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晚期糖基化终末产物(AGEs):糖尿病中的药理学抑制作用

Advanced glycation endproducts (AGEs): Pharmacological inhibition in diabetes.

作者信息

Peyroux J, Sternberg M

机构信息

Equipe de recherche Protéines Modifiées, Protéases et Physiopathologie de l'Endothélium Vasculaire, laboratoire de pharmacologie, faculté de pharmacie, université Paris-V, Paris, France.

出版信息

Pathol Biol (Paris). 2006 Sep;54(7):405-19. doi: 10.1016/j.patbio.2006.07.006. Epub 2006 Sep 15.

Abstract

AGE inhibitors may act by various mechanisms at different steps of advanced glycation endproduct (AGE) formation (depending on oxidative stress and/or carbonyl stress) and AGE-mediated damage: trapping of reactive dicarbonyl species; antioxidant activity by transition metal chelation; other antioxidant activity including free radical scavenging; AGE cross-link breaking; AGE receptor (RAGE) blocking; RAGE signaling blocking; glycemia reduction by anti-diabetic therapy; aldose reductase inhibition; shunting of trioses-P towards the pentose-P pathway by transketolase activation. Most of the inhibitors have several sites of action. Practically one can distinguish drugs specifically developed as AGE inhibitors or AGE breakers; RAGE and receptor signaling blockers; other therapeutic compounds which were found subsequently to possess also AGE inhibitor activity, including dietary antioxidants. Encouraging results obtained in studies of various AGE inhibitors, conducted in vitro and in diabetic animals, are summarized in this review. However most of the clinical trials have been more or less disappointing, in part because of side effects; the long-term therapeutic interest of the most recently developed AGE inhibitors or breakers remains to be demonstrated in diabetes.

摘要

晚期糖基化终产物(AGE)抑制剂可通过多种机制作用于AGE形成的不同步骤(取决于氧化应激和/或羰基应激)以及AGE介导的损伤:捕获活性二羰基化合物;通过过渡金属螯合发挥抗氧化活性;包括清除自由基在内的其他抗氧化活性;破坏AGE交联;阻断AGE受体(RAGE);阻断RAGE信号传导;通过抗糖尿病治疗降低血糖;抑制醛糖还原酶;通过激活转酮醇酶将磷酸丙糖导向磷酸戊糖途径。大多数抑制剂具有多个作用位点。实际上,可以区分专门开发为AGE抑制剂或AGE裂解剂的药物;RAGE和受体信号传导阻断剂;其他后来发现也具有AGE抑制剂活性的治疗化合物,包括膳食抗氧化剂。本文综述了在体外和糖尿病动物中对各种AGE抑制剂进行研究时获得的令人鼓舞的结果。然而,大多数临床试验或多或少都令人失望,部分原因是副作用;最新开发的AGE抑制剂或裂解剂的长期治疗价值仍有待在糖尿病中得到证实。

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