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Glycation Induced Modification and Identification of AGEs-Precursors and AGEs in Human Serum albumin

机译:糖化诱导人血清白蛋白中生前体和年龄的修饰和鉴定

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AGEs are a heterogeneous group of proteins that have been shown to react with the amino group of the N-terminal amino acid residue and the side-chains of arginine and lysine residues. Glycation induced protein modifications has been implicated in diabetes and its associated complications like nephropathy, retinopathy, aging as well as in atherosclerosis, Alzheimer's and Parkinson's diseases. The identification and structure elucidation of AGEs is therefore of great importance. Mass spectrometry, due to its high specificity and sensitivity, has widely been applied for the identification and structure elucidation of AGEs. We report the identification of AGEs-precursors and AGEs based on relative mass changes due to specific AGEs formation. HPLC-ESIMS, ESI-MS/MS and mascot data base were used to identify peptides sequence for non-glycated HSA. The relative mass changes due to specific AGE-precursors and AGEs formation were added to the non-glycated peptides followed by a thorough manual search of the glycated samples that resulted in the identification of ten modified peptides for the formation of five AGEs namely CML (1), Pyrraline (3), Imidazolone A (2), Imidazolone B (1) and AFGP (3). Also, seven glycated peptides were identified for the formation of AGEs-precursors.
机译:年龄是一种异质的蛋白质组,已被证明与N-末端氨基酸残基的氨基和精氨酸和赖氨酸残基的侧链反应。糖糖诱导的蛋白质修饰涉及糖尿病及其相关的并发症,如肾病,视网膜病变,老化以及动脉粥样硬化,阿尔茨海默氏症和帕金森病。因此,年龄阐释的鉴定和结构非常重要。由于其高特异性和灵敏度,质谱广泛应用于年龄的鉴定和结构阐明。我们报告了基于特异性年龄的相对质量变化来鉴定年龄和年龄。 HPLC-ESIMS,ESI-MS / MS和吉祥物数据碱用于鉴定非糖化HSA的肽序列。由于特异性前体和年龄形成的相对质量变化加入到非糖化肽中,然后进行彻底的手动搜索糖化样品,导致鉴定10个改性肽的含量为5时代即CML(1 ),咪唑酮A(2),咪唑酮B(1)和AFGP(3)。此外,鉴定出七种糖化肽以形成血液前体的形成。

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