含铁蛋白介导的铁转运分子机制

铁是生命体必需的微量元素,因为它是一些重要功能酶的协同因子。这些功能酶有着广泛的功能,从呼吸作用到核酸的复制。但是,当铁含量多于细胞稳态的时候,它将产生对机体有毒的羟基。生物体已经发展了自身的调控机制,包括铁的摄取,存储和输出来控制细胞内的铁处于平衡态。二价阳离子转运蛋白,铁输出蛋白和hephaestin参与小肠吸收,转铁蛋白和转铁蛋白受体参与铁的摄取和转运,铁蛋白可以存储铁,铁调控蛋白的功能是调节铁代谢。这篇文章综述着重阐述了含铁蛋白介导的铁传递机制。     

A radioactive tracer and radiation study of the stability of ferric and ferrous ions and ascorbic acid

A preliminary liquid-liquid extraction study of ferric and ferrous ions has been undertaken using the radioactive tracer technique with⁵⁹Fe as an indicator of iron. Various solvents were studied and suitable media and solvents were selected for the separation of the two oxidation states of iron. Such separation was used to study the effect of ascorbic acid and other reducing agents on the reduction of ferric ions. The oxidation of ferrous ions to the ferric state under the effect of gamma radiation from⁶⁰Co has also been investigated in the absence and presence of ascorbic acid, using spectrophotometry. In addition, a calculation of the amount of iron oxidized by gamma radiation is given with a discussion of its mechanism and possible effects on the metabolism of iron in the human body.     

微量元素铜、铁、锰、锗与自由基

自由基所造成的脂质过氧化损伤与许多病理过程有关,但体内存在消除氧自由基的酶等抗自由基物质,微量元素是酶的结构成分和活性中心,铜、铁、锰、猪等微量元素对自由基的代谢产生影响。     

Hepcidin in iron metabolism

Hepcidin, which has been recently identified both by biochemical and genomic approaches, is a 25 amino acid polypeptide synthesized mainly by hepatocytes and secreted into the plasma. Besides its potential activity in antimicrobial defense, hepcidin plays a major role in iron metabolism. It controls two key steps of iron bioavailability, likely through a hormonal action: digestive iron absorption by enterocytes and iron recycling by macrophages. In humans, this could explain that low levels of hepcidin found during juvenile haemochromatosis and HFE-1 genetic haemochromatosis are associated with an iron overload phenotype. Conversely, an increase of hepcidin expression is suspected to play a major role in the development of anemia of chronic inflammatory diseases. However, the regulatory mechanisms of hepcidin expression are multiple, including iron-related parameters, anemia, hypoxia, inflammation and hepatocyte function. Therefore, many physiological and pathological situations may modulate hepcidin expression and subsequently iron metabolism. A better knowledge of the biological effects of hepcidin and of its expression regulatory mechanisms will clarify the place of hepcidin in the diagnosis and treatment of iron-related diseases.     

Proteomics of metal transport and metal-associated diseases

Proteomics technology has the potential to identify groups of proteins that have similar biological function. However, few attempts have been made to identify and characterize metal-binding proteins by using proteomics strategies. Many transition metals are essential to sustain life. Copper, iron, and zinc are the most abundant transition metals relevant to biological systems. In addition to their important biological functions, metals can also catalyze the formation of damaging free radical species. Hence, their intracellular transport is tightly regulated. Despite recent insights into the intracellular transport of copper and other metals, our overall understanding of intracellular metal metabolism remains incomplete and it is likely that many metal-binding proteins remain undiscovered. Furthermore, the protein targets for metals during metal-associated disease states or during exposure to toxic levels of environmental metals are yet to be unravelled. A proteomics strategy for the analysis of metal-transporting or metal-binding proteins has the potential to uncover how a large number of proteins function in normal or metal-associated diseased states. Here we discuss the principal aspects of metal metabolism, and the recent developments in the area of the proteomics of metal transport.     

ICG/Lecithin: A promising theranostic agent for simultaneous therapy and diagnosis of MRI and PAI

A chronic liver disease usually results in iron accumulation, and an excess of iron will further aggravate liver injury, forming a vicious circle. Likewise, it also plays a significant role in other organs when it comes to iron metabolism. A long time passes between the time it takes to break through to MRI-based iron diagnosis and its ability to distinguish the types of iron accumulation accurately and quickly. This work highlighted a new type of iron accumulation treatment solution integrated with diagnosis and treatment. A chelating method for ICG and Leci that can assist PAI and MRI to achieve better diagnostic and therapeutic effects. This work revealed biomaterial engineering techniques are being adapted to address clinical medical problems through cutting-edge research.     

