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转谷氨酰胺酶1的一种新功能:通过酯键形成将长链ω-羟基神经酰胺连接到内披蛋白上。

A novel function for transglutaminase 1: attachment of long-chain omega-hydroxyceramides to involucrin by ester bond formation.

作者信息

Nemes Z, Marekov L N, Fésüs L, Steinert P M

机构信息

Laboratory of Skin Biology, National Institute of Arthritis and Musculoskeletal and Skin Diseases, National Institutes of Health, Bethesda, MD 20892-2752, USA.

出版信息

Proc Natl Acad Sci U S A. 1999 Jul 20;96(15):8402-7. doi: 10.1073/pnas.96.15.8402.

Abstract

Transglutaminases (TGases) are defined as enzymes capable of forming isopeptide bonds by transfer of an amine onto glutaminyl residues of a protein. Here we show that the membrane-bound form of the TGase 1 enzyme can also form ester bonds between specific glutaminyl residues of human involucrin and a synthetic analog of epidermal specific omega-hydroxyceramides. The formation of a approximately 5-nm-thick lipid envelope on the surface of epidermal keratinocytes is an important component of normal barrier function. The lipid envelope consists of omega-hydroxyceramides covalently linked by ester bonds to cornified envelope proteins, most abundantly to involucrin. We synthesized an analog of natural omega-hydroxyceramides N-[16-(16-hydroxyhexadecyl)oxypalmitoyl]sphingosine (lipid Z). When recombinant human TGase 1 and involucrin were reacted on the surface of synthetic lipid vesicles containing lipid Z, lipid Z was attached to involucrin and formed saponifiable protein-lipid adducts. By mass spectroscopy and sequencing of tryptic lipopeptides, the ester linkage formation used involucrin glutamine residues 107, 118, 122, 133, and 496 by converting the gamma-carboxamido groups to lipid esters. Several of these residues have been found previously to be attached to ceramides in vivo. Mass spectrometric analysis after acetonide derivatization also revealed that ester formation involved primarily the omega-hydroxyl group of lipid Z. Our data reveal a dual role for TGase 1 in epidermal barrier formation and provide insights into the pathophysiology of lamellar ichthyosis resulting from defects of TGase 1 enzyme.

摘要

转谷氨酰胺酶(TGases)被定义为能够通过将胺转移到蛋白质的谷氨酰胺残基上来形成异肽键的酶。在此我们表明,TGase 1酶的膜结合形式还能在人内披蛋白的特定谷氨酰胺残基与表皮特异性ω-羟基神经酰胺的合成类似物之间形成酯键。在表皮角质形成细胞表面形成约5纳米厚的脂质包膜是正常屏障功能的重要组成部分。脂质包膜由通过酯键共价连接到角质包膜蛋白上的ω-羟基神经酰胺组成,其中与内披蛋白的连接最为丰富。我们合成了天然ω-羟基神经酰胺N-[16-(16-羟基十六烷基)氧基棕榈酰]鞘氨醇(脂质Z)的类似物。当重组人TGase 1和内披蛋白在含有脂质Z的合成脂质囊泡表面反应时,脂质Z附着在内披蛋白上并形成可皂化的蛋白质-脂质加合物。通过对胰蛋白酶消化的脂肽进行质谱分析和测序,酯键的形成利用了内披蛋白的谷氨酰胺残基107、118、122、133和496,即将γ-羧酰胺基团转化为脂质酯。先前已发现这些残基中的几个在体内与神经酰胺相连。丙酮化物衍生化后的质谱分析还表明,酯的形成主要涉及脂质Z的ω-羟基。我们的数据揭示了TGase 1在表皮屏障形成中的双重作用,并为TGase 1酶缺陷导致的板层状鱼鳞病的病理生理学提供了见解。

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