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使用精密切割组织切片和碳13核磁共振技术进行安全性研究时细胞代谢组学的方案与应用

Protocols and applications of cellular metabolomics in safety studies using precision-cut tissue slices and carbon 13 NMR.

作者信息

Baverel Gabriel, Renault Sophie, Faiz Hassan, El Hage Maha, Gauthier Catherine, Duplany Agnès, Ferrier Bernard, Martin Guy

机构信息

Metabolys Inc, Lyon Cedex, France.

出版信息

Methods Mol Biol. 2011;691:205-25. doi: 10.1007/978-1-60761-849-2_12.

Abstract

Numerous xenobiotics are toxic to human and animal cells by interacting with their metabolism, but the precise metabolic step affected and the biochemical mechanism behind such a toxicity often remain unknown. In an attempt to reduce the ignorance in this field, we have developed a new approach called cellular metabolomics. This approach, developed in vitro, provides a panoramic view not only of the pathways involved in the metabolism of physiologic substrates of any normal or pathologic human or animal cell but also of the beneficial and adverse effects of xenobiotics on these metabolic pathways. Unlike many cell lines, precision-cut tissue slices, for which there is a renewed interest, remain metabolically differentiated for at least 24-48 h and allow to study the effect of xenobiotics during short-term and long-term incubations. Cellular metabolomics (or cellular metabonomics), which combines enzymatic and carbon 13 NMR measurements with mathematical modeling of metabolic pathways, is illustrated in this brief chapter for studying the effect of insulin on glucose metabolism in rat liver precision-cut slices, and of valproate on glutamine metabolism in human renal cortical precision-cut slices. The use of very small amounts of test compounds allows to predict their toxic effect and eventually their beneficial effects very early in the research and development processes. Cellular metabolomics is complementary to other omics approaches, but, unlike them, provides functional and dynamic pieces of information by measuring enzymatic fluxes.

摘要

许多外源性物质通过与人体和动物细胞的新陈代谢相互作用而对其产生毒性,但受影响的具体代谢步骤以及这种毒性背后的生化机制往往仍不为人知。为了减少该领域的未知,我们开发了一种名为细胞代谢组学的新方法。这种在体外开发的方法不仅能全景展示任何正常或病理状态的人体或动物细胞生理底物代谢所涉及的途径,还能呈现外源性物质对这些代谢途径的有益和不利影响。与许多细胞系不同,重新受到关注的精密组织切片在至少24 - 48小时内仍保持代谢分化,并且能够研究外源性物质在短期和长期孵育过程中的作用。本章简要介绍了细胞代谢组学(或细胞代谢物组学),它将酶促测量和碳13核磁共振测量与代谢途径的数学建模相结合,用于研究胰岛素对大鼠肝脏精密组织切片中葡萄糖代谢的影响,以及丙戊酸对人肾皮质精密组织切片中谷氨酰胺代谢的影响。使用极少量的测试化合物能够在研发过程的早期就预测它们的毒性作用以及最终的有益作用。细胞代谢组学与其他组学方法互补,但与它们不同的是,它通过测量酶通量提供功能和动态信息。

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