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糖尿病与质谱分析

Diabetes and mass spectrometry.

作者信息

Lapolla A, Fedele D, Traldi P

机构信息

Dipartimento di Scienze Mediche e Chirurgiche, Cattedra di Malattie del Metabolismo - Padova University, Via Vendramini 7, 35100 Padova, Italy.

出版信息

Diabetes Metab Res Rev. 2001 Mar-Apr;17(2):99-112. doi: 10.1002/dmrr.189.

Abstract

Mass spectrometry (MS) has been successfully employed to investigate non-enzymatic protein glycation, a process relevant in diabetic disease. The high sensitivity and specificity of this technique allowed the development of methods that can individuate and evaluate some glycation markers to be validly employed in monitoring diabetes. More recent mass spectrometric techniques, such as the matrix-assisted laser desorption/ionization (MALDI), are able to determine the molecular weight of intact proteins. They were first employed in studying the in vitro reaction between hexoses and different proteins. Once the validity of the results obtained by this analytical approach was confirmed, a series of investigations on plasma proteins were undertaken in healthy and diabetic subjects. The method led to the evaluation of the number of glucose molecules condensed on the protein being studied, and consequently can be validly used for an accurate follow-up of metabolic control in diabetic patients. When applied to studies on haemoglobin glycation, the method showed that both alpha- and beta-globins are glycated to a similar extent and that the simply glycated molecules are accompanied by glyco-oxidized species therefore giving information on the oxidative stress experimented on in the subject. Furthermore, in the case of immunoglobulins, MALDI/MS was able to determine not only the total glycation level of IgG, but also to establish that the fragment antigen binding (Fab) moiety is the most glycated one, thus suggesting that the possible immunological impairment sometimes invoked in diabetes is related to the inhibition of the process of molecular recognition between antibody and antigen.

摘要

质谱分析法(MS)已成功用于研究非酶蛋白糖基化,这是一个与糖尿病相关的过程。该技术的高灵敏度和特异性使得能够开发出一些方法,这些方法可以识别和评估某些糖基化标记物,从而有效地用于监测糖尿病。更新的质谱技术,如基质辅助激光解吸/电离(MALDI),能够确定完整蛋白质的分子量。它们最初用于研究己糖与不同蛋白质之间的体外反应。一旦通过这种分析方法获得的结果的有效性得到证实,便对健康和糖尿病受试者的血浆蛋白进行了一系列研究。该方法能够评估凝结在所研究蛋白质上的葡萄糖分子数量,因此可有效地用于对糖尿病患者的代谢控制进行准确的跟踪。当应用于血红蛋白糖基化研究时,该方法表明α-和β-珠蛋白的糖基化程度相似,并且简单糖基化的分子伴随着糖氧化产物,从而提供了有关受试者所经历的氧化应激的信息。此外,就免疫球蛋白而言,MALDI/MS不仅能够确定IgG的总糖基化水平,还能够确定片段抗原结合(Fab)部分是糖基化程度最高的部分,因此表明糖尿病中有时提到的可能的免疫损伤与抗体和抗原之间分子识别过程的抑制有关。

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