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支链磷脂酰胆碱通过增强胆固醇结合、膜整合和蛋白质交换来刺激磷脂囊泡中细胞色素P450SCC(CYP11A1)的活性。

Branched phosphatidylcholines stimulate activity of cytochrome P450SCC (CYP11A1) in phospholipid vesicles by enhancing cholesterol binding, membrane incorporation, and protein exchange.

作者信息

Kisselev P, Wessel R, Pisch S, Bornscheuer U, Schmid R D, Schwarz D

机构信息

Institute of Clinical Pharmacology, Charite-Humboldt University of Berlin, Berlin/Max Delbrueck Centrum for Molecular Medicine, Berlin-Buch, Germany.

出版信息

J Biol Chem. 1998 Jan 16;273(3):1380-6. doi: 10.1074/jbc.273.3.1380.

Abstract

Phosphatidylcholines (PCs) with branched fatty acyl chains substituted in the two positions of the main chains (branched PCs) have been shown to be potent activators of the side chain cleavage activity of cytochrome P450SCC (CYP11A1) (Schwarz, D., Kisselev, P., Wessel, R., Jueptner, O., and Schmid, R. D. (1996) J. Biol. Chem. 271, 12840-12846). The present study reports on the effect of a series of branched PC on cholesterol binding, membrane integration, and protein exchange in large unilamellar vesicles prepared by an extrusion technique. Enzyme kinetics using vesicles as well as optical titration using a micelle system with the detergent Tween 20 demonstrate that activation is correlated with the fraction of P450SCC in the high spin form. The potency of branched PCs both to activate the enzyme and to induce spin state changes increases with increasing lengths of both the branched and main fatty acyl chains. We found that the extent as well as the rate of integration of P450SCC into vesicle membranes studied by gel chromatography and stopped flow kinetics were increased by branched PC. Finally, it is demonstrated by measurement of the enzymatic activity in primary and secondary vesicles that branched PCs are potent in retaining a very rapid exchange of P450SCC between vesicles, in contrast to cardiolipin, that partially inhibits this exchange process. The data suggest that different properties of P450SCC in membrane systems including cholesterol binding, membrane integration, and protein exchange are affected by branched PCs and probably by other phospholipids, too, and therefore must be considered in an explanation of the observed high stimulation of activity.

摘要

在主链两个位置被支链脂肪酰链取代的磷脂酰胆碱(PCs,即支链PCs)已被证明是细胞色素P450SCC(CYP11A1)侧链裂解活性的有效激活剂(施瓦茨,D.,基斯列夫,P.,韦塞尔,R.,尤普特纳,O.,以及施密德,R.D.(1996年)《生物化学杂志》271卷,第12840 - 12846页)。本研究报告了一系列支链PC对通过挤压技术制备的大单层囊泡中胆固醇结合、膜整合及蛋白质交换的影响。使用囊泡的酶动力学以及使用含有去污剂吐温20的胶束系统的光学滴定表明,激活作用与高自旋形式的P450SCC的比例相关。支链PC激活酶以及诱导自旋状态变化的能力随着支链和主脂肪酰链长度的增加而增强。我们发现,通过凝胶色谱和停流动力学研究,支链PC增加了P450SCC整合到囊泡膜中的程度和速率。最后,通过测量初级和次级囊泡中的酶活性表明,与部分抑制这种交换过程的心磷脂相反,支链PC在保持P450SCC在囊泡之间非常快速的交换方面很有效。数据表明,膜系统中P450SCC的不同特性,包括胆固醇结合、膜整合和蛋白质交换,受到支链PC的影响,可能也受到其他磷脂的影响,因此在解释观察到的高活性刺激时必须予以考虑。

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