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胆固醇对微粒体动力学和尿苷二磷酸葡萄糖醛酸基转移酶动力学的依赖性修饰。

Cholesterol-dependent modification of microsomal dynamics and UDPglucuronyltransferase kinetics.

作者信息

Castuma C E, Brenner R R

出版信息

Biochemistry. 1986 Aug 26;25(17):4733-8. doi: 10.1021/bi00365a002.

Abstract

The effect of both in vitro incorporation and removal of cholesterol in guinea pig liver microsomes on the lipid composition, dynamic properties of the membrane, and kinetic constants of UDPglucuronyltransferase was studied. No significant changes either in the fatty acid composition or in the distribution of phospholipid classes were observed upon cholesterol incorporation and removal. Lateral and rotational mobility measured by the efficiency of pyrene excimer formation and fluorescence of 1,6-diphenylhexatriene decreased with cholesterol incorporation and increased in parallel to cholesterol removal. These changes were associated with alterations in the kinetic properties of UDPglucuronyltransferase. Whereas Vmax increased, the Km of the different steps of the reaction decreased with cholesterol incorporation. The negative homotropic effect and apparent cooperativity of UDP-glucuronic acid decreased when cholesterol was incorporated and increased after cholesterol removal. Moreover, the UDP-N-acetylglucosamine-dependent activation of the enzyme decreased in correlation with an increase of cholesterol concentration in microsomes. It has been demonstrated that both the shift of the non-Michaelian kinetics of the enzyme to Michaelian and the decrease of the UDP-N-acetylglucosamine-dependent activation of the enzyme are evoked by a change of the physical state of the UDPglucuronyltransferase milieu from a gel phase to a liquid-crystalline phase. Therefore, we must admit that cholesterol incorporation in the microsomes while producing an increased packing of the bulk lipids would also cause the separation of more fluid phospholipids, which increase the proportion of molecules in the liquid-crystalline state within the enzyme environment.

摘要

研究了豚鼠肝微粒体中胆固醇的体外掺入和去除对脂质组成、膜的动态特性以及UDP-葡萄糖醛酸基转移酶动力学常数的影响。在胆固醇掺入和去除过程中,未观察到脂肪酸组成或磷脂类分布有显著变化。通过芘激基缔合物形成效率和1,6-二苯基己三烯荧光测量的横向和旋转流动性随胆固醇掺入而降低,随胆固醇去除而平行增加。这些变化与UDP-葡萄糖醛酸基转移酶的动力学性质改变有关。随着胆固醇掺入,Vmax增加,反应不同步骤的Km降低。当胆固醇掺入时,UDP-葡萄糖醛酸的负同促效应和表观协同性降低,胆固醇去除后增加。此外,酶的UDP-N-乙酰葡糖胺依赖性激活与微粒体中胆固醇浓度的增加相关而降低。已经证明,酶的非米氏动力学向米氏动力学的转变以及酶的UDP-N-乙酰葡糖胺依赖性激活的降低是由UDP-葡萄糖醛酸基转移酶环境的物理状态从凝胶相变为液晶相引起的。因此,我们必须承认,微粒体中胆固醇的掺入虽然会使大量脂质的堆积增加,但也会导致更多流动性较强的磷脂分离,从而增加酶环境中处于液晶态的分子比例。

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