糖尿病患者治疗前后血细胞内液和血浆锌、铜、铁、镁和铷含量的研究

采用原子吸收分光光度计对６４名糖尿病患者血细胞内液和血浆中锌、铜、铁、镁、铷含量进行了测定．结果发现糖尿病组血细胞内液锌含量显著低于正常对照组（Ｐ＜０．０１），血细胞内液铁含量亦显著低于正常对照组（Ｐ＜０．０１），血浆铜含量显著高于正常对照组（Ｐ＜０．０１）．提示糖尿病患者锌、铁、铜的代谢方面均存在一定缺陷，认为糖尿病患者补充锌、铁元素，可能对治病有益处．     

Computational approach to the blood–aluminum problem?

Aluminum has no known function in biota and, when biologically available, is inimical to life. A key to understanding its potential toxicity in humans is its transport in blood. A consensus of opinion has identified the binding of aluminum by the iron‐transport protein transferrin as the preeminent factor in the transport of aluminum in blood, although this idea has emanated from in vitro analysis of isolated blood and has never been tested in vivo. We have highlighted what we believe to be inadequacies of our present understanding of aluminum transport in blood, and we have proposed the application of computational methods to test rigorously what we have coined “the blood‐aluminum problem.” © 2006 Wiley Periodicals, Inc. Int J Quantum Chem, 2007     

Nutritional iron supplementation studies based on enriched (57) Fe, added to milk in rats, and isotope pattern deconvolution-ICP-MS analysis

Enriched stable iron isotopes in combination with isotope pattern deconvolution and ICP-MS have been used to study the absorption and bioavailability of iron from supplemented formula milk administrated to lactating rats. The use of two enriched stable isotope tracers, one as the metabolic tracer (here (57) Fe) and the other ((54) Fe) as quantitation tracer, is shown to provide quantitative data about endogenous and exogenous (supplemented) total Fe distribution in rat feces, urine, red blood cells (RBCs), serum, liver, and kidney. The proposed analytical methodology was validated using reference materials (serum, urine, and liver) spiked with both (54) Fe and (57) Fe. Quantitative information about iron absorption/bioavailability and/or metabolism can be obtained from the amounts of endogenous and exogenous iron found in the tissues and fluids analyzed, and about its kinetic after 2 weeks of iron supplementation. The obtained results are discussed in terms of iron exchanged and its half-life in lactating rats and the observed iron levels in serum, RBCs, liver, and kidney comparing nonsupplemented rats and maternal feed rats.     

Understanding the structure/activity relationships of the iron regulatory peptide hepcidin

The peptide hormone hepcidin is a key homeostatic regulator of iron metabolism and involved in pathological regulation of iron in response to infection, inflammation, hypoxia, and anemia. It acts by binding to the iron exporter ferroportin, causing it to be internalized and degraded; however, little is known about the structure/activity relationships of the interaction of hepcidin with ferroportin. We show that there are key residues in the N-terminal region of hepcidin that influence its interaction with ferroportin, and we explore the structure/function relationships at these positions. A series of hepcidin mutants in which disulfide bonds were replaced with diselenide bonds showed no change in activity compared to native hepcidin. These results identify important constraints for the development of hepcidin congeners for the treatment of hereditary iron overload.     

微量元素硒与生物体健康

从硒在生物体内的分布、存在形态及代谢,硒的生物学功能,硒缺乏及硒中毒,生物体日需要量等方面阐述了硒与生物体健康的关系。     

The Bioavailability and Biological Activities of Phytosterols as Modulators of Cholesterol Metabolism

Phytosterols are natural sterols widely found in plants that have a variety of physiological functions, and their role in reducing cholesterol absorption has garnered much attention. Although the bioavailability of phytosterols is only 0.5–2%, they can still promote cholesterol balance in the body. A mechanism of phytosterols for lowering cholesterol has now been proposed. They not only reduce the uptake of cholesterol in the intestinal lumen and affect its transport, but also regulate the metabolism of cholesterol in the liver. In addition, phytosterols can significantly reduce the plasma concentration of total cholesterol, triglycerides, and low-density lipoprotein cholesterol (LDL-C), with a dose-response relationship. Ingestion of 3 g of phytosterols per day can reach the platform period, and this dose can reduce LDL-C by about 10.7%. On the other hand, phytosterols can also activate the liver X receptor α-CPY7A1 mediated bile acids excretion pathway and accelerate the transformation and metabolism of cholesterol. This article reviews the research progress of phytosterols as a molecular regulator of cholesterol and the mechanism of action for this pharmacological effect.     

Current Use of Fenton Reaction in Drugs and Food

Iron is the most abundant mineral in the human body and plays essential roles in sustaining life, such as the transport of oxygen to systemic organs. The Fenton reaction is the reaction between iron and hydrogen peroxide, generating hydroxyl radical, which is highly reactive and highly toxic to living cells. “Ferroptosis”, a programmed cell death in which the Fenton reaction is closely involved, has recently received much attention. Furthermore, various applications of the Fenton reaction have been reported in the medical and nutritional fields, such as cancer treatment or sterilization. Here, this review summarizes the recent growing interest in the usefulness of iron and its biological relevance through basic and practical information of the Fenton reaction and recent reports.     

