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地塞米松对肝脏微粒体总脂质和磷脂酰胆碱分子种类脂肪酸组成的影响。

Effect of dexamethasone on the fatty acid composition of total liver microsomal lipids and phosphatidylcholine molecular species.

作者信息

Brenner R R, Ayala S, Garda H A

机构信息

Instituto de Investigaciones Bioquímicas de La Plata (INIBIOLP), CONICET-UNLP, Facultad de Ciencias Médicas, Argentina.

出版信息

Lipids. 2001 Dec;36(12):1337-45. doi: 10.1007/s11745-001-0850-1.

DOI:10.1007/s11745-001-0850-1
PMID:11834086
Abstract

Dexamethasone depresses delta6 and delta5 and increases delta9 desaturase and synthase activities. Therefore, we investigated the effect on the fatty acid composition of microsomal liver lipids and phosphatidylcholine (PtdCho) molecular species. After 15 d of treatment we found a notable decrease in arachidonic acid, a small decrease in stearic acid, and increases of linoleic, oleic, palmitoleic, and palmitic acids in liver microsomal total lipids and PtdCho. The study of the distribution of the PtdCho molecular species indicated that 18:0/20:4n-6, 16:0/20:4n-6, and 16:0/18:2n-6 predominated in the control animals. Dexamethasone, as expected because of its depressing effect on arachidonic acid synthesis and activation of oleic and palmitic acid synthesis, evoked a very significant decrease in 18:0/20:4n-6 PtdCho (P<0.001) and an important increase in 16:0/18:2n-6. The invariability of 16:0/20:4n-6 PtdCho could be related to the antagonistic effect of arachidonic and palmitic acid synthesis. PtdCho species containing oleic acid were not significant. The bulk fluidity and dynamic properties of the microsomal lipid bilayer measured by fluorometry using the probes 1,6-diphenyl-1,3,5-hexatriene and 4-trimethylammonium-phenyl-6-phenyl-1,3,5-hexatriene showed no significant modification, probably owing to a compensatory effect of the different molecular species, but changes of particular domains not detected by this technique are possible. However, the extremely sensitive Laurdan detected increased lipid packing in the less-fluid domains of the polar-nonpolar interphase of the bilayer, possibly evoked by the change of molecular species and cholesterol/phospholipid ratio. The most important effect found is the decrease of arachidonic acid pools in liver phospholipids as one of the corresponding causes of dexamethasone-dependent pharmacological effects.

摘要

地塞米松会抑制Δ6和Δ5去饱和酶,并增加Δ9去饱和酶和合成酶的活性。因此,我们研究了其对肝微粒体脂质和磷脂酰胆碱(PtdCho)分子种类脂肪酸组成的影响。治疗15天后,我们发现肝微粒体总脂质和PtdCho中的花生四烯酸显著减少,硬脂酸略有减少,而亚油酸、油酸、棕榈油酸和棕榈酸增加。对PtdCho分子种类分布的研究表明,18:0/20:4n-6、16:0/20:4n-6和16:0/18:2n-6在对照动物中占主导地位。由于地塞米松对花生四烯酸合成有抑制作用且能激活油酸和棕榈酸合成,正如预期的那样,它引起18:0/20:4n-6 PtdCho显著减少(P<0.001),而16:0/18:2n-6则显著增加。16:0/20:4n-6 PtdCho的不变性可能与花生四烯酸和棕榈酸合成的拮抗作用有关。含油酸的PtdCho种类不显著。使用探针1,6-二苯基-1,3,5-己三烯和4-三甲基铵-苯基-6-苯基-1,3,5-己三烯通过荧光法测量的微粒体脂质双层的整体流动性和动态特性没有显著改变,这可能是由于不同分子种类的补偿作用,但也有可能存在该技术未检测到的特定结构域的变化。然而,极其敏感的劳丹荧光染料检测到双层极性-非极性界面流动性较小区域的脂质堆积增加,这可能是由分子种类和胆固醇/磷脂比例的变化引起的。发现的最重要的影响是肝磷脂中花生四烯酸池的减少,这是地塞米松依赖性药理作用的相应原因之一。

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