首页> 外文期刊>Journal of chromatography, B. Analytical technologies in the biomedical and life sciences >Quantitative profiling of bile acids in biofluids and tissues based on accurate mass high resolution LC-FT-MS: compound class targeting in a metabolomics workflow.
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Quantitative profiling of bile acids in biofluids and tissues based on accurate mass high resolution LC-FT-MS: compound class targeting in a metabolomics workflow.

机译:基于精确的高质量高分辨率LC-FT-MS:在代谢组学工作流程中定位化合物类别的生物流体和组织中胆汁酸的定量谱分析。

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We report a sensitive, generic method for quantitative profiling of bile acids and other endogenous metabolites in small quantities of various biological fluids and tissues. The method is based on a straightforward sample preparation, separation by reversed-phase high performance liquid-chromatography mass spectrometry (HPLC-MS) and electrospray ionisation in the negative ionisation mode (ESI-). Detection is performed in full scan using the linear ion trap Fourier transform mass spectrometer (LTQ-FTMS) generating data for many (endogenous) metabolites, not only bile acids. A validation of the method in urine, plasma and liver was performed for 17 bile acids including their taurine, sulfate and glycine conjugates. The method is linear in the 0.01-1 mu M range. The accuracy in human plasma ranges from 74 to 113%, in human urine 77 to 104% and in mouse liver 79 to 140%. The precision ranges from 2 to 20% for pooled samples even in studies with large number of samples (n > 250). The method was successfully applied to a multi-compartmental APOE*3-Leiden mouse study, the main goal of which was to analyze the effect of increasing dietary cholesterol concentrations on hepatic cholesterol homeostasis and bile acid synthesis. Serum and liver samples from different treatment groups were profiled with the new method. Statistically significant differences between the diet groups were observed regarding total as well as individual bile acid concentrations. (C) 2008 Elsevier B.V. All rights reserved.
机译:我们报告了一种敏感的通用方法,用于定量分析各种生物流体和组织中的少量胆汁酸和其他内源性代谢物。该方法基于简单的样品制备,通过反相高效液相色谱质谱(HPLC-MS)进行分离以及以负离子化模式(ESI-)进行电喷雾离子化。使用线性离子阱傅里叶变换质谱仪(LTQ-FTMS)在全扫描中进行检测,不仅生成胆汁酸,还生成许多(内源)代谢物的数据。对尿液,血浆和肝脏中17种胆汁酸(包括牛磺酸,硫酸盐和甘氨酸共轭物)的方法进行了验证。该方法在0.01-1μM范围内是线性的。人血浆中的准确度为74%至113%,人尿中的准确度为77%至104%,小鼠肝中的准确度为79%至140%。对于合并样本,即使在具有大量样本(n> 250)的研究中,其精度范围也从2%到20%。该方法已成功应用于多室APOE * 3-Leiden小鼠研究,其主要目标是分析饮食中胆固醇浓度的升高对肝胆固醇稳态和胆汁酸合成的影响。用新方法分析了不同治疗组的血清和肝样品。饮食组之间在总胆汁酸浓度和个别胆汁酸浓度方面均存在统计学差异。 (C)2008 Elsevier B.V.保留所有权利。

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