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肾小球上皮细胞通过受体介导摄取肾病患者的中间密度脂蛋白(IDL)和低密度脂蛋白(LDL)。

Receptor-mediated uptake of IDL and LDL from nephrotic patients by glomerular epithelial cells.

作者信息

Krämer A, Nauck M, Pavenstädt H, Schwedler S, Wieland H, Schollmeyer P, Wanner C

机构信息

Department of Medicine, University of Freiburg, Germany.

出版信息

Kidney Int. 1993 Dec;44(6):1341-51. doi: 10.1038/ki.1993.387.

Abstract

Although hyperlipidemia is a well-recognized complication of the nephrotic syndrome, the precise interaction of human glomerular cells and human lipoproteins, abnormal in lipid and protein composition, has not been clearly defined. This study examines receptor mediated binding, internalization and degradation as well as intracellular cholesterol metabolism of apoB-100 containing LDL and apoB,E containing IDL, isolated from patients with the nephrotic syndrome (N = 6), in human glomerular epithelial cells and skin fibroblasts. In the patients, serum LDL cholesterol level was increased threefold and IDL elevenfold as compared to healthy subjects. IDL of nephrotic patients contained 72% more cholesterol than IDL of healthy controls. No difference in lipid/protein composition was found in the LDL density range. Therefore, nephrotic and control LDL showed identical affinities for receptor mediated binding, internalization and degradation. Furthermore, inhibition of intracellular sterol synthesis and cholesteryl ester formation after incubation with LDL was comparable. In contrast, cholesterol-rich IDL of nephrotic patients was taken up by glomerular epithelial cells with higher affinity than LDL and control IDL, as well as intracellular sterol synthesis was suppressed more effectively than by control IDL. The cholesterol esterification rate of IDL from patients was enhanced 3.5-fold as compared to control IDL. In comparison to fibroblasts, glomerular epithelial cells showed about 15% of the maximal capacity for LDL uptake, but 31% for IDL from nephrotic patients. The data indicate that hypercholesterolemia of nephrotic origin cannot be explained by reduced ligand binding for LDL. ApoE containing IDL, which accumulate in nephrotic patients, were avidly taken up by glomerular epithelial cells via receptor dependent pathway. These lipoproteins could therefore play the predominant role in glomerular lipid accumulation and development of glomerulosclerosis.

摘要

虽然高脂血症是肾病综合征公认的并发症,但人类肾小球细胞与脂质和蛋白质组成异常的人类脂蛋白之间的确切相互作用尚未明确界定。本研究检测了从肾病综合征患者(N = 6)分离出的含载脂蛋白B-100的低密度脂蛋白(LDL)和含载脂蛋白B、E的中间密度脂蛋白(IDL)在人肾小球上皮细胞和皮肤成纤维细胞中的受体介导结合、内化和降解以及细胞内胆固醇代谢。与健康受试者相比,患者血清LDL胆固醇水平增加了两倍,IDL增加了十倍。肾病患者的IDL所含胆固醇比健康对照者的IDL多72%。在LDL密度范围内未发现脂质/蛋白质组成有差异。因此,肾病患者和对照者的LDL在受体介导的结合、内化和降解方面表现出相同的亲和力。此外,与LDL孵育后细胞内固醇合成和胆固醇酯形成的抑制作用相当。相比之下,肾病患者富含胆固醇的IDL被肾小球上皮细胞摄取的亲和力高于LDL和对照IDL,并且细胞内固醇合成的抑制作用比对照IDL更有效。患者IDL的胆固醇酯化率比对照IDL提高了3.5倍。与成纤维细胞相比,肾小球上皮细胞对LDL摄取的最大能力约为15%,但对肾病患者IDL的摄取能力为31%。数据表明,肾病源性高胆固醇血症不能用LDL配体结合减少来解释。肾病患者体内蓄积的含载脂蛋白E的IDL通过受体依赖途径被肾小球上皮细胞 avidly摄取。因此,这些脂蛋白可能在肾小球脂质蓄积和肾小球硬化的发展中起主要作用。

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