Magnetic, electronic, and structural characterization of nonstoichiometric iron oxides at the nanoscale

We have investigated the structural, magnetic, and electronic properties of nonstoichiometric iron oxide nanocrystals prepared by decomposition of iron(II) and iron(0) precursors in the presence of organic solvents and capping groups. The highly uniform, crystalline, and monodisperse nanocrystals that were produced enabled a full structural and compositional survey by electron microscopy and X-ray diffraction. The complex and metastable behavior of nonstoichiometric iron oxide (wüstite) at the nanoscale was studied by a combination of Mossbauer spectroscopy and magnetic characterization. Deposition from hydrocarbon solvents with subsequent self-assembly of iron oxide nanocrystals into superlattices allowed the preparation of continuous thin films suitable for electronic transport measurements.     

Siderophores and Iron‐Transport in Microorganisms

Iron is an essential element in many biological systems, and in spite of its abundance (5% of the earth crust), its availability is dramatically limited by the very high insolubility of iron(III) at physiological pHs where the concentration of free iron(III) is less than 10^?17 M, a value which is much too low to allow any possible growth to aerobic microorganisms. Iron metabolization by the microorganisms necessitates generally the biosynthesis of low molecular weight compounds (300 to 2000 Da) called siderophores. These molecules which are generally excreted into the culture medium, chelate very strongly iron(III), solubilize it and transport it into the cells using an ATP‐dependent high affinity transport system. For nearly fourty years, the structural studies on siderophores have shown a great diversity of structures for these iron‐chelating molecules synthesized by microorganisms. These structures are characterized by the presence of one, two and in most cases, three bidentate chelating groups, generally oxygenated, necessary for the formation of very stable hexacoordinated octahedric complexes between the siderophores and iron(III). These groups are generally either catecholates, or hydroxamates or hydroxyacids, but can be any other bidentate groups In what follows several typical examples of siderophores belonging to each of these categories are given. It is clear that considering the very high number of siderophores having so many different structures so far isolated and characterized (more than 200), we have restricted this report to the most representative structures of each category, with a special emphasis to pyoverdins, the fluorescent peptidic siderophores of the fluorescent pseudomonads. Similarly the siderophore‐mediated iron‐transport mechanisms of Gram‐negative bacteria described therafter will report mainly on those of Escherichia coli with a special emphasis to Pseudomonas when information is available. The pyoverdin‐mediated iron‐transport in fluorescent pseudomonads implies biochemical mechanisms which involve signal and energy exchanges between the two membranes across the periplasmic space. The energy transduction mechanism in the case of the pyoverdin‐mediated active transport in P. aeruginosa has not been completely elucidated so far. Nevertheless from the data obtained for ferric enterobactin and ferrichrome in E. coli, it is plausible that a common mechanism of transport can take place for all the enterobacteria. The key element of this mechanism is protein TonB in E. coli, head of a series of TonB proteins having a very close structure and characterized in P. putida WCS358 and P. aeruginosa ATCC 156942. The striking similarities existing between the various iron‐transport steps in these different bacterial species is highly in favour of a common energy‐dependent siderophore‐mediated iron‐transport mechanism in microorganisms.     

Brain iron metabolism and its perturbation in neurological diseases

Abstract  

Enormous advances have been made in the last decade in understanding iron metabolism and iron homeostasis at both the cellular and the systemic level. This includes the identification of genes and proteins involved in iron transport, such as the ferric reductase DcytB, the proton-coupled ferrous (divalent) iron transporter DMT1, the iron exporter ferroportin and the membrane-bound ferroxidase hephaestin. The modulation of their translation by the iron regulatory protein (IRP) system has also been identified together with the impressive signalling cascades involved in regulating the chef d’orchestre of systemic iron homeostasis, hepcidin. However, exactly how the brain regulates fluxes and storage of iron between neurons, oligodendrocytes, astrocytes and microglial cells remains an enigma. In this review we discuss the possible mechanisms which may be involved in the transfer of iron across the blood–brain barrier, together with the possible role played by astrocytes. The consequences of iron deficiency and iron excess on brain function are described. Finally, various neurodegenerative diseases, where accumulation of iron may be important in the pathogenesis, are presented as well as the possible use of iron chelators to diminish disease progression.     

Lactoferrin: A Glycoprotein Involved in Immunomodulation,Anticancer, and Antimicrobial Processes

Lactoferrin is an iron binding glycoprotein with multiple roles in the body. Its participation in apoptotic processes in cancer cells, its ability to modulate various reactions of the immune system, and its activity against a broad spectrum of pathogenic microorganisms, including respiratory viruses, have made it a protein of broad interest in pharmaceutical and food research and industry. In this review, we have focused on describing the most important functions of lactoferrin and the possible mechanisms of action that lead to its function.     

铅污染与儿童健康

综述了环境铅污染与儿童健康的关系,包括：儿童铅中毒的原因,铅对儿童健康的危害和儿童铅污染的防治等,主要参考文献７篇。