首页> 美国卫生研究院文献>Cell Regulation >Intercellular transport of lysosomal acid lipase mediates lipoprotein cholesteryl ester metabolism in a human vascular endothelial cell-fibroblast coculture system.
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Intercellular transport of lysosomal acid lipase mediates lipoprotein cholesteryl ester metabolism in a human vascular endothelial cell-fibroblast coculture system.

机译:溶酶体酸性脂肪酶的细胞间转运介导人血管内皮细胞-成纤维细胞共培养系统中的脂蛋白胆固醇酯代谢。

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摘要

We present results from studies of human cell culture models to support the premise that the extracellular transport of lysosomal acid lipase has a function in lipoprotein cholesteryl ester metabolism in vascular tissue. Vascular endothelial cells secreted a higher fraction of cellular acid lipase than did smooth muscle cells and fibroblasts. Acid lipase and lysosomal beta-hexosaminidase were secreted at approximately the same rate from the apical and basolateral surface of an endothelial cell monolayer. Stimulation of secretion with NH4Cl did not affect the polarity. We tested for the ability of secreted endothelial lipase to interact with connective tissue cells and influence lipoprotein cholesterol metabolism in a coculture system in which endothelial cells on a micropore filter were suspended above a monolayer of acid lipase-deficient (Wolman disease) fibroblasts. After 5-7 d, acid lipase activity in the fibroblasts reached 10%-20% of the level in normal cells; cholesteryl esters that had accumulated from growth in serum were cleared. Addition of mannose 6-phosphate to the coculture medium blocked acid lipase uptake and cholesterol clearance, indicating that lipase released from endothelial cells was packaged into fibroblast lysosomes by a phosphomannosyl receptor-mediated pathway. Supplementation of the coculture medium with serum was not required for lipase uptake and cholesteryl ester hydrolysis by the fibroblasts, but was necessary for cholesterol clearance. Results from our coculture model suggest that acid lipase may be transported from intact endothelium to cells in the lumen or the wall of a blood vessel. We postulate that delivery of acid hydrolases and lipoproteins to a common endocytic compartment may occur and have an impact on cellular lipoprotein processing.
机译:我们目前从人类细胞培养模型的研究结果来支持溶酶体酸性脂肪酶的细胞外运输在血管组织中的脂蛋白胆固醇酯代谢中具有功能。与平滑肌细胞和成纤维细胞相比,血管内皮细胞分泌更高比例的细胞酸性脂肪酶。酸性脂肪酶和溶酶体β-己糖胺酶以大约相同的速率从内皮细胞单层的顶表面和基底外侧表面分泌。用NH 4 Cl刺激分泌不影响极性。我们在共培养系统中测试了分泌的内皮脂肪酶与结缔组织细胞相互作用并影响脂蛋白胆固醇代谢的能力,该共培养系统中微孔滤膜上的内皮细胞悬浮在单层酸性脂肪酶缺陷(沃尔曼病)成纤维细胞上方。 5-7天后,成纤维细胞中的酸性脂肪酶活性达到正常细胞水平的10%-20%。清除了由于血清生长而积累的胆固醇酯。向共培养基中添加6-磷酸甘露糖可阻止酸性脂肪酶的摄取和胆固醇清除,这表明从内皮细胞释放的脂肪酶是通过磷酸甘露糖基受体介导的途径包装到成纤维细胞溶酶体中的。脂肪酶摄取和成纤维细胞水解胆固醇酯不需要补充血清的共培养基,但对于清除胆固醇是必需的。我们的共培养模型的结果表明,酸性脂肪酶可能​​从完整的内皮运输到管腔或血管壁中的细胞。我们假设可能发生酸性水解酶和脂蛋白向常见的内吞区室的传递,并影响细胞脂蛋白的加工。

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