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血浆血小板活化因子乙酰水解酶(PAF-AH)。

Plasma platelet activating factor-acetylhydrolase (PAF-AH).

作者信息

Karasawa Ken, Harada Ayako, Satoh Noriko, Inoue Keizo, Setaka Morio

机构信息

Faculty of Pharmaceutical Sciences, Teikyo University, Sagamiko, Kanagawa, Japan.

出版信息

Prog Lipid Res. 2003 Mar;42(2):93-114. doi: 10.1016/s0163-7827(02)00049-8.

DOI:10.1016/s0163-7827(02)00049-8
PMID:12547653
Abstract

The platelet-activating factor-acetylhydrolase (PAF-AH) is an enzyme which catalyzes the hydrolysis of acetyl ester at the sn-2 position of PAF. The family of PAF-AHs consists of two intracellular isoforms (Ib and II), and one secreted isoform (plasma). These PAF-AHs show different biochemical characteristics and molecular structures. Plasma PAF-AH and intracellular isoform, II degrade not only PAF but also oxidatively fragmented phospholipids with potent biological activities. Among these PAF-AHs, plasma PAF-AH has been the target of many clinical studies in inflammatory diseases, such as asthma, sepsis, and vascular diseases, because the plasma PAF-AH activity in the patients with these diseases is altered when compared with normal individuals. Finding a genetic deficiency in the plasma PAF-AH opened the gate in elucidating the protecting role of this enzyme in inflammatory diseases. The most common loss-of-function mutation, V279F, is found in more than 30% of Japanese subjects (4% homozygous, 27% heterozygous). This single nucleotide polymorphism in plasma PAF-AH and the resulting enzymatic deficiency is thought to be a genetic risk factor in various inflammatory diseases in Japanese subjects. Administration of recombinant plasma PAF-AH or transfer of the plasma PAF-AH gene improves pathology in animal models. Therefore, substitution of plasma PAF-AH would be an effective in the treatment of the patients with the inflammatory diseases and a novel clinical approach. In addition, the detection of polymorphisms in the plasma PAF-AH gene and abnormalities in enzyme activity would be beneficial in the diagnosis of the inflammatory diseases.

摘要

血小板活化因子乙酰水解酶(PAF-AH)是一种催化PAF sn-2位乙酰酯水解的酶。PAF-AH家族由两种细胞内同工型(Ib和II)和一种分泌型同工型(血浆型)组成。这些PAF-AH表现出不同的生化特性和分子结构。血浆PAF-AH和细胞内同工型II不仅能降解PAF,还能降解具有强大生物活性的氧化碎片化磷脂。在这些PAF-AH中,血浆PAF-AH一直是许多炎症性疾病临床研究的靶点,如哮喘、败血症和血管疾病,因为与正常个体相比,这些疾病患者的血浆PAF-AH活性会发生改变。发现血浆PAF-AH的基因缺陷为阐明该酶在炎症性疾病中的保护作用打开了大门。最常见的功能丧失突变V279F在超过30%的日本受试者中被发现(4%纯合子,27%杂合子)。血浆PAF-AH中的这种单核苷酸多态性以及由此导致的酶缺乏被认为是日本受试者各种炎症性疾病的遗传风险因素。给予重组血浆PAF-AH或转移血浆PAF-AH基因可改善动物模型中的病理状况。因此,替代血浆PAF-AH将是治疗炎症性疾病患者的有效方法和一种新的临床途径。此外,检测血浆PAF-AH基因的多态性和酶活性异常将有助于炎症性疾病的诊断。

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