Literature DB >> 26940091

Developmental Origins for Kidney Disease Due to Shroom3 Deficiency.

Hadiseh Khalili1, Alexandra Sull2, Sanjay Sarin1, Felix J Boivin1, Rami Halabi2, Bruno Svajger1, Aihua Li1, Valerie Wenche Cui1, Thomas Drysdale3, Darren Bridgewater4.   

Abstract

CKD is a significant health concern with an underlying genetic component. Multiple genome-wide association studies (GWASs) strongly associated CKD with the shroom family member 3 (SHROOM3) gene, which encodes an actin-associated protein important in epithelial morphogenesis. However, the role of SHROOM3 in kidney development and function is virtually unknown. Studies in zebrafish and rat showed that alterations in Shroom3 can result in glomerular dysfunction. Furthermore, human SHROOM3 variants can induce impaired kidney function in animal models. Here, we examined the temporal and spatial expression of Shroom3 in the mammalian kidney. We detected Shroom3 expression in the condensing mesenchyme, Bowman's capsule, and developing and mature podocytes in mice. Shroom3 null (Shroom3Gt/Gt) mice showed marked glomerular abnormalities, including cystic and collapsing/degenerating glomeruli, and marked disruptions in podocyte arrangement and morphology. These podocyte-specific abnormalities are associated with altered Rho-kinase/myosin II signaling and loss of apically distributed actin. Additionally, Shroom3 heterozygous (Shroom3Gt/+) mice showed developmental irregularities that manifested as adult-onset glomerulosclerosis and proteinuria. Taken together, our results establish the significance of Shroom3 in mammalian kidney development and progression of kidney disease. Specifically, Shroom3 maintains normal podocyte architecture in mice via modulation of the actomyosin network, which is essential for podocyte function. Furthermore, our findings strongly support the GWASs that suggest a role for SHROOM3 in human kidney disease.
Copyright © 2016 by the American Society of Nephrology.

Entities:  

Keywords:  Shroom3; chronic kidney disease; kidney development; kidney disease; podocyte

Mesh:

Substances:

Year:  2016        PMID: 26940091      PMCID: PMC5042660          DOI: 10.1681/ASN.2015060621

Source DB:  PubMed          Journal:  J Am Soc Nephrol        ISSN: 1046-6673            Impact factor:   10.121


  20 in total

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