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确定 PORCN 的膜拓扑结构,PORCN 是一种酰基转移酶,可修饰 Wnt 信号蛋白。

Determination of the membrane topology of PORCN, an O-acyl transferase that modifies Wnt signalling proteins.

机构信息

Department of Biology, San Francisco State University, 1600 Holloway Avenue, San Francisco, CA 94132, USA.

Department of Chemistry and Biochemistry, San Francisco State University, 1600 Holloway Avenue, San Francisco, CA 94132, USA.

出版信息

Open Biol. 2021 Jun;11(6):200400. doi: 10.1098/rsob.200400. Epub 2021 Jun 30.

DOI:10.1098/rsob.200400
PMID:34186010
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8241489/
Abstract

Wnt gradients elicit distinct cellular responses, such as proliferation, specification, differentiation and survival in a dose-dependent manner. Porcupine (PORCN), a membrane-bound O-acyl transferase (MBOAT) that resides in the endoplasmic reticulum, catalyses the addition of monounsaturated palmitate to Wnt proteins and is required for Wnt gradient formation and signalling. In humans, PORCN mutations are causal for focal dermal hypoplasia (FDH), an X-linked dominant syndrome characterized by defects in mesodermal and endodermal tissues. PORCN is also an emerging target for cancer therapeutics. Despite the importance of this enzyme, its structure remains poorly understood. Recently, the crystal structure of DltB, an MBOAT family member from bacteria, was solved. In this report, we use experimental data along with homology modelling to DltB to determine the membrane topology of PORCN. Our studies reveal that PORCN has 11 membrane domains, comprising nine transmembrane spanning domains and two reentrant domains. The N-terminus is oriented towards the lumen while the C-terminus is oriented towards the cytosol. Like DltB, PORCN has a funnel-like structure that is encapsulated by multiple membrane-spanning helices. This new model for PORCN topology allows us to map residues that are important for biological activity (and implicated in FDH) onto its three-dimensional structure.

摘要

Wnt 梯度以剂量依赖的方式引发不同的细胞反应,如增殖、特化、分化和存活。Porcupine(PORCN)是一种位于内质网中的膜结合酰基转移酶(MBOAT),它催化 Wnt 蛋白中不饱和棕榈酸的添加,是 Wnt 梯度形成和信号传导所必需的。在人类中,PORCN 突变是局灶性皮肤发育不良(FDH)的原因,这是一种 X 连锁显性综合征,其特征是中胚层和内胚层组织缺陷。PORCN 也是癌症治疗的新兴靶点。尽管这种酶很重要,但它的结构仍然知之甚少。最近,从细菌中分离出的 MBOAT 家族成员 DltB 的晶体结构被解析。在本报告中,我们使用实验数据以及与 DltB 的同源建模来确定 PORCN 的膜拓扑结构。我们的研究表明,PORCN 有 11 个跨膜结构域,包括 9 个跨膜结构域和 2 个折返结构域。N 端朝向腔,而 C 端朝向细胞质。与 DltB 一样,PORCN 具有一个漏斗状结构,由多个跨膜螺旋包裹。PORCN 拓扑结构的这个新模型使我们能够将对生物学活性很重要的残基(与 FDH 有关)映射到其三维结构上。

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The ghrelin -acyltransferase structure reveals a catalytic channel for transmembrane hormone acylation.胃饥饿素酰基转移酶结构揭示了跨膜激素酰化的催化通道。
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PORCN inhibition synergizes with PI3K/mTOR inhibition in Wnt-addicted cancers.
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