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首页> 外文期刊>Journal of biological inorganic chemistry: JBIC: a publication of the Society of Biological Inorganic Chemistry >EGCG decreases binding of calcium oxalate monohydrate crystals onto renal tubular cells via decreased surface expression of alpha-enolase
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EGCG decreases binding of calcium oxalate monohydrate crystals onto renal tubular cells via decreased surface expression of alpha-enolase

机译:EGCG通过降低α-烯醇酶的表面表达来降低草酸钙一水合物晶体与肾小管细胞的结合

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摘要

Crystal retention on tubular cell surface inside renal tubules is considered as the earliest and crucial step for kidney stone formation. Therapeutics targeting this step would cease the development of kidney stone. This study thus aimed to investigate the potential role of epigallocatechin-3-gallate (EGCG), a major antioxidant found in green tea leaves, in the reduction of calcium oxalate monohydrate (COM) crystal binding onto renal tubular cells. Pretreatment of the cells with EGCG for up to 6 h significantly diminished crystal-binding capability in a dose-dependent manner. Indirect immunofluorescence assay without and with cell permeabilization followed by laser-scanning confocal microscopy revealed that EGCG significantly reduced surface expression of alpha-enolase, whereas its intracellular level was increased. Western blot analysis confirmed such contradictory changes in membrane and cytosolic fractions of EGCG-treated cells, whereas the total level in whole cell lysate remained unchanged. Moreover, overexpression of surface alpha-enolase and enhancement of cell-crystal adhesion induced by 10 mM sodium oxalate were completely abolished by EGCG. Taken together, these data indicate that EGCG decreases binding of COM crystals onto renal tubular cells by decreasing the surface expression of alpha-enolase via re-localization or inhibition of alpha-enolase shuttling from the cytoplasm to the plasma membrane. These findings may also explain the effects of EGCG in reducing COM crystal deposition in previous animal models of kidney stone disease. Thus, EGCG may be useful for the prevention of new or recurrent stone formation.
机译:肾小管内肾小管细胞表面的晶体保留被认为是肾结石形成的最早且至关重要的步骤。针对这一步骤的治疗药物将停止肾结石的发展。因此,本研究旨在研究表没食子儿茶素-3-没食子酸酯(EGCG)(一种绿茶中发现的主要抗氧化剂)在减少草酸钙一水合物(COM)晶体与肾小管细胞结合方面的潜在作用。用EGCG预处理细胞长达6小时,以剂量依赖性方式大大降低了晶体结合能力。间接免疫荧光测定在不进行细胞透化和细胞透化的情况下进行,然后进行激光扫描共聚焦显微镜检查,结果表明,EGCG显着降低了α-烯醇化酶的表面表达,而其细胞内水平却升高了。 Western印迹分析证实,EGCG处理的细胞的膜和胞质部分存在这种矛盾的变化,而全细胞裂解液的总水平保持不变。此外,EGCG完全消除了表面α-烯醇酶的过表达和10 mM草酸钠诱导的细胞晶体粘附的增强。综上所述,这些数据表明,EGCG通过重新定位或抑制从细胞质到质膜穿梭的α-烯醇酶来降低α-烯醇酶的表面表达,从而降低了COM晶体与肾小管细胞的结合。这些发现也可以解释在先前的肾结石动物模型中EGCG减少COM晶体沉积的作用。因此,EGCG可用于预防新的或复发性结石形成。

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