Bigenic mouse models of focal segmental glomerulosclerosis involving pairwise interaction of CD2AP, Fyn, and synaptopodin
Tobias B. Huber, … , Peter Mundel, Andrey S. Shaw
Tobias B. Huber, … , Peter Mundel, Andrey S. Shaw
Published May 1, 2006
Citation Information: J Clin Invest. 2006;116(5):1337-1345. https://doi.org/10.1172/JCI27400.
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Research Article Nephrology

Bigenic mouse models of focal segmental glomerulosclerosis involving pairwise interaction of CD2AP, Fyn, and synaptopodin

Abstract

Focal segmental glomerulosclerosis (FSGS) is the most common primary glomerular diagnosis resulting in end-stage renal disease. Defects in several podocyte proteins have been implicated in the etiology of FSGS, including podocin, α-actinin–4, CD2-associated protein (CD2AP), and TRPC6. Despite our growing understanding of genes involved in the pathogenesis of focal segmental sclerosis, the vast majority of patients with this disease, even those with a familial linkage, lack a clear genetic diagnosis. Here, we tested whether combinations of genetic heterozygosity (bigenic heterozygosity) that alone do not result in clinical kidney disease could function together to enhance susceptibility to glomerular damage and FSGS. Combinations of Cd2ap heterozygosity and heterozygosity of either synaptopodin (Synpo) or Fyn proto-oncogene (Fyn) but not kin of IRRE like 1 (Neph1) resulted in spontaneous proteinuria and in FSGS-like glomerular damage. These genetic interactions were also reflected at a functional level, as we found that CD2AP associates with Fyn and Synpo but not with Neph1. This demonstrates that bigenic heterozygosity can lead to FSGS and suggests that combined mutations in 2 or multiple podocyte genes may be a common etiology for glomerular disease.

Authors

Tobias B. Huber, Christopher Kwoh, Hui Wu, Katsuhiko Asanuma, Markus Gödel, Björn Hartleben, Ken J. Blumer, Jeffrey H. Miner, Peter Mundel, Andrey S. Shaw

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Figure 5

CD2AP forms an endogenous complex with Fyn and Synpo.

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CD2AP forms an endogenous complex with Fyn and Synpo. (A) Endogenous CD2...
(A) Endogenous CD2AP interacts with endogenous Fyn in cells (upper panel) and rat glomeruli (lower panel). Lysates were prepared from HEK 293 cells or isolated rat glomeruli, respectively (input lysate, 25 μl out of 800 ml; lane 1). Immunoprecipitates were prepared with a control antibody (rabbit serum, lane 2) or with polyclonal antisera to Fyn (lane 3). Immunoblotting was performed with a polyclonal antibody to CD2AP. (B) Endogenous CD2AP interacts with endogenous Synpo in podocytes. Lysates were prepared from differentiated podocytes. Immunoprecipitates were prepared with a control antibody and anti-Synpo (upper panel) or anti-CD2AP (lower panel) antibodies and immunoblotted with anti-Synpo or anti-CD2AP.