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巨膜蛋白在视黄醇跨上皮转运中起关键作用的证据。

Evidence for an essential role of megalin in transepithelial transport of retinol.

作者信息

Christensen E I, Moskaug J O, Vorum H, Jacobsen C, Gundersen T E, Nykjaer A, Blomhoff R, Willnow T E, Moestrup S K

机构信息

Department of Cell Biology, Institute of Anatomy, University of Aarhus, Denmark.

出版信息

J Am Soc Nephrol. 1999 Apr;10(4):685-95. doi: 10.1681/ASN.V104685.

Abstract

Transepithelial transport of retinol is linked to retinol-binding protein (RBP), which is taken up and also synthesized in a number of epithelia. By immunocytochemistry of human, rat, and mouse renal proximal tubules, a strong staining in apical endocytic vacuoles, lysosomes, endoplasmic reticulum, Golgi, and basal vesicles was observed, in accordance with luminal endocytic uptake as well as a constitutive synthesis and basal secretion of RBP. Analysis of mice with target disruption of the gene for the major endocytic receptor of proximal tubules, megalin, revealed no RBP in proximal tubules of these mice. Western blotting and HPLC of the urine of the megalin-deficient mice instead revealed a highly increased urinary excretion of RBP and retinol, demonstrating that glomerular filtered RBP-retinol of megalin-deficient mice escapes uptake by proximal tubules. A direct megalin-mediated uptake of purified RBP-retinol was indicated by surface plasmon resonance analysis and uptake in immortalized rat yolk sac cells. Uptake was partially inhibited by a polyclonal megalin antibody and the receptor-associated protein. The present data show that the absence of RBP-binding megalin causes a significantly increased loss of RBP and retinol in the urine, demonstrating a crucial role of megalin in vitamin A homeostasis.

摘要

视黄醇的跨上皮转运与视黄醇结合蛋白(RBP)相关,RBP在多种上皮细胞中被摄取并合成。通过对人、大鼠和小鼠肾近端小管进行免疫细胞化学分析,观察到顶端内吞泡、溶酶体、内质网、高尔基体和基底小泡中有强烈染色,这与管腔的内吞摄取以及RBP的组成型合成和基底分泌情况相符。对近端小管主要内吞受体巨蛋白基因发生靶向破坏的小鼠进行分析发现,这些小鼠的近端小管中没有RBP。相反,对巨蛋白缺陷小鼠的尿液进行蛋白质印迹分析和高效液相色谱分析发现,RBP和视黄醇的尿排泄量大幅增加,这表明巨蛋白缺陷小鼠经肾小球滤过的RBP - 视黄醇无法被近端小管摄取。表面等离子体共振分析以及在永生化大鼠卵黄囊细胞中的摄取实验表明存在巨蛋白介导的对纯化RBP - 视黄醇的直接摄取。摄取过程部分受到多克隆巨蛋白抗体和受体相关蛋白的抑制。目前的数据表明,缺乏与RBP结合的巨蛋白会导致尿液中RBP和视黄醇的损失显著增加,这证明了巨蛋白在维生素A稳态中起着关键作用。

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