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Published in: Clinical and Experimental Nephrology 3/2020

Open Access 01-03-2020 | Invited review article

New insight into podocyte slit diaphragm, a therapeutic target of proteinuria

Authors: Hiroshi Kawachi, Yoshiyasu Fukusumi

Published in: Clinical and Experimental Nephrology | Issue 3/2020

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Abstract

Dysfunction of slit diaphragm, a cell–cell junction of glomerular podocytes, is involved in the development of proteinuria in several glomerular diseases. Slit diaphragm should be a target of a novel therapy for proteinuria. Nephrin, NEPH1, P-cadherin, FAT, and ephrin-B1 were reported to be extracellular components forming a molecular sieve of the slit diaphragm. Several cytoplasmic proteins such as ZO-1, podocin, CD2AP, MAGI proteins and Par-complex molecules were identified as scaffold proteins linking the slit diaphragm to the cytoskeleton. In this article, new insights into these molecules and the pathogenic roles of the dysfunction of these molecules were introduced. The slit diaphragm functions not only as a barrier but also as a signaling platform transfer the signal to the inside of the cell. For maintaining the slit diaphragm function properly, the phosphorylation level of nephrin is strictly regulated. The recent studies on the signaling pathway from nephrin, NEPH1, and ephrin-B1 were reviewed. Although the mechanism regulating the function of the slit diaphragm had remained unclear, recent studies revealed TRPC6 and angiotensin II-regulating mechanisms play a critical role in regulating the barrier function of the slit diaphragm. In this review, recent investigations on the regulation of the slit diaphragm function were reviewed, and a strategy for the establishment of a novel therapy for proteinuria was proposed.
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Metadata
Title
New insight into podocyte slit diaphragm, a therapeutic target of proteinuria
Authors
Hiroshi Kawachi
Yoshiyasu Fukusumi
Publication date
01-03-2020
Publisher
Springer Singapore
Published in
Clinical and Experimental Nephrology / Issue 3/2020
Print ISSN: 1342-1751
Electronic ISSN: 1437-7799
DOI
https://doi.org/10.1007/s10157-020-01854-3

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