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Quantitative screening of advanced glycation endproducts in cellular and extracellular proteins by tandem mass spectrometry.

机译:通过串联质谱定量筛选细胞和细胞外蛋白中高级糖基化终产物。

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摘要

Glycation of proteins forms fructosamines and advanced glycation endproducts. Glycation adducts may be risk markers and risk factors of disease development. We measured the concentrations of the early glycation adduct fructosyl-lysine and 12 advanced glycation endproducts by liquid chromatography with tandem mass spectrometric detection. Underivatized analytes were detected free in physiological fluids and in enzymic hydrolysates of cellular and extracellular proteins. Hydroimidazolones were the most important glycation biomarkers quantitatively; monolysyl adducts (N(epsilon)-carboxymethyl-lysine and N(epsilon)-1-carboxyethyl-lysine) were found in moderate amounts, and bis(lysyl)imidazolium cross-links and pentosidine in lowest amounts. Quantitative screening showed high levels of advanced glycation endproducts in cellular protein and moderate levels in protein of blood plasma. Glycation adduct accumulation in tissues depended on the particular adduct and tissue type. Low levels of free advanced glycation endproducts were found in blood plasma and levels were 10-100-fold higher in urine. Advanced glycation endproduct residues were increased in blood plasma and at sites of vascular complications development in experimental diabetes; renal glomeruli, retina and peripheral nerve. In clinical uraemia, the concentrations of plasma protein advanced glycation endproduct residues increased 1-7-fold and free adduct concentrations increased up to 50-fold. Comprehensive screening of glycation adducts revealed the relative and quantitative importance of alpha-oxoaldehyde-derived advanced glycation endproducts in physiological modification of proteins-particularly hydroimidazolones, the efficient renal clearance of free adducts, and the marked increases of glycation adducts in diabetes and uraemia-particularly free advanced glycation endproducts in uraemia. Increased levels of these advanced glycation endproducts were associated with vascular complications in diabetes and uraemia.
机译:蛋白质的糖基化形成果糖胺和高级糖基化终产物。糖化加合物可能是疾病发展的危险标志和危险因素。我们通过串联质谱检测的液相色谱法测量了早期糖基化加合物果糖基赖氨酸和12种晚期糖基化终产物的浓度。在生理液以及细胞和细胞外蛋白的酶水解物中,未检测到未衍生化的分析物。在定量上,氢咪唑酮是最重要的糖基化生物标志物。发现单糖基加合物(N(ε)-羧甲基赖氨酸和N(ε)-1-羧乙基赖氨酸)的量适中,而双(赖氨酰)咪唑鎓的交联和戊糖苷的量最低。定量筛选显示细胞蛋白中高级糖基化终产物水平高,血浆蛋白中度水平中等。组织中糖基化加合物的积累取决于特定的加合物和组织类型。在血浆中发现低水平的游离高级糖基化终产物,而在尿中的水平高10-100倍。实验性糖尿病患者血浆和血管并发症发生部位的晚期糖基化终产物残留增加;肾小球,视网膜和周围神经。在临床尿毒症中,血浆蛋白晚期糖基化终产物残留物的浓度增加1-7倍,游离加合物浓度增加至50倍。糖基化加合物的全面筛选揭示了α-氧醛衍生的高级糖基化终产物在蛋白质(尤其是氢咪唑啉酮)的生理修饰,游离加合物的有效肾脏清除以及糖基化加合物在糖尿病和尿毒症中的显着增加中的相对和定量重要性。尿毒症中的免费晚期糖基化终产物。这些晚期糖基化终产物水平的增加与糖尿病和尿毒症中的血管并发症有关。

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