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胰腺胆固醇酯酶的胆固醇转运功能:肠细胞中定向甾醇摄取与酯化

Cholesterol transport function of pancreatic cholesterol esterase: directed sterol uptake and esterification in enterocytes.

作者信息

Lopez-Candales A, Bosner M S, Spilburg C A, Lange L G

机构信息

CV Therapeutics, California 94043.

出版信息

Biochemistry. 1993 Nov 16;32(45):12085-9. doi: 10.1021/bi00096a019.

Abstract

We have recently hypothesized that neutral lipids can, in part, move across biological membranes via a mechanism involving enzymes anchored to membrane proteoglycans such as those found in the brush border of the enterocyte [Bosner, M. S., Gulick, T., Riley, D. J. S., Spilburg, C. A., & Lange, L. G. (1988) Proc. Natl. Acad. Sci. U.S.A. 85, 7438-7442]. Present results now show a subsequent, essential protein-mediated sorting of neutral lipids for further intracellular metabolism. Thus, in the absence of enzyme, 0.002 pmol of cellular ester appeared after 2 h, and its level increased only 3.5-fold after 12 h. However, in the presence of cholesterol esterase, the level of cholesterol ester increased 39-fold in the same time period, indicating that the enzyme-mediated uptake accounts for 10-fold greater ester synthesis than that from basal absorption. Kinetic analysis reveals that both enzyme-mediated and background absorption depend on taurocholate concentration and are second-order reactions more likely dependent on collision than diffusion. Other lipid-recognizing proteins such as pancreatic triglyceride lipase and the intestinal fatty acid binding protein are not stimulatory to intracellular cholesterol processing. Taken together, these data suggest that pancreatic cholesterol esterase and possibly other proteoglycan-binding extracellular enzymes of neutral lipid metabolism may facilitate movement of neutral lipids into the plasma membrane and direct them into functional intracellular sites.

摘要

我们最近推测,中性脂质可以部分地通过一种机制穿过生物膜,该机制涉及锚定在膜蛋白聚糖上的酶,如在肠上皮细胞刷状缘中发现的那些酶[博斯纳,M. S.,古利克,T.,莱利,D. J. S.,斯皮尔伯格,C. A.,& 兰格,L. G.(1988年)《美国国家科学院院刊》85,7438 - 7442]。目前的结果表明,随后存在一种由蛋白质介导的中性脂质分选过程,以进行进一步的细胞内代谢。因此,在没有酶的情况下,2小时后出现了0.002皮摩尔的细胞酯,12小时后其水平仅增加了3.5倍。然而,在胆固醇酯酶存在的情况下,胆固醇酯水平在同一时间段内增加了39倍,这表明酶介导的摄取导致的酯合成比基础吸收多10倍。动力学分析表明,酶介导的摄取和背景吸收都取决于牛磺胆酸盐浓度,并且是二级反应,更可能依赖于碰撞而非扩散。其他脂质识别蛋白,如胰脂肪酶和肠脂肪酸结合蛋白,对细胞内胆固醇加工没有刺激作用。综上所述,这些数据表明,胰胆固醇酯酶以及中性脂质代谢中可能的其他与蛋白聚糖结合的细胞外酶,可能促进中性脂质进入质膜并将它们导向细胞内的功能位点。

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