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Lysophospholipase D and its role in LPA production

机译:溶血磷脂酶D及其在LPA产生中的作用

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Lysophosphatidic acid (LPA) is an important lipid mediator that binds to G-protein-coupled receptors of the Edg family, inducing proliferation and migration in many cell lines. Much has been learned about pathways involved in LPA signaling, but the pathways responsible for LPA production remain to be fully resolved. Several potential routes have been proposed for LPA production. One involves the sequential actions of phopholipase D (PLD) and phospholipase A(2) (PLA(2)). Another route involves the sequential actions of PLA2 and lysophospholipase D (lysoPLD). LysoPLD is defined as an enzyme which hydrolyzes lysophospholipids to produce LPA. Two major forms of lysoPLD, microsomal and extracellular forms, have been reported. A microsomal lysoPLD plays an important role in the metabolism of platelet-activating factor (PAF) because of its preference for alkyl-phospholipids. The extracellular form of lysoPLD coexists with its substrate, lysophosphatidylcholine (LPC), in the extracellular compartment. LysoPLDs purified from the extracellular space have recently been shown to be molecularly identical to autotaxin (ATX). ATX, an enzyme previously known to possess 5'-nucleotide pyrophosphatase and phosphodiesterase (PDE) activities, was subsequently shown to have lysoPLD activity. The unexpected linkage of the extracellular lysoPLD with ATX has raised many interesting questions. The characterization and purification of lysoPLDs are reviewed here. (C) 2004 Elsevier Inc. All rights reserved.
机译:溶血磷脂酸(LPA)是一种重要的脂质介体,可与Edg家族的G蛋白偶联受体结合,在许多细胞系中诱导增殖和迁移。关于LPA信号转导的途径已学到很多,但是负责LPA产生的途径仍有待完全解决。已经提出了用于LPA生产的几种潜在路线。一个涉及磷脂酶D(PLD)和磷脂酶A(2)(PLA(2))的顺序作用。另一途径涉及PLA2和溶血磷脂酶D(lysoPLD)的顺序作用。 LysoPLD被定义为水解溶血磷脂以产生LPA的酶。 lysoPLD的两种主要形式,即微粒体形式和细胞外形式,已有报道。微粒体溶血PLD在血小板活化因子(PAF)的代谢中起重要作用,因为它偏爱烷基磷脂。 lysoPLD的细胞外形式与其底物溶血磷脂酰胆碱(LPC)共存于细胞外区室。从细胞外空间纯化的LysoPLDs最近被证明与自分泌紫杉醇(ATX)在分子上相同。 ATX是一种先前已知具有5'-核苷酸焦磷酸酶和磷酸二酯酶(PDE)活性的酶,后来被证明具有lysoPLD活性。细胞外lysoPLD与ATX的意外连接引发了许多有趣的问题。 lysoPLDs的表征和纯化在这里进行综述。 (C)2004 Elsevier Inc.保留所有权利。

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