首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Biliary proteins. Unique inhibitors of cholesterol crystal nucleation in human gallbladder bile.
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Biliary proteins. Unique inhibitors of cholesterol crystal nucleation in human gallbladder bile.

机译:胆汁蛋白质。人胆囊胆汁中胆固醇晶体成核的独特抑制剂。

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摘要

The onset time for cholesterol crystal nucleation of supersaturated normal human gallbladder biles is consistently prolonged when compared with biles from patients with cholesterol gallstone disease. Investigation of the factor(s) responsible for the suspended supersaturation (metastability) of normal human biles revealed that model bile solutions of cholesterol saturation index (CSI) and molar lipid composition identical to individual gallbladder bile specimens had much shorter crystal nucleation times, i.e., exhibited decreased metastability. Unsaturated normal biles, after supplementation with lecithin, cholesterol, and sodium taurocholate to a 'standard' supersaturated lipid composition, also demonstrated nucleation times three- to 15-fold longer than the comparable standard model bile. Total lipid extracts of normal biles, however, when similarly supplemented, did not differ in nucleation time from the control model solution. Gallbladder biles were fractionated by gel chromatography and the eluted fractions were pooled into two fractions. The fractions eluting in about the first 25% of the included volume when mixed with the supersaturated standard model bile induced a modest increase in nucleation time of approximately 1.5 times the control value. The fractions eluting in the second 25% of the included volume and which contained all of the bile lipids, were concentrated and supplemented with lipids to the standard composition. The nucleation times of these supplements were 3-10 times longer than the control nucleation times. Delipidated bile protein mixtures, purified by discontinuous sucrose gradient centrifugation, were recombined with purified lipids at the standard composition used previously. The nucleation times of these mixtures were significantly prolonged to the same extent as those associated with the second chromatographic fraction. These observations demonstrate that the delayed onset (inhibition) of cholesterol crystal nucleation observed in normal human gallbladder bile is produced by a factor(s) present in the biliary protein fraction.
机译:与胆固醇胆结石病患者的胆汁相比,超饱和正常人胆囊胆汁中胆固醇晶体成核的开始时间持续延长。对导致正常人胆汁悬浮过饱和(转移性)的因素进行调查后发现,与单个胆囊胆汁样品相同的胆固醇饱和指数(CSI)和摩尔脂质组成的模型胆汁溶液具有短得多的晶体成核时间,即表现出降低的亚稳态。在向“标准”过饱和脂质成分中添加卵磷脂,胆固醇和牛磺胆酸钠后,不饱和正常胆汁的成核时间也比同等标准模型胆汁长3至15倍。然而,当正常补充胆汁的总脂质提取物时,其与对照模型溶液的成核时间没有差异。通过凝胶色谱法分离胆囊胆汁,并将洗脱的级分合并为两个级分。当与过饱和的标准模型胆汁混合时,洗脱在所含体积的大约前25%的馏分会引起成核时间的适度增加,约为对照值的1.5倍。浓缩包含体积的后25%且包含所有胆汁脂质的级分,并在脂质中添加标准组合物。这些补充剂的成核时间比对照成核时间长3-10倍。通过不连续蔗糖梯度离心纯化的去脂胆汁蛋白质混合物与纯化的脂质以先前使用的标准组合物重组。这些混合物的成核时间与与第二色谱级分相关的成核时间显着延长。这些观察结果表明,在正常人胆囊胆汁中观察到的胆固醇晶体成核的延迟发作(抑制)是由胆汁蛋白级分中存在的一种或多种因子产生的。

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