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Iron and genome stability: An update

机译:铁和基因组稳定性:更新

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Iron is an essential micronutrient which is required in a relatively narrow range for maintaining metabolic homeostasis and genome stability. Iron participates in oxygen transport and mitochondrial respiration as well as in antioxidant and nucleic acid metabolism. Iron deficiency impairs these biological pathways, leading to oxidative stress and possibly carcinogenesis. Iron overload has been linked to genome instability as well as to cancer risk increase, as seen in hereditary hemochromatosis. Iron is an extremely reactive transition metal that can interact with hydrogen peroxide to generate hydroxyl radicals that form the 8-hydroxy-guanine adduct, cause point mutations as well as DNA single and double strand breaks. Iron overload also induces DNA hypermethylation and can reduce telomere length. The current Recommended Dietary Allowances (RDA) for iron, according with Institute of Medicine Dietary Reference Intake (DRI), is based in the concept of preventing anemia, and ranges from 7. mg/day to 18. mg/day depending on life stage and gender. Pregnant women need 27. mg/day. The maximum safety level for iron intake, the Upper Level (UL), is 40-45. mg/day, based on the prevention of gastrointestinal distress associated to high iron intakes. Preliminary evidence indicates that 20. mg/day iron, an intake slightly higher than the RDA, may reduce the risk of gastrointestinal cancer in the elderly as well as increasing genome stability in lymphocytes of children and adolescents. Current dietary recommendations do not consider the concept of genome stability which is of concern because damage to the genome has been linked to the origin and progression of many diseases and is the most fundamental pathology. Given the importance of iron for homeostasis and its potential influence over genome stability and cancer it is recommended to conduct further studies that conclusively define these relationships.
机译:铁是一种必需的微量营养素,在相对狭窄的范围内才能维持代谢稳态和基因组稳定性。铁参与氧气运输和线粒体呼吸以及抗氧化剂和核酸代谢。缺铁会破坏这些生物途径,导致氧化应激并可能致癌。如遗传性血色素沉着病中所见,铁超载与基因组不稳定以及癌症风险增加有关。铁是一种极活泼的过渡金属,可以与过氧化氢相互作用,生成羟基自由基,形成8-羟基鸟嘌呤加合物,引起点突变以及DNA单链和双链断裂。铁超负荷还会诱导DNA甲基化,并可以减少端粒的长度。根据医学研究所膳食参考摄入量(DRI)的规定,当前铁的推荐膳食津贴(RDA)基于预防贫血的概念,其范围从7毫克/天到18毫克/天不等。和性别。孕妇需要27.毫克/天。进铁的最大安全级别,上级(UL)为40-45。毫克/天,基于预防与高铁摄入有关的胃肠道不适。初步证据表明,每天摄入20毫克铁(略高于RDA)可以降低老年人胃肠道癌的风险,并可以提高儿童和青少年淋巴细胞的基因组稳定性。当前的饮食建议没有考虑基因组稳定性的概念,这是令人关注的,因为对基因组的损害已与许多疾病的起源和进展相关联,并且是最基本的病理学。鉴于铁对于体内平衡的重要性及其对基因组稳定性和癌症的潜在影响,建议进行进一步研究以明确定义这些关系。

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