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莱氏无胆甾原体和肺炎链球菌中合成主要双层和非双层倾向膜脂的糖基转移酶的结构特征。

Structural features of glycosyltransferases synthesizing major bilayer and nonbilayer-prone membrane lipids in Acholeplasma laidlawii and Streptococcus pneumoniae.

作者信息

Edman Maria, Berg Stefan, Storm Patrik, Wikström Malin, Vikström Susanne, Ohman Anders, Wieslander Ake

机构信息

Department of Biochemistry, Umeå University, Sweden.

出版信息

J Biol Chem. 2003 Mar 7;278(10):8420-8. doi: 10.1074/jbc.M211492200. Epub 2002 Dec 2.

Abstract

In membranes of Acholeplasma laidlawii two consecutively acting glucosyltransferases, the (i) alpha-monoglucosyldiacylglycerol (MGlcDAG) synthase (alMGS) (EC ) and the (ii) alpha-diglucosyl-DAG (DGlcDAG) synthase (alDGS) (EC ), are involved in maintaining (i) a certain anionic lipid surface charge density and (ii) constant nonbilayer/bilayer conditions (curvature packing stress), respectively. Cloning of the alDGS gene revealed related uncharacterized sequence analogs especially in several Gram-positive pathogens, thermophiles and archaea, where the encoded enzyme function of a potential Streptococcus pneumoniae DGS gene (cpoA) was verified. A strong stimulation of alDGS by phosphatidylglycerol (PG), cardiolipin, or nonbilayer-prone 1,3-DAG was observed, while only PG stimulated CpoA. Several secondary structure prediction and fold recognition methods were used together with SWISS-MODEL to build three-dimensional model structures for three MGS and two DGS lipid glycosyltransferases. Two Escherichia coli proteins with known structures were identified as the best templates, the membrane surface-associated two-domain glycosyltransferase MurG and the soluble GlcNAc epimerase. Differences in electrostatic surface potential between the different models and their individual domains suggest that electrostatic interactions play a role for the association to membranes. Further support for this was obtained when hybrids of the N- and C-domain, and full size alMGS with green fluorescent protein were localized to different regions of the E. coli inner membrane and cytoplasm in vivo. In conclusion, it is proposed that the varying abilities to bind, and sense lipid charge and curvature stress, are governed by typical differences in charge (pI values), amphiphilicity, and hydrophobicity for the N- and (catalytic) C-domains of these structurally similar membrane-associated enzymes.

摘要

在莱氏无胆甾原体的膜中,两种连续作用的葡糖基转移酶,即(i)α-单葡糖基二酰甘油(MGlcDAG)合酶(alMGS)(EC )和(ii)α-二葡糖基-DAG(DGlcDAG)合酶(alDGS)(EC ),分别参与维持(i)一定的阴离子脂质表面电荷密度和(ii)恒定的非双层/双层条件(曲率堆积应力)。alDGS基因的克隆揭示了相关的未表征序列类似物,特别是在几种革兰氏阳性病原体、嗜热菌和古细菌中,其中潜在的肺炎链球菌DGS基因(cpoA)的编码酶功能得到了验证。观察到磷脂酰甘油(PG)、心磷脂或易于形成非双层的1,3-DAG对alDGS有强烈刺激,而只有PG刺激CpoA。几种二级结构预测和折叠识别方法与SWISS-MODEL一起用于构建三种MGS和两种DGS脂质糖基转移酶的三维模型结构。两种具有已知结构的大肠杆菌蛋白被确定为最佳模板,即膜表面相关的双结构域糖基转移酶MurG和可溶性GlcNAc差向异构酶。不同模型及其各个结构域之间静电表面电位的差异表明,静电相互作用在与膜的结合中起作用。当N结构域和C结构域的杂交体以及全尺寸alMGS与绿色荧光蛋白在体内定位于大肠杆菌内膜和细胞质的不同区域时,得到了对此的进一步支持。总之,有人提出,这些结构相似的膜相关酶的N结构域和(催化)C结构域在电荷(pI值)、两亲性和疏水性方面的典型差异决定了它们结合、感知脂质电荷和曲率应力的不同能力。

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