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培养的人类细胞中天然铀同位素分馏的证据。

Evidence of isotopic fractionation of natural uranium in cultured human cells.

作者信息

Paredes Eduardo, Avazeri Emilie, Malard Véronique, Vidaud Claude, Reiller Pascal E, Ortega Richard, Nonell Anthony, Isnard Hélène, Chartier Frédéric, Bresson Carole

机构信息

Den-Service d'Etudes Analytiques et de Réactivité des Surfaces (SEARS), Commissariat à l'Energie Atomique et aux Énergies Alternatives (CEA), Université Paris-Saclay, F-91191 Gif sur Yvette, France;

CEA, Direction de la Recherche Fondamentale (DRF), Biosciences and Biotechnologies Institute (BIAM), F-30207 Bagnols-sur-Cèze, France.

出版信息

Proc Natl Acad Sci U S A. 2016 Dec 6;113(49):14007-14012. doi: 10.1073/pnas.1610885113. Epub 2016 Nov 21.

Abstract

The study of the isotopic fractionation of endogen elements and toxic heavy metals in living organisms for biomedical applications, and for metabolic and toxicological studies, is a cutting-edge research topic. This paper shows that human neuroblastoma cells incorporated small amounts of uranium (U) after exposure to 10 µM natural U, with preferential uptake of the U isotope with regard to U. Efforts were made to develop and then validate a procedure for highly accurate n(U)/n(U) determinations in microsamples of cells. We found that intracellular U is enriched in U by 0.38 ± 0.13‰ (2σ, n = 7) relative to the exposure solutions. These in vitro experiments provide clues for the identification of biological processes responsible for uranium isotopic fractionation and link them to potential U incorporation pathways into neuronal cells. Suggested incorporation processes are a kinetically controlled process, such as facilitated transmembrane diffusion, and the uptake through a high-affinity uranium transport protein involving the modification of the uranyl (UO) coordination sphere. These findings open perspectives on the use of isotopic fractionation of metals in cellular models, offering a probe to track uptake/transport pathways and to help decipher associated cellular metabolic processes.

摘要

研究生物体内内源性元素和有毒重金属的同位素分馏,用于生物医学应用、代谢和毒理学研究,是一个前沿研究课题。本文表明,人类神经母细胞瘤细胞在暴露于10µM天然铀后会摄取少量铀(U),相对于铀,优先摄取铀同位素。我们努力开发并验证了一种用于在细胞微量样品中高精度测定n(U)/n(U)的方法。我们发现,细胞内的铀相对于暴露溶液中的铀,铀同位素富集了0.38±0.13‰(2σ,n = 7)。这些体外实验为识别导致铀同位素分馏的生物过程提供了线索,并将它们与铀进入神经元细胞的潜在途径联系起来。推测的摄取过程是一个动力学控制的过程,如促进跨膜扩散,以及通过涉及铀酰(UO)配位球修饰的高亲和力铀转运蛋白进行摄取。这些发现为在细胞模型中利用金属同位素分馏开辟了前景,提供了一个追踪摄取/运输途径并帮助解读相关细胞代谢过程的探针。

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Evidence of isotopic fractionation of natural uranium in cultured human cells.培养的人类细胞中天然铀同位素分馏的证据。
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