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Reductive Amination Combining Dimethylation for Quantitative Analysis of Early-Stage Glycated Proteins

机译:结合二甲基化与早期糖化蛋白定量分析的还原胺化

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摘要

Due to the critical role glycation plays in many serious pathological conditions, such as diabetes, it is of great significance to discover protein glycation at an early stage for precaution and prediction of the disease. Here, a method of reductive amination combining dimethylation (RAD) was developed for the quantification of early-stage glycated proteins. The quantitative analysis was first carried out by reducing the samples using NaBH3CN or NaBD3CN, resulting in a 1 Da mass shift and the stabilization of early-stage protein glycation. The two samples were then digested and isotopically dimethylated to achieve the mass shift of 4m + 3n (m represents the number of N-termini and Lys residues, and n represents the number of glycated sites) between light-and heavy-labeled glycated peptides for quantification. Consequently, the false positive result can be removed according to the different mass shifts of glycated peptides and non-glycated peptides. In quantification of glycated myoglobin, RAD showed good linearity (R-2 0.99) and reproducibility (CVs = 1.6%) in 2 orders of magnitude (1:10-10:1). RAD was then applied to quantify the endogenous glycated proteins in the serum of diabetic patients, revealing significant differences in the glycation level between the patients with complicated retinal detachment and those without. In conclusion, RAD is an effective method for quantifying endogenous glycated proteins.
机译:由于关键的作用糖甘露花在许多严重的病理病症中起作用,例如糖尿病,在早期阶段发现蛋白质糖化是预防和预测这种疾病的重要意义。这里,开发了结合二甲基化(Rad)的还原胺化的方法以进行早期糖化蛋白的定量。首先通过使用NaBH 3Cn或NaBD3CN减少样品来进行定量分析,导致1A大规模转移和早期蛋白质糖化的稳定性。然后将两个样品消化和同位素二甲基化以达到4m + 3N(表示N-末端和Lys残基的数量,并且N表示光和重标记的糖化肽之间的糖化位点的数量)量化。因此,可以根据糖化肽和非糖化肽的不同质量偏移去除假阳性结果。在定量糖化术骨蛋白蛋白,rAt显示出良好的线性度(R-2& 0.99)和再现性(CVS& = 1.6%)2个数量级(1:10-10:1)。然后施用Rad以量化糖尿病患者血清中的内源性糖化蛋白,揭示了复杂视网膜脱离和那些患者之间的糖化水平的显着差异。总之,RAD是定量内源性糖化蛋白的有效方法。

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  • 来源
    《Analytical chemistry》 |2018年第6期|共7页
  • 作者单位

    Fudan Univ Minist Publ Hlth Shanghai Canc Ctr Shanghai 200032 Peoples R China;

    Fudan Univ Dept Chem Shanghai 200433 Peoples R China;

    Fudan Univ Minist Publ Hlth Shanghai Canc Ctr Shanghai 200032 Peoples R China;

    Fudan Univ Minist Publ Hlth Shanghai Canc Ctr Shanghai 200032 Peoples R China;

    Fudan Univ Minist Publ Hlth Shanghai Canc Ctr Shanghai 200032 Peoples R China;

    Fudan Univ Minist Publ Hlth Shanghai Canc Ctr Shanghai 200032 Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
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