胆固醇酯水解酶的调节。

D P Hajjar
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引用次数: 3

摘要

最近在了解CE水解酶的生化和分子性质及其对细胞胆固醇运输的影响方面的进展进一步明确了酶的作用机制。人类溶酶体酸性脂肪酶/CE水解酶和激素敏感脂肪酶cDNA探针的出现,使研究CE水解酶基因在人体组织中的调控和表达成为可能;现在可以更肯定地说,细胞质CE水解酶(NCEH)很可能是通过环amp依赖性蛋白激酶的磷酸化而激活的。证据还表明,NCEH很可能与激素敏感的脂肪酶相同,并且它在细胞的胆固醇外排特性中起重要作用。最近关于类二十烷/细胞因子网络在CE水解调控中的作用的研究进展(如图10所示)进一步强调了细胞中胆固醇运输过程有趣但复杂的本质,特别是在病理生理条件下,如细胞损伤、修复和炎症。可以推测,若干年后,当已知CE水解酶的晶体结构时,该酶的催化结构域的结构-功能特性,因为它与CE底物的物理状态有关,应该进一步阐明该酶在各种细胞条件下在细胞内胆固醇动员和运输中的确切作用。
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Regulation of cholesteryl ester hydrolases.

Recent developments in understanding the biochemical and molecular nature of the CE hydrolases and their impact on cellular cholesterol trafficking have further defined the enzyme's mechanism of action with reasonable clarity. The availability of the cDNA probe for the human lysosomal acid lipase/CE hydrolase and the hormone-sensitive lipase now makes it possible to study CE hydrolase gene regulation and expression in human tissue; and it can now be stated with more assurance that the cytoplasmic CE hydrolase (NCEH) is most likely activated through phosphorylation by the cyclic AMP-dependent protein kinase. Evidence also shows that the NCEH is most likely identical to the hormone-sensitive lipase and that it plays an important role in cholesterol efflux properties of the cell. Recent advances in the discovery of the role of the eicosanoid/cytokine network in the regulation of CE hydrolysis, highlighted in Figure 10, further emphasize the interesting but complex nature of the cholesterol trafficking processes in cells, particularly under pathophysiological conditions such as cell injury, repair, and inflammation. It can be speculated that in several years, when the crystal structure of the CE hydrolase is known, the structure-function properties of this enzyme's catalytic domain, as it relates to the physical state of the CE substrates, should further clarify the precise role of this enzyme in intracellular cholesterol mobilization and trafficking under a variety of cellular conditions.

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