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准确分离胆汁脂质聚集体需要正确的混合胶束/囊泡间胆汁盐浓度。

Accurate separation of biliary lipid aggregates requires the correct intermixed micellar/intervesicular bile salt concentration.

作者信息

Donovan J M, Jackson A A

机构信息

Department of Medicine, Harvard Medical School, Boston, MA, USA.

出版信息

Hepatology. 1998 Mar;27(3):641-8. doi: 10.1002/hep.510270301.

Abstract

The intermixed micellar/intervesicular bile salt (BS) concentration (IMC), composed of BS monomers and simple micelles, is in dynamic equilibrium with mixed micelles and vesicles. Accurate separation of biliary lipid aggregates is believed to depend on accurately measuring the IMC. Using centrifugal ultrafiltration, we measured the IMC of cholesterol-supersaturated model biles that were physiologically composed. Gel chromatography was performed using eluants containing the following: 1) the IMC; 2) the same BS composition as the IMC but higher or lower BS concentrations; 3) the same BS concentration as the IMC, but with more hydrophilic or hydrophobic BS; and 4) 10 mmol/L cholate. Compared with an eluant containing the same BS composition as the IMC, an eluant containing the same relative BS composition but 75% of the IMC increased the proportion of cholesterol in vesicles and decreased the vesicular cholesterol/egg yolk phosphatidylcholine (EYPC) ratio. In contrast, an eluant containing 150% of the IMC entirely transformed vesicles to micelles. Eluants containing slightly more hydrophobic or more hydrophilic BS eliminated or increased vesicular cholesterol content, respectively. An eluant of 10 mmol/L cholate overestimated vesicular cholesterol and in concentrated biles reproducibly produced an incompletely separated intermediate peak, possibly because of re-equilibration between mixed micelles and vesicles. Further, in concentrated biles, fractions eluting at volumes corresponding to mixed micelles were visibly turbid, irrespective of the eluant used. The correct IMC allows accurate separation of biliary lipid aggregates, but differences in BS concentration or composition substantially alter the vesicular percentage of cholesterol as well as the cholesterol/EYPC ratio. Elution with 10 mmol/L cholate may introduce artifactual gel-filtration peaks and inadequate separation of particles with widely differing molecular weights, both of which have confused previous analyses of biliary lipid aggregates.

摘要

由胆盐单体和简单微胶粒组成的混合微胶粒/微泡间胆盐(BS)浓度(IMC)与混合微胶粒和微泡处于动态平衡。据信,胆汁脂质聚集体的准确分离取决于对IMC的精确测量。我们使用离心超滤法测量了生理组成的胆固醇过饱和模型胆汁的IMC。使用含有以下成分的洗脱液进行凝胶色谱分析:1)IMC;2)与IMC相同的胆盐组成,但胆盐浓度更高或更低;3)与IMC相同的胆盐浓度,但含有更多亲水性或疏水性胆盐;4)10 mmol/L胆酸盐。与含有与IMC相同胆盐组成的洗脱液相比,含有相同相对胆盐组成但为IMC 75%的洗脱液增加了微泡中胆固醇的比例,并降低了微泡胆固醇/蛋黄磷脂酰胆碱(EYPC)比率。相反,含有150% IMC的洗脱液将微泡完全转化为微胶粒。含有略多疏水性或更多亲水性胆盐的洗脱液分别消除或增加了微泡胆固醇含量。10 mmol/L胆酸盐的洗脱液高估了微泡胆固醇含量,并且在浓缩胆汁中可重复产生一个未完全分离的中间峰,这可能是由于混合微胶粒和微泡之间的重新平衡所致。此外,在浓缩胆汁中,对应于混合微胶粒体积洗脱的级分明显浑浊,与所使用的洗脱液无关。正确的IMC允许准确分离胆汁脂质聚集体,但胆盐浓度或组成的差异会显著改变胆固醇的微泡百分比以及胆固醇/EYPC比率。用10 mmol/L胆酸盐洗脱可能会引入人为的凝胶过滤峰,并且对分子量差异很大的颗粒分离不充分,这两者都使先前对胆汁脂质聚集体的分析产生了混淆。

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