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首页> 外文期刊>Journal of the American Society for Mass Spectrometry >Micro-Heterogeneity of Human Saliva Peptide P-C Characterized by High-Resolution Top-Down Fourier-Transform Mass Spectrometry
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Micro-Heterogeneity of Human Saliva Peptide P-C Characterized by High-Resolution Top-Down Fourier-Transform Mass Spectrometry

机译:高分辨率自上而下的傅立叶变换质谱法表征人唾液肽P-C的微异质性

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摘要

Top-down proteomics characterizes protein primary structures with unprejudiced descriptions of expressed and processed gene products. Gene sequence polymorphisms, protein post-translational modifications, and gene sequence errors can all be identified using topdown proteomics. Saliva offers advantages for proteomic research because of availability and the noninvasiveness of collection and, for these reasons, is being used to search for disease biomarkers. The description of natural protein variants, and intra- and inter-individual polymorphisms, is necessary for a complete description of any proteome, and essential for the discovery of disease biomarkers. Here, we report a striking example of natural protein variants with the discovery by top-down proteomics of two new variants of Peptide P-C. Intact mass measurements, and collisionally activated-, infrared multiphoton-, and electron capturedissociation, were used for characterization of the form predicted from the gene sequence with an average mass 4371 Da, a form postulated to result from a single nucleotide polymorphism of mass 4372 Da, and another form of mass 4370 Da postulated to arise from a novel protein sequence polymorphism. While the biological significance of such subtle variations in protein structure remains unclear, their importance cannot be assigned without their characterization, as is reported here for one of the major salivary proteins.
机译:自上而下的蛋白质组学以不偏颇的表达和加工基因产物描述来表征蛋白质一级结构。基因序列多态性,蛋白质翻译后修饰和基因序列错误都可以使用自上而下的蛋白质组学进行鉴定。唾液为蛋白质组学研究提供了优势,因为其可用性和采集的无创性,由于这些原因,唾液被用于寻找疾病的生物标志物。天然蛋白变异体以及个体内部和个体间多态性的描述对于任何蛋白质组的完整描述都是必要的,并且对于发现疾病生物标记物至关重要。在这里,我们通过自上而下的蛋白质组学发现了肽P-C的两个新变体,报道了一个天然蛋白质变体的惊人例子。使用完整质量测量以及碰撞激活,红外多光子和电子捕获解离来表征从基因序列预测的平均质量为4371 Da的形式,该形式被推测为质量为4372 Da的单核苷酸多态性导致的形式,以及另一种形式的质量4370 Da可能是由一种新的蛋白质序列多态性引起的。尽管蛋白质结构中这种细微变化的生物学意义尚不清楚,但如果不对其进行表征,就无法确定其重要性,如本文中对一种主要唾液蛋白的报道。

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