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首页> 外文期刊>Environmental health perspectives. >Genetic Effects on Toxic and Essential Elements in Humans: Arsenic, Cadmium, Copper, Lead, Mercury, Selenium, and Zinc in Erythrocytes
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Genetic Effects on Toxic and Essential Elements in Humans: Arsenic, Cadmium, Copper, Lead, Mercury, Selenium, and Zinc in Erythrocytes

机译:对人类有毒和必需元素的遗传效应:红细胞中的砷,镉,铜,铅,汞,硒和锌

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Background and objectives An excess of toxic trace elements or a deficiency of essential ones has been implicated in many common diseases or public health problems, but little is known about causes of variation between people living within similar environments. We estimated effects of personal and socioeconomic characteristics on concentrations of arsenic (As), cadmium (Cd), copper (Cu), mercury (Hg), lead (Pb), selenium (Se), and zinc (Zn) in erythrocytes and tested for genetic effects using data from twin pairs. Methods We used blood samples from 2,926 adult twins living in Australia (1,925 women and 1,001 men; 30–92 years of age) and determined element concentrations in erythrocytes by inductively coupled plasma-mass spectrometry. We assessed associations between element concentrations and personal and socioeconomic characteristics, as well as the sources of genetic and environmental variation and covariation in element concentrations. We evaluated the chromosomal locations of genes affecting these characteristics by linkage analysis in 501 dizygotic twin pairs. Results Concentrations of Cu, Se, and Zn, and of As and Hg showed substantial correlations, concentrations of As and Hg due mainly to common genetic effects. Genetic linkage analysis showed significant linkage for Pb [chromosome 3, near SLC4A7 (solute carrier family 4, sodium bicarbonate cotransporter, member 7)] and suggestive linkage for Cd (chromosomes 2, 18, 20, and X), Hg (chromosome 5), Se (chromosomes 4 and 8), and Zn {chromosome 2, near SLC11A1 [solute carrier family 11 (proton-coupled divalent metal ion transporters)]}. Conclusions Although environmental exposure is a precondition for accumulation of toxic elements, individual characteristics and genetic factors are also important. Identification of the contributory genetic polymorphisms will improve our understanding of trace and toxic element uptake and distribution mechanisms.
机译:背景和目标许多常见疾病或公共卫生问题都涉及过量的有毒微量元素或必需元素的缺乏,但人们对生活在相似环境中的人之间变异的成因知之甚少。我们估算了个人和社会经济特征对红细胞中砷(As),镉(Cd),铜(Cu),汞(Hg),铅(Pb),硒(Se)和锌(Zn)浓度的影响,并进行了测试使用双胞胎对的数据进行遗传效应分析。方法我们使用了居住在澳大利亚的2,926名成年双胞胎(1,925名女性和1,001名男性; 30-92岁)的血液样本,并通过电感耦合等离子体质谱法测定了红细胞中的元素浓度。我们评估了元素浓度​​与个人和社会经济特征之间的关联,以及元素浓度的遗传和环境变异以及协变的来源。我们通过501双合双生子中的连锁分析评估了影响这些特征的基因的染色体位置。结果Cu,Se和Zn的浓度以及As和Hg的浓度显示出显着的相关性,As和Hg的浓度主要是由于常见的遗传效应。遗传连锁分析显示Pb [在SLC4A7附近的3号染色体(溶质载体家族4,碳酸氢钠共转运蛋白,成员7)的显着连锁]和Cd(2、18、20和X染色体),Hg(5号染色体)的显着连锁。 ,Se(染色体4和8)和Zn {染色体2,靠近SLC11A1 [溶质载体家族11(质子偶联的二价金属离子转运蛋白)]]。结论尽管环境暴露是积累有毒元素的前提,但是个人特征和遗传因素也很重要。有助于遗传多态性的鉴定将提高我们对痕量和有毒元素摄取和分布机制的了解。

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