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晚期糖基化终末产物及其受体在高血压病理生理学中起作用吗?

Do Advanced Glycation End Products and Its Receptor Play a Role in Pathophysiology of Hypertension?

作者信息

Prasad Kailash, Mishra Manish

机构信息

Department of Physiology, College of Medicine, University of Saskatchewan, Saskatchewan, Canada.

出版信息

Int J Angiol. 2017 Mar;26(1):1-11. doi: 10.1055/s-0037-1598183. Epub 2017 Feb 3.

Abstract

There is a close relationship between arterial stiffness and blood pressure. The studies suggest that the advanced glycation end products (AGEs) and its cell receptor (RAGE) are involved in the arterial stiffness in two ways: changes in arterial structure and vascular function. Plasma levels of AGEs and expression of RAGE are elevated, while the levels of soluble RAGE (sRAGE) and endogenous secretory RAGE (esRAGE) are lowered in patients with hypertension (HTN). There is a positive correlation between plasma levels of AGEs and arterial stiffness, and an inverse association between arterial stiffness/HTN, and serum levels of sRAGE and esRAGE. Various measures can reduce the levels of AGEs and expression of RAGE, and elevate sRAGE. Arterial stiffness and blood pressure could be reduced by lowering the serum levels of AGEs, and increasing the levels of sRAGE. Levels of AGEs can be lowered by reducing the consumption of AGE-rich diet, short duration of cooking in moist heat at low temperature, and cessation of cigarette smoking. Drugs such as aminoguanidine, vitamins, angiotensin-converting enzyme (ACE) inhibitors, angiotensin-II receptor blockers, statins, and metformin inhibit AGE formation. Alagebrium, an AGE breakers reduces levels of AGEs. Clinical trials with some drugs tend to reduce stiffness. Systemic administration of sRAGE has beneficial effect in animal studies. In conclusion, AGE-RAGE axis is involved in arterial stiffness and HTN. The studies suggest that inhibition of AGEs formation, reduction of AGE consumption, blockade of AGE-RAGE interaction, suppression of RAGE expression, and exogenous administration of sRAGE may be novel therapeutic strategies for treatment of arterial stiffness and HTN.

摘要

动脉僵硬度与血压之间存在密切关系。研究表明,晚期糖基化终产物(AGEs)及其细胞受体(RAGE)通过两种方式参与动脉僵硬度:动脉结构改变和血管功能变化。高血压(HTN)患者的血浆AGEs水平和RAGE表达升高,而可溶性RAGE(sRAGE)和内源性分泌型RAGE(esRAGE)水平降低。血浆AGEs水平与动脉僵硬度呈正相关,动脉僵硬度/HTN与血清sRAGE和esRAGE水平呈负相关。多种措施可降低AGEs水平和RAGE表达,并提高sRAGE水平。降低血清AGEs水平并提高sRAGE水平可降低动脉僵硬度和血压。减少富含AGE饮食的摄入、低温湿热处理的短烹饪时间以及戒烟可降低AGEs水平。氨基胍、维生素、血管紧张素转换酶(ACE)抑制剂、血管紧张素II受体阻滞剂、他汀类药物和二甲双胍等药物可抑制AGE形成。AGE裂解剂阿格列汀可降低AGEs水平。一些药物的临床试验倾向于降低僵硬度。在动物研究中,全身给予sRAGE具有有益作用。总之,AGE-RAGE轴参与动脉僵硬度和HTN。研究表明,抑制AGEs形成、减少AGE消耗、阻断AGE-RAGE相互作用、抑制RAGE表达以及外源性给予sRAGE可能是治疗动脉僵硬度和HTN的新型治疗策略。

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