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首页> 外文期刊>Molecular & cellular proteomics: MCP >Biomarker discovery by imaging mass spectrometry: transthyretin is a biomarker for gentamicin-induced nephrotoxicity in rat.
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Biomarker discovery by imaging mass spectrometry: transthyretin is a biomarker for gentamicin-induced nephrotoxicity in rat.

机译:通过成像质谱法发现生物标志物:运甲状腺素蛋白是庆大霉素诱导的大鼠肾毒性的生物标志物。

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摘要

Adverse drug effects are often associated with pathological changes in tissue. An accurate depiction of the undesired affected area, possibly supported by mechanistic data, is important to classify the effects with regard to relevance for human patients. MALDI imaging MS represents a new analytical tool to directly provide the spatial distribution and the relative abundance of proteins in tissue. Here we evaluate this technique to investigate potential toxicity biomarkers in kidneys of rats that were administered gentamicin, a well known nephrotoxicant. Differential analysis of the mass spectrum profiles revealed a spectral feature at 12,959 Da that strongly correlates with histopathology alterations of the kidney. We unambiguously identified this spectral feature as transthyretin (Ser(28)-Gln(146)) using an innovative combination of tissue microextraction and fractionation by reverse-phase liquid chromatography followed by a top-down tandem mass spectrometric approach. Our findings clearly demonstratethe emerging role of imaging MS in the discovery of toxicity biomarkers and in obtaining mechanistic insights concerning toxicity mechanisms.
机译:药物不良反应通常与组织的病理变化有关。准确描述不良影响区域(可能由机械数据支持)对于分类与人类患者相关性的影响非常重要。 MALDI成像MS代表了一种直接提供组织中蛋白质的空间分布和相对丰度的新分析工具。在这里,我们评估这项技术,以调查庆大霉素,一种众所周知的肾毒性药,在大鼠肾脏中的潜在毒性生物标志物。质谱图的差异分析显示,在12959 Da处的光谱特征与肾脏的组织病理学变化密切相关。我们使用组织微萃取和反相液相色谱分离,然后采用自顶向下的串联质谱方法的创新组合,明确地将此光谱特征鉴定为运甲状腺素蛋白(Ser(28)-Gln(146))。我们的发现清楚地证明了成像MS在毒性生物标志物的发现以及获得有关毒性机制的机械见解方面的新兴作用。

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