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心血管系统中的铁、氧化应激与氧化还原信号传导

Iron, oxidative stress, and redox signaling in the cardiovascular system.

作者信息

Gudjoncik Aurélie, Guenancia Charles, Zeller Marianne, Cottin Yves, Vergely Catherine, Rochette Luc

机构信息

Laboratoire de Physiopathologie et Pharmacologie Cardio-métaboliques (LPPCM) Inserm UMR866, Facultés de Médecine et de Pharmacie, Université de Bourgogne, Dijon, France; Service de Cardiologie CHU Bocage, Dijon, France.

出版信息

Mol Nutr Food Res. 2014 Aug;58(8):1721-38. doi: 10.1002/mnfr.201400036. Epub 2014 May 30.

Abstract

The redox state of the cell is predominantly dependent on an iron redox couple and is maintained within strict physiological limits. Iron is an essential metal for hemoglobin synthesis in erythrocytes, for oxidation-reduction reactions, and for cellular proliferation. The maintenance of stable iron concentrations requires the coordinated regulation of iron transport into plasma from dietary sources in the duodenum, from recycled senescent red cells in macrophages, and from storage in hepatocytes. The absorption of dietary iron, which is present in heme or nonheme form, is carried out by mature villus enterocytes of the duodenum and proximal jejunum. Multiple physiological processes are involved in maintaining iron homeostasis. These include its storage at the intracellular and extracellular level. Control of iron balance in the whole organism requires communication between sites of uptake, utilization, and storage. Key protein transporters and the molecules that regulate their activities have been identified. In this field, ferritins and hepcidin are the major regulator proteins. A variety of transcription factors may be activated depending on the level of oxidative stress, leading to the expression of different genes. Major preclinical and clinical trials have shown advances in iron-chelation therapy for the treatment of iron-overload disease as well as cardiovascular and chronic inflammatory diseases.

摘要

细胞的氧化还原状态主要取决于铁的氧化还原对,并维持在严格的生理限度内。铁是红细胞中血红蛋白合成、氧化还原反应以及细胞增殖所必需的金属。维持稳定的铁浓度需要对从十二指肠的膳食来源、巨噬细胞中衰老红细胞的再循环以及肝细胞储存中转运到血浆中的铁进行协调调节。膳食中铁以血红素或非血红素形式存在,其吸收由十二指肠和空肠近端的成熟绒毛肠上皮细胞进行。维持铁稳态涉及多个生理过程。这些过程包括细胞内和细胞外水平的储存。整个机体中铁平衡的控制需要摄取、利用和储存部位之间的沟通。关键的蛋白质转运体及其调节活性的分子已被确定。在这个领域,铁蛋白和铁调素是主要的调节蛋白。根据氧化应激水平,多种转录因子可能被激活,从而导致不同基因的表达。主要的临床前和临床试验表明,铁螯合疗法在治疗铁过载疾病以及心血管和慢性炎症性疾病方面取得了进展。

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