Design, synthesis and bioactions of novel stable mimetics of lipoxins and aspirin-triggered lipoxins

被引:50
|
作者
Petasis, NA [1 ]
Akritopoulou-Zanze, I
Fokin, VV
Bernasconi, G
Keledjian, R
Yang, R
Uddin, J
Nagulapalli, KC
Serhan, CN
机构
[1] Univ So Calif, Dept Chem, Los Angeles, CA 90089 USA
[2] Univ So Calif, Loker Hydrocarbon Res Inst, Los Angeles, CA 90089 USA
[3] Brigham & Womens Hosp, Dept Anesthesiol Perioperat & Pain Med, Ctr Expt Therapeut & Reperfus Injury, Boston, MA 02115 USA
[4] Harvard Univ, Sch Med, Boston, MA 02115 USA
关键词
D O I
10.1016/j.plefa.2005.05.020
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The lipoxins (LX) are a class of potent endogenous oxygenated products that are enzymatically generated from arachidonic acid and have novel anti-inflammatory properties and promote resolution. Elucidation of the biochemical pathways involved in the metabolic inactivation of LX and the discovery of the aspirin-triggered lipoxins (ATL) provided the basis for the design and synthesis of stable analogs of LX and ATL. This special issue review describes the efforts that led to the design and synthesis of stable LX/ATL mimetics, which permitted the detailed elucidation of their novel biological roles, leading to the development of new anti-inflammatory agents that mimic their actions. These synthetic molecules provided the means to uncover the physiologic roles of both the LX and the ATL biosynthetic pathways which led to several unexpected discoveries. Among these findings is the involvement of polyisoprenyl phosphates (PIPP) in intracellular signaling mediated by presqualene diphosphate (PSDP), and the recognition of the novel roles of these lipid mediators in regulating cell trafficking during inflammation as well as in promoting resolution of inflammatory processes. These efforts also provided the basis for examining the potential therapeutic role of LX/ATL stable mimetics and led to the development of new analogs with improved pharmacokinetics that opened the way to potentially new approaches to treating human diseases. (c) 2005 Elsevier Ltd. All rights reserved.
引用
收藏
页码:301 / 321
页数:21
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