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甲羟戊酸激酶的生化及遗传学方面及其缺乏症

Biochemical and genetic aspects of mevalonate kinase and its deficiency.

作者信息

Houten S M, Wanders R J, Waterham H R

机构信息

Department of Pediatrics, Emma Children's Hospital, Academic Medical Center, University of Amsterdam, P.O. Box 22700, 1100 DE, Amsterdam, The Netherlands.

出版信息

Biochim Biophys Acta. 2000 Dec 15;1529(1-3):19-32. doi: 10.1016/s1388-1981(00)00135-9.

Abstract

Mevalonate kinase (MK) is an essential enzyme in the mevalonate pathway which produces numerous cellular isoprenoids. The enzyme has been characterized both at the biochemical and the molecular level in a variety of organisms. Despite the fact that mevalonate kinase is not the rate-limiting enzyme in isoprenoid biosynthesis, its activity is subject to feedback regulation by the branch-point intermediates geranyldiphosphate, farnesyldiphosphate and geranylgeranyldiphosphate. Recently, the importance of mevalonate kinase was demonstrated by the identification of its deficiency as the biochemical and molecular cause of the inherited human disorders mevalonic aciduria and hyperimmunoglobulinemia D and periodic fever syndrome. The pathophysiology of these disorders is not yet understood, but eventually will give insight into the in vivo role of mevalonate kinase and isoprenoid biosynthesis with respect to the acute phase response and fever. The subcellular localization of mevalonate kinase is still a matter of debate. The enzyme could be localized predominantly in the cytosol, or in peroxisomes, or it is associated differentially with peroxisomes. Here we review the biochemical and molecular properties of MK, and discuss its biological significance, the regulation of its enzyme activity and finally its subcellular localization.

摘要

甲羟戊酸激酶(MK)是甲羟戊酸途径中的一种关键酶,该途径可产生多种细胞类异戊二烯。在多种生物体中,已经在生化和分子水平上对该酶进行了表征。尽管甲羟戊酸激酶不是类异戊二烯生物合成中的限速酶,但其活性受到分支点中间体香叶基二磷酸、法尼基二磷酸和香叶基香叶基二磷酸的反馈调节。最近,通过鉴定其缺乏是遗传性人类疾病甲羟戊酸尿症、高免疫球蛋白血症D和周期性发热综合征的生化和分子原因,证明了甲羟戊酸激酶的重要性。这些疾病的病理生理学尚未完全了解,但最终将有助于深入了解甲羟戊酸激酶和类异戊二烯生物合成在急性期反应和发热方面的体内作用。甲羟戊酸激酶的亚细胞定位仍然存在争议。该酶可能主要定位于细胞质中,或过氧化物酶体中,或者它与过氧化物酶体存在差异关联。在此,我们综述了MK的生化和分子特性,并讨论了其生物学意义、酶活性的调节以及最终的亚细胞定位。

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