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使用胞质分裂阻滞微核细胞分析法测定,作为硒代蛋氨酸的硒对人淋巴细胞基因组稳定性和细胞毒性的影响。

The effect of selenium, as selenomethionine, on genome stability and cytotoxicity in human lymphocytes measured using the cytokinesis-block micronucleus cytome assay.

作者信息

Wu Jing, Lyons Graham H, Graham Robin D, Fenech Michael F

机构信息

Nutrigenomics Laboratory, CSIRO Human Nutrition, SA, Australia.

出版信息

Mutagenesis. 2009 May;24(3):225-32. doi: 10.1093/mutage/gen074. Epub 2009 Jan 20.

DOI:10.1093/mutage/gen074
PMID:19155331
Abstract

A supranutritional intake of selenium (Se) may be required for cancer prevention, but an excessively high dose could be toxic. Therefore, the effect on genome stability of seleno-L-methionine (Se-met), the most important dietary form of Se, was measured to determine its bioefficacy and safety limit. Peripheral blood lymphocytes were isolated from six volunteers and cultured with medium supplemented with Se-met in a series of Se concentrations (3, 31, 125, 430, 1880 and 3850 microg Se/litre) while keeping the total methionine (i.e. Se-met + L-methionine) concentration constant at 50 microM. Baseline genome stability of lymphocytes and the extent of DNA damage induced by 1.5-Gy gamma-ray were investigated using the cytokinesis-block micronucleus cytome assay after 9 days of culture in 96-microwell plates. High Se concentrations (>or=1880 microg Se/litre) caused strong inhibition of cell division and increased cell death (P < 0.0001). Baseline frequency of nucleoplasmic bridges and nuclear buds, however, declined significantly (P trend < 0.05) as Se concentration increased from 3 to 430 microg Se/litre. Se concentration (<or=430 microg Se/litre) had no significant effect on baseline frequency of micronuclei and had no protective effect against genome damage induced by exposure to 1.5-Gy gamma-ray irradiation. In conclusion, Se, as Se-met, may improve genome stability at concentrations up to 430 microg Se/litre, but higher doses may be cytotoxic. Therefore, a cautious approach to supplementation with Se-met is required to ensure that optimal genome health is achieved without cytotoxic effects.

摘要

预防癌症可能需要超营养剂量的硒(Se),但过高剂量可能有毒。因此,对硒的最重要膳食形式硒代-L-蛋氨酸(Se-met)对基因组稳定性的影响进行了测定,以确定其生物功效和安全限度。从六名志愿者中分离出外周血淋巴细胞,并在一系列硒浓度(3、31、125、430、1880和3850微克硒/升)下,用添加了Se-met的培养基进行培养,同时将总蛋氨酸(即Se-met + L-蛋氨酸)浓度保持在50微摩尔不变。在96孔板中培养9天后,使用胞质分裂阻滞微核细胞分析法研究淋巴细胞的基线基因组稳定性以及1.5 Gy γ射线诱导的DNA损伤程度。高硒浓度(≥1880微克硒/升)导致细胞分裂强烈抑制并增加细胞死亡(P < 0.0001)。然而,随着硒浓度从3微克硒/升增加到430微克硒/升,核质桥和核芽的基线频率显著下降(P趋势< 0.05)。硒浓度(≤430微克硒/升)对微核的基线频率没有显著影响,并且对暴露于1.5 Gy γ射线照射诱导的基因组损伤没有保护作用。总之,作为Se-met的硒在浓度高达430微克硒/升时可能会改善基因组稳定性,但更高剂量可能具有细胞毒性。因此,需要谨慎补充Se-met,以确保在不产生细胞毒性作用的情况下实现最佳的基因组健康。

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