胆红素)的限速步骤,因此是铁和一氧化碳(CO)的主要细胞内来源。近年来,内源性产生的CO已被证明具有影响众多关键细胞功能的有趣信号特性,包括但不限于炎症、细胞增殖和凋亡性细胞死亡。生物医学研究和人类疾病中气态分子的时代始于发现内皮细胞衍生的舒张因子与气态分子一氧化氮(NO)相同。内源性产生的气态分子如NO以及现在的CO可发挥强大的生理和生物学效应功能这一发现,确实代表了一种范式转变,并开辟了深入研究的新途径。本综述涵盖了血红素加氧酶的分子和生化特性,讨论了介导环境应激诱导HO-1的信号转导和基因调控机制。此外,将从每种代谢副产物的角度讨论目前对血红素加氧酶功能意义的理解,特别强调CO。最后,本报告旨在为这些系统未来潜在的临床应用奠定基础。

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