Investigation of coenzyme Q biosynthesis in human fibroblast and HepG2 cells

Michael Tekle , Mikael Turunen , Gustav Dallner , Tadeusz Chojnacki , Ewa Swiezewska
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引用次数: 7

Abstract

Coenzyme Q (CoQ) deficiency occurs in genetic disorders, during aging and various diseases. Diagnosis requires skin fibroblasts in tissue culture. [3H]Mevalonate incorporation was appropriate to measure the rate of CoQ synthesis in fibroblasts and hepatoblastoma cells. [14C]p-Hydroxybenzoate had limited permeability, but it could be increased with Fugene and cyclodextrin. Inhibition of decaprenyl-4-hydroxybenzoate transferase results in the accumulation of decaprenyl diphosphate, an indicator of enzyme deficiency. Also, analysis of the corresponding mRNAs in this case is useful. In vitro assays to measure trans-prenyltransferase and decaprenyl-4-hydroxybenzoate transferase activities are not available. Neither measurement of methyltransferases is reliable in human cells. In vitro reconstruction of CoQ synthesis, in opposite to cholesterol synthesis, proved to be unsuccessful. Thus, the biochemical characterization of the CoQ biosynthetic system in human cells is restricted to a few reliable analytical procedures.

人成纤维细胞和HepG2细胞中辅酶Q生物合成的研究
辅酶Q (CoQ)缺乏发生在遗传疾病、衰老和各种疾病中。诊断需要组织培养的皮肤成纤维细胞。[3H]甲羟戊酸掺入可用于测定成纤维细胞和肝母细胞瘤细胞中CoQ的合成率。[14C]对羟基苯甲酸酯的渗透性有限,但氟金和环糊精可以增加渗透性。抑制十戊烯基-4-羟基苯甲酸转移酶导致二磷酸十戊烯基积累,这是酶缺乏的一个指标。此外,在这种情况下,分析相应的mrna是有用的。体外测定反式戊烯基转移酶和癸戊烯基-4-羟基苯甲酸转移酶活性的方法是不可用的。在人类细胞中,两种甲基转移酶的测定方法都不可靠。体外重建CoQ合成,与胆固醇合成相反,被证明是不成功的。因此,人类细胞中CoQ生物合成系统的生化表征仅限于一些可靠的分析方法。
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