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Merck
CN

N-wasp is required for stabilization of podocyte foot processes.

Journal of the American Society of Nephrology : JASN (2013-03-09)
Christoph Schell, Lisa Baumhakl, Sarah Salou, Ann-Christin Conzelmann, Charlotte Meyer, Martin Helmstädter, Christoph Wrede, Florian Grahammer, Stefan Eimer, Dontscho Kerjaschki, Gerd Walz, Scott Snapper, Tobias B Huber
摘要

Alteration of cortical actin structures is the common final pathway leading to podocyte foot process effacement and proteinuria. The molecular mechanisms that safeguard podocyte foot process architecture and maintain the three-dimensional actin network remain elusive. Here, we demonstrate that neuronal Wiskott-Aldrich syndrome protein (N-WASP), which promotes actin nucleation, is required to stabilize podocyte foot processes. Mice lacking N-WASP specifically in podocytes were born with normal kidney function but developed significant proteinuria 3 weeks after birth, suggesting an important role for N-WASP in maintaining foot processes. In addition, inducing deletion of N-WASP in adult mice resulted in severe proteinuria and kidney failure. Electron microscopy showed an accumulation of electron-dense patches of actin and strikingly altered morphology of podocyte foot processes. Although basic actin-based processes such as cell migration were not affected, primary cultures of N-WASP-deficient podocytes revealed significant impairment of dynamic actin reorganization events, including the formation of circular dorsal ruffles. Taken together, our findings suggest that N-WASP-mediated actin nucleation of branched microfilament networks is specifically required for the maintenance of foot processes, presumably sustaining the mechanical resistance of the filtration barrier.

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抗-ARP2抗体,小鼠单克隆, clone FMS96, purified from hybridoma cell culture