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营养遗传学、营养基因组学与硒

Nutrigenetics, nutrigenomics, and selenium.

作者信息

Ferguson Lynnette R, Karunasinghe Nishi

机构信息

Discipline of Nutrition, Faculty of Medical and Health Sciences, The University of Auckland Auckland, New Zealand.

出版信息

Front Genet. 2011 Apr 25;2:15. doi: 10.3389/fgene.2011.00015. eCollection 2011.

DOI:10.3389/fgene.2011.00015
PMID:22303312
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3268570/
Abstract

Selenium (Se) is an important micronutrient that, as a component of selenoproteins, influences oxidative and inflammatory processes. Its' levels vary considerably, with different ethnic and geographic population groups showing varied conditions, ranging from frank Se deficiencies to toxic effects. An optimum Se level is essential for the maintenance of homeostasis, and this optimum may vary according to life stage, general state of health, and genotype. Nutrigenetic studies of different Se levels, in the presence of genetic variants in selenoproteins, suggest that an effective dietary Se intake for one individual may be very different from that for others. However, we are just starting to learn the significance of various genes in selenoprotein pathways, functional variants in these, and how to combine such data from genes into pathways, alongside dietary intake or serum levels of Se. Advances in systems biology, genetics, and genomics technologies, including genetic/genomic, epigenetic/epigenomic, transcriptomic, proteomic, and metabolomic information, start to make it feasible to assess a comprehensive spectrum of the biological activity of Se. Such nutrigenomic approaches may prove very sensitive biomarkers of optimal Se status at the individual or population level. The premature cessation of a major human Se intervention trial has led to considerable controversy as to the value of Se supplementation at the population level. New websites provide convenient links to current information on methodologies available for nutrigenetics and nutrigenomics. These new technologies will increasingly become an essential tool in optimizing the level of Se and other micronutrients for optimal health, in individuals and in population groups. However, definitive proof of such effects will require very large collaborative studies, international agreement on study design, and innovative approaches to data analysis.

摘要

硒(Se)是一种重要的微量营养素,作为硒蛋白的组成部分,它会影响氧化和炎症过程。其水平差异很大,不同种族和地理人群呈现出不同状况,从明显的硒缺乏到中毒效应不等。最佳硒水平对于维持体内平衡至关重要,而这个最佳水平可能因生命阶段、总体健康状况和基因型的不同而有所差异。对不同硒水平以及硒蛋白存在基因变异情况下的营养遗传学研究表明,一个人有效的膳食硒摄入量可能与其他人有很大不同。然而,我们才刚刚开始了解硒蛋白途径中各种基因的意义、这些基因中的功能变异,以及如何将来自基因的数据与膳食摄入量或血清硒水平一起整合到途径中。系统生物学、遗传学和基因组学技术的进步,包括遗传/基因组、表观遗传/表观基因组、转录组、蛋白质组和代谢组信息,开始使得评估硒的全面生物活性成为可能。这种营养基因组学方法可能会在个体或群体层面上成为最佳硒状态非常敏感的生物标志物。一项主要的人类硒干预试验提前终止,引发了关于人群层面补充硒的价值的相当大的争议。新网站提供了便捷链接,可获取有关营养遗传学和营养基因组学可用方法的当前信息。这些新技术将越来越成为优化个体和人群组中硒及其他微量营养素水平以实现最佳健康的重要工具。然而,要明确证明这种效果需要非常大规模的合作研究、关于研究设计的国际共识以及创新的数据分析方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1efd/3268570/b58ebfa4a69d/fgene-02-00015-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1efd/3268570/b58ebfa4a69d/fgene-02-00015-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1efd/3268570/b58ebfa4a69d/fgene-02-00015-g001.jpg

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