足细胞中TRPC6离子通道的调节-对局灶节段性肾小球硬化和获得性蛋白尿疾病的影响

T. Szabó, L. Ambrus, N. Zákány, G. Balla, T. Bíró
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引用次数: 14

摘要

肾小球滤过屏障是一个高度特化的三层结构,具有独特的功能特性。足细胞功能障碍和细胞骨架紊乱导致横膈膜裂隙破裂和蛋白尿。涉及肾脏的炎症性疾病以及遗传性足细胞病或糖尿病肾病可引起足细胞网络的损伤。局灶节段性肾小球硬化(FSGS)是一种病理实体,是成人和儿童肾病综合征伴严重蛋白尿的常见原因。在FSGS的发病机制中已经发现了几个致病基因。瞬时受体电位-6 (TRPC6)是一种直接被二酰基甘油(DAG)激活的非选择性阳离子通道,它的突变会导致一种特别具有侵袭性的FSGS。血管紧张素II通过其AT1受体发挥作用,在包括FSGS在内的许多肾脏疾病中,在蛋白尿的产生和肾损伤的进展中起关键作用。越来越多的证据表明,TRPC6和其他TRPC通道在FSGS以及获得性蛋白尿(如糖尿病肾病或高血压)的发病机制中起着核心作用。鉴定TRPC6下游的信号通路可能为治疗蛋白尿和预防足细胞损伤的进展提供新的靶点。
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Regulation of TRPC6 ion channels in podocytes - Implications for focal segmental glomerulosclerosis and acquired forms of proteinuric diseases.
The glomerular filtration barrier is a highly specialized tri-layer structure with unique functional properties. Podocyte dysfunction and cytoskeletal disorganization leads to disruption of the slit diaphragma, and proteinuria. Inflammatory diseases involving the kidney as well as inherited podocytopathies or diabetic nephropathy cause injury of the podocyte network. Focal segmental glomerulosclerosis (FSGS) is a pathologic entity that is a common cause of nephrotic syndrome with severe proteinuria in both adults and children. Several causative genes have been identified in the pathogenesis of FSGS. Mutations of the transient receptor potential canonical-6 (TRPC6), a non-selective cation channel that is directly activated by diacylglycerol (DAG), cause a particularly aggressive form of FSGS. Angiotensin II, acting through its AT1 receptor, plays a critical role in generation of proteinuria and progression of kidney injury in a number of kidney diseases, including FSGS. Mounting evidence suggest the central role of TRPC6 and perhaps other TRPC channels in the pathogenesis of FSGS as well as of acquired forms of proteinuria such as diabetic nephropathy or hypertension. Identification of signaling pathways downstream of TRPC6 may provide novel targets for the treatment of proteinuria and prevent progression of podocyte injury.
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来源期刊
Acta physiologica Hungarica
Acta physiologica Hungarica 医学-生理学
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