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Characterization of the Human Cerebrospinal Fluid Phosphoproteome by Titanium Dioxide Affinity Chromatography and Mass Spectrometry

机译:二氧化钛亲和色谱和质谱法表征人脑脊液磷酸化蛋白质组

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摘要

Biomarkers in the cerebrospinal fluid (CSF) may be important for the diagnosis of chronic degenerative disorders in the central nervous system including dementia. Existing CSF biomarkers for dementia, however, are relatively nonspecific. More specific markers may be found by targeting investigations based on knowledge of the molecular pathology of the disease in question. In Alzheimer's disease, hyperphosphorylation of the tau protein is a characteristic feature and thus a comprehensive characterization of the phosphoproteome of the CSF may be pursued to obtain a complete picture of phosphorylation aberrations in health and disease. Toward that goal we here describe a method for a comprehensive isolation and identification of phosphorylated tryptic peptides derived from CSF proteins using a simple sample preparation step and titanium dioxide-affinity chromatography followed by MALDI-TOF or LC-MS/MS linear ion-trap-FT mass spectrometry. Whereas not all previously reported phosphoproteins were found in normal CSF, we detected 56 putative novel phosphorylation sites in 38 proteins in addition to known sites. The approach seems to be a promising foundation for the discovery of new biomarkers embedded in the CSF phosphoproteome.
机译:脑脊液(CSF)中的生物标志物对于诊断包括痴呆症在内的中枢神经系统的慢性退行性疾病可能很重要。然而,现有的脑脊液痴呆生物标志物相对而言是非特异性的。通过基于有关疾病的分子病理学知识进行有针对性的研究,可以找到更具体的标记。在阿尔茨海默氏病中,tau蛋白的过度磷酸化是一个特征性特征,因此可以对CSF的磷酸化蛋白质组进行全面表征,以获取健康和疾病中磷酸化异常的完整图像。为实现该目标,我们在此描述了一种方法,该方法使用简单的样品制备步骤和二氧化钛亲和色谱,然后进行MALDI-TOF或LC-MS / MS线性离子阱-捕获,全面分离和鉴定源自CSF蛋白的磷酸化胰蛋白酶肽FT质谱。尽管并非所有先前报道的磷蛋白都在正常CSF中发现,但除了已知位点,我们还在38种蛋白中检测到56个推定的新型磷酸化位点。该方法似乎是发现嵌入CSF磷酸蛋白质组中的新生物标记物的有前途的基础。

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