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糖化血清白蛋白与 AGE 受体

Glycated Serum Albumin and AGE Receptors.

机构信息

School of Pharmacy, North Dakota State University, Fargo, North Dakota, USA.

出版信息

Adv Clin Chem. 2015;72:205-75. doi: 10.1016/bs.acc.2015.07.005. Epub 2015 Sep 19.

Abstract

In vivo modification of proteins by molecules with reactive carbonyl groups leads to intermediate and advanced glycation end products (AGE). Glucose is a significant glycation reagent due to its high physiological concentration and poorly controlled diabetics show increased albumin glycation. Increased levels of glycated and AGE-modified albumin have been linked to diabetic complications, neurodegeneration, and vascular disease. This review discusses glycated albumin formation, structural consequences of albumin glycation on drug binding, removal of circulating AGE by several scavenger receptors, as well as AGE-induced proinflammatory signaling through activation of the receptor for AGE. Analytical methods for quantitative detection of protein glycation and AGE formation are compared. Finally, the use of glycated albumin as a novel clinical marker to monitor glycemic control is discussed and compared to glycated hemoglobin (HbA1c) as long-term indicator of glycemic status.

摘要

体内具有反应性羰基基团的分子对蛋白质的修饰会导致中间和晚期糖基化终产物(AGE)。由于葡萄糖的生理浓度高且控制不佳,糖尿病患者的白蛋白糖化作用增加,因此葡萄糖是一种重要的糖化试剂。糖化和 AGE 修饰的白蛋白水平升高与糖尿病并发症、神经退行性变和血管疾病有关。本文综述了糖化白蛋白的形成、白蛋白糖化对药物结合的结构后果、几种清道夫受体对循环 AGE 的清除,以及 AGE 通过激活 AGE 受体诱导的促炎信号。比较了定量检测蛋白质糖化和 AGE 形成的分析方法。最后,讨论了将糖化白蛋白作为新型临床标志物来监测血糖控制的用途,并与作为血糖状态长期指标的糖化血红蛋白(HbA1c)进行了比较。

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