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血红素及其降解产物在急性肺及炎症性疾病发病机制中的意义。

Significance of Heme and Heme Degradation in the Pathogenesis of Acute Lung and Inflammatory Disorders.

机构信息

Proterris, Inc., Boston, MA 02118, USA.

出版信息

Int J Mol Sci. 2021 May 24;22(11):5509. doi: 10.3390/ijms22115509.

Abstract

The heme molecule serves as an essential prosthetic group for oxygen transport and storage proteins, as well for cellular metabolic enzyme activities, including those involved in mitochondrial respiration, xenobiotic metabolism, and antioxidant responses. Dysfunction in both heme synthesis and degradation pathways can promote human disease. Heme is a pro-oxidant via iron catalysis that can induce cytotoxicity and injury to the vascular endothelium. Additionally, heme can modulate inflammatory and immune system functions. Thus, the synthesis, utilization and turnover of heme are by necessity tightly regulated. The microsomal heme oxygenase (HO) system degrades heme to carbon monoxide (CO), iron, and biliverdin-IXα, that latter which is converted to bilirubin-IXα by biliverdin reductase. Heme degradation by heme oxygenase-1 (HO-1) is linked to cytoprotection via heme removal, as well as by activity-dependent end-product generation (i.e., bile pigments and CO), and other potential mechanisms. Therapeutic strategies targeting the heme/HO-1 pathway, including therapeutic modulation of heme levels, elevation (or inhibition) of HO-1 protein and activity, and application of CO donor compounds or gas show potential in inflammatory conditions including sepsis and pulmonary diseases.

摘要

血红素分子作为氧运输和储存蛋白的必需辅基,以及细胞代谢酶活性的必需辅基,包括参与线粒体呼吸、外源化学物质代谢和抗氧化反应的酶活性。血红素合成和降解途径的功能障碍可促进人类疾病。血红素通过铁催化作为一种促氧化剂,可诱导细胞毒性和血管内皮损伤。此外,血红素还可以调节炎症和免疫系统功能。因此,血红素的合成、利用和周转必然受到严格调控。微粒体血红素加氧酶(HO)系统将血红素降解为一氧化碳(CO)、铁和胆绿素-IXα,后者由胆绿素还原酶转化为胆红素-IXα。血红素加氧酶-1(HO-1)通过血红素去除以及活性依赖性终产物生成(即胆汁色素和 CO)与细胞保护相关,以及其他潜在机制。针对血红素/HO-1 途径的治疗策略,包括血红素水平的治疗性调节、HO-1 蛋白和活性的升高(或抑制),以及 CO 供体化合物或气体的应用,在包括败血症和肺部疾病在内的炎症情况下具有潜在应用价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a02b/8197128/c9021e5334b3/ijms-22-05509-g001.jpg

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