异戊酰半胱氨酸羧基甲基转移酶在肿瘤坏死因子- agr中的作用内皮细胞中血管细胞粘附分子-1表达的刺激

Mushtaq Ahmad, Yan Zhang, Yong Zhang, Christopher Papharalambus, R. Alexander
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引用次数: 30

摘要

我们之前已经表明,细胞因子刺激血管细胞粘附分子-1 (VCAM-1)的表达,而不是细胞间粘附分子-1 (ICAM-1)的表达,在内皮细胞中是氧化还原敏感的。在这里,我们研究了异戊酰半胱氨酸羧甲基转移酶(ICMTase)的作用,该酶能甲基化异戊酰化CAAX(其中C表示半胱氨酸;A,脂肪族氨基酸;和X,几乎任何其他氨基酸)蛋白质,包括Rac1,一种产生超氧化物的NAD(P)H氧化酶的成分,在VCAM-1的表达中。特异性ICMTase抑制剂n -乙酰基- s -法尼基-l-半胱氨酸(AFC)或n -乙酰基- s -香叶基-l-半胱氨酸(AGGC)预处理内皮细胞可抑制肿瘤坏死因子-&agr;(TNF-&agr;)刺激VCAM-1 mRNA表达,但对ICAM-1无影响。内皮细胞表达了组成性活性的ICMTase,这表明细胞中存在甲基化的Rac1和AFC。TNF -&agr;刺激细胞显著增加内皮细胞中AFC和Rac1的甲基化。ICMTase是氧化还原敏感信号通路的一个组成部分,TNF-&agr;对活性氧产生的AFC抑制也表明了这一点。有趣的是,Rac1的显性阴性亚型没有选择性,而是抑制TNF-&agr;刺激VCAM-1和ICAM-1 mRNA表达。因此,ICMTase是氧化还原敏感的vcam -1选择性信号通路的关键组成部分,它似乎通过Rac1的甲基化激活了一个离散的炎症信号通路,至少部分是这样。
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Role of Isoprenylcysteine Carboxyl Methyltransferase in Tumor Necrosis Factor-&agr; Stimulation of Expression of Vascular Cell Adhesion Molecule-1 in Endothelial Cells
We have previously shown that cytokine stimulation of the expression of vascular cell adhesion molecule-1 (VCAM-1), but not that of intercellular adhesion molecule-1 (ICAM-1), is redox sensitive in endothelial cells. Here, we investigated the role of isoprenylcysteine carboxyl methyltransferase (ICMTase), which methylates isoprenylated CAAX (where C indicates cysteine; A, aliphatic amino acids; and X, almost any other amino acid) proteins, including Rac1, a component of superoxide-generating NAD(P)H oxidase, in the expression of VCAM-1. Pretreatment of endothelial cells with N-acetyl-S-farnesyl-l-cysteine (AFC) or N-acetyl-S-geranylgeranyl-l-cysteine (AGGC), specific inhibitors of ICMTase, inhibited the tumor necrosis factor-&agr; (TNF-&agr;) stimulation of mRNA expression of VCAM-1 but not that of ICAM-1. Endothelial cells expressed constitutively active ICMTase, as suggested by the presence of methylated Rac1 and the methylation of AFC by the cells. TNF-&agr; stimulation of the cells significantly increased the methylation of AFC and Rac1 in endothelial cells. That ICMTase was a component of the redox-sensitive signaling pathway was also suggested by the AFC inhibition of the generation of reactive oxygen species by TNF-&agr;. Interestingly, the dominant-negative isoform of Rac1 was not selective but inhibited the TNF-&agr; stimulation of the mRNA expression of VCAM-1 and ICAM-1. Thus, ICMTase is a critical component of the redox-sensitive VCAM-1-selective signaling pathway, and it appears to activate a discrete inflammatory signaling pathway, at least in part, through the methylation of Rac1.
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