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Ironing out the Details: Untangling Dietary Iron and Genetic Background in Diabetes

机译:消除细节:弄清糖尿病患者的膳食铁和遗传背景

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摘要

The search for genetic risk factors in type-II diabetes has been hindered by a failure to consider dietary variables. Dietary nutrients impact metabolic disease risk and severity and are essential to maintaining metabolic health. Genetic variation between individuals confers differences in metabolism, which directly impacts response to diet. Most studies attempting to identify genetic risk factors in disease fail to incorporate dietary components, and thus are ill-equipped to capture the breadth of the genome’s impact on metabolism. Understanding how genetic background interacts with nutrients holds the key to predicting and preventing metabolic diseases through the implementation of personalized nutrition. Dysregulation of iron homeostasis is associated with type-II diabetes, but the link between dietary iron and metabolic dysfunction is poorly defined. High iron burden in adipose tissue induces insulin resistance, but the mechanisms underlying adipose iron accumulation remain unknown. Hepcidin controls dietary iron absorption and distribution in metabolic tissues, but it is unknown whether genetic variation influencing hepcidin expression modifies susceptibility to dietary iron-induced insulin resistance. This review highlights discoveries concerning the axis of iron homeostasis and adipose function and suggests that genetic variation underlying dietary iron metabolism is an understudied component of metabolic disease.
机译:未能考虑饮食因素阻碍了II型糖尿病遗传危险因素的研究。膳食营养素影响代谢疾病的风险和严重性,对于维持代谢健康至关重要。个体之间的遗传变异会带来新陈代谢的差异,从而直接影响对饮食的反应。大多数试图确定疾病的遗传危险因素的研究都没有纳入饮食成分,因此缺乏足够的能力来捕捉基因组对代谢的影响的广度。了解遗传背景如何与营养物质相互作用,是通过实施个性化营养预测和预防代谢疾病的关键。铁稳态的失调与II型糖尿病有关,但饮食铁与代谢功能障碍之间的联系尚不清楚。脂肪组织中高铁负荷可诱导胰岛素抵抗,但脂肪铁蓄积的机制尚不清楚。铁调素控制饮食中铁在代谢组织中的吸收和分布,但是尚不清楚影响铁调素表达的遗传变异是否会改变对铁引起的胰岛素抵抗的敏感性。这篇综述重点介绍了有关铁稳态和脂肪功能轴的发现,并提出了饮食中铁代谢的遗传变异是代谢疾病的一个未被充分研究的组成部分。

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