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. 2017 May 24;292(29):12100–12110. doi: 10.1074/jbc.M117.775700

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© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.

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Figure 6. — Schematic overview of β-catenin regulation by PKCϵ in wild-type and PKCϵ^−/− podocytes. In wild-type podocytes, PKCϵ regulates cytoplasmic β-catenin level in balance with other PKC isoforms: PKCα phosphorylates β-catenin and, thus, leads to its degradation. PKCϵ inhibits degradation via its interaction sites (Ser-352, Thr-472/Ser-473, and Ser-663) in a GSK3β-independent manner and leads to a predominantly cytosolic localization of β-catenin, which then might bind to the actin-bundling protein fascin1 in filopodia of the podocytes or localize to the membrane, forming the cell adhesion complex with P-cadherin and α-catenin, resulting in a stabilized actin cytoskeleton and cell adhesion. In PKCϵ-deficient podocytes, this balance is disturbed, leading to degradation of β-catenin, abolished P-cadherin expression, and lower fascin1 expression, which then results in impaired cell adhesion and actin bundling and, thus, in a weakened actin cytoskeleton.