AI Article Synopsis
- About 40 genes are known to be linked to congenital anomalies of the kidney and urinary tract (CAKUT), which is a major cause of chronic kidney disease in children; however, these genes only explain 20% of cases.
- A study identified ARHGEF6 gene variants that could contribute to CAKUT by affecting cell signaling, particularly involving proteins that facilitate cell movement and adhesion.
- The research used exome sequencing on 1,265 families and found mutations in ARHGEF6 in some individuals, suggesting that defects in this gene can disrupