首页> 外文期刊>Frontiers in Cell and Developmental Biology >The structure and function of acylglycerophosphate acyltransferase 4/ lysophosphatidic acid acyltransferase delta (AGPAT4/LPAATd)
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The structure and function of acylglycerophosphate acyltransferase 4/ lysophosphatidic acid acyltransferase delta (AGPAT4/LPAATd)

机译:酰基甘油磷酸酯酰基转移酶4 /溶血磷脂酸酰基转移酶δ(AGPAT4 / LPAATd)的结构和功能

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Lipid-modifying enzymes serve crucial roles in cellular processes such as signal transduction (producing lipid-derived second messengers), intracellular membrane transport (facilitating membrane remodeling needed for membrane fusion/fission), and protein clustering (organizing lipid domains as anchoring platforms). The lipid products crucial in these processes can derive from different metabolic pathways, thus it is essential to know the localization, substrate specificity, deriving products (and their function) of all lipid-modifying enzymes. Here we discuss an emerging family of these enzymes, the lysophosphatidic acid acyltransferases (LPAATs), also known as acylglycerophosphate acyltransferases (AGPATs), that produce phosphatidic acid (PA) having as substrates lysophosphatidic acid (LPA) and acyl-CoA. Eleven LPAAT/AGPAT enzymes have been identified in mice and humans based on sequence homologies, and their localization, specific substrates and functions explored. We focus on one member of the family, LPAATδ, a protein expressed mainly in brain and in muscle (though to a lesser extent in other tissues); while at the cellular level it is localized at the trans-Golgi network membranes and at the mitochondrial outer membranes. LPAAT??is a physiologically-essential enzyme since mice knocked-out for Lpaatδ show severe dysfunctions including cognitive impairment, impaired force contractility and altered white adipose tissue. The LPAAT??physiological roles are related to the formation of its product PA. PA is a multifunctional lipid involved in cell signalling as well as in membrane remodelling. In particular, the LPAAT?-catalyzed conversion of LPA (inverted-cone-shaped lipid) to PA (cone-shaped lipid) is considered a mechanism of deformation of the bilayer that favors membrane fission. Indeed, LPAAT? is an essential component of the fission-inducing machinery driven by the protein BARS. In this process, a protein-tripartite complex (BARS/14-3-3??phosphoinositide kinase PI4KIII???is recruited at the trans-Golgi network, at the sites where membrane fission is to occur; there, LPAAT??directly interacts with BARS and is activated by BARS. The resulting formation of PA is essential for membrane fission occurring at those spots. Also in mitochondria PA formation has been related to fusion/fission events. Since PA is formed by various enzymatic pathways in different cell compartments, the BARS-LPAAT? interaction indicates the relevance of lipid-modifying enzymes acting exactly where their products are needed (i.e., PA at the Golgi membranes).
机译:脂质修饰酶在细胞过程中起着至关重要的作用,例如信号转导(产生脂质衍生的第二信使),细胞内膜运输(促进膜融合/裂变所需的膜重塑)和蛋白质聚类(将脂质结构域作为锚定平台组织)。在这些过程中至关重要的脂质产物可以源自不同的代谢途径,因此必须了解所有脂质修饰酶的定位,底物特异性,衍生产物(及其功能)。在这里,我们讨论了这些酶的新兴家族,即溶血磷脂酸酰基转移酶(LPAAT),也称为酰基甘油磷酸酯酰基转移酶(AGPAT),它们产生以溶血磷脂酸(LPA)和酰基辅酶A为底物的磷脂酸(PA)。根据序列同源性,已在小鼠和人类中鉴定出11种LPAAT / AGPAT酶,并对其定位,特定底物和功能进行了研究。我们关注家族中的一个成员LPAATδ,该蛋白主要在大脑和肌肉中表达(尽管在其他组织中表达较少);而在细胞水平上,它位于反高尔基网络膜和线粒体外膜。 LPAATβ是一种生理必需的酶,因为敲除Lpaatδ的小鼠表现出严重的功能障碍,包括认知障碍,力收缩力受损和白色脂肪组织改变。 LPAATα的生理作用与其产物PA的形成有关。 PA是一种参与细胞信号转导和膜重塑的多功能脂质。特别是,LPAAT 2催化的LPA(倒圆锥形脂质)向PA(圆锥形脂质)的转化被认为是双层变形的有利于膜裂变的机制。确实,LPAAT吗?是蛋白质BARS驱动的裂变诱导机器的重要组成部分。在这一过程中,蛋白质-三方复合物(BARS /14-3-3β-磷酸肌醇激酶PI4KIIIβ-β)在反式高尔基网络中发生膜裂变的位置被募集;在那里,LPAATβ3-β直接与BARS相互作用并被BARS激活,由此形成的PA的形成对于在这些点发生的膜裂变是必不可少的,而且在线粒体中,PA的形成与融合/裂变事件有关,因为PA是通过不同细胞室内各种酶促途径形成的,BARS-LPAAT?相互作用表明脂质修饰酶确实在需要其产物的地方起作用(即高尔基体膜上的PA)具有相关性。

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