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Assessing the Extent of Bone Degradation Using Glutamine Deamidation in Collagen

机译:使用谷氨酰胺在胶原蛋白中的脱酰胺作用评估骨降解的程度

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摘要

Collagen peptides are analyzed using a low-cost, high-throughput method for assessing deamidation using matrix-assisted laser desorption/ionization mass spectrometry (MALDI-MS). For each chosen peptide, the theoretical distribution is calculated and the measured distribution for each sample compared with this to determine the extent of glutamine deamidation. The deamidation of glutamine (Q) to glutamic acid (E) results in a mass shift of +0.984 Da. Thus, from the resolution of our data, the second peak in the isotope distribution for a peptide containing one glutamine residue coincides with the first peak of the isotope distribution for the peptide in which the residue is deamidated. A genetic algorithm is used to determine the extent of deamidation that gives the best fit to the measured distribution. The method can be extended to peptides containing more than one glutamine residue. The extent of protein degradation assessed in this way could be used, for example, to assess the damage of collagen, and screen samples for radiocarbon dating and DNA analysis.
机译:使用低成本,高通量方法分析胶原蛋白肽,以使用基质辅助激光解吸/电离质谱(MALDI-MS)评估脱酰胺作用。对于每种选择的肽,计算理论分布,并将每个样品的测量分布与之比较以确定谷氨酰胺脱酰胺的程度。谷氨酰胺(Q)脱氨基至谷氨酸(E)导致质量偏移+0.984 Da。因此,从我们的数据分辨率来看,含有一个谷氨酰胺残基的肽的同位素分布的第二个峰与残基被酰胺化的肽的同位素分布的第一个峰重合。遗传算法用于确定脱酰胺程度,使其最适合所测分布。该方法可以扩展到包含一个以上谷氨酰胺残基的肽。以此方式评估的蛋白质降解程度可用于评估胶原蛋白的损伤,并筛选样品进行放射性碳测年和DNA分析。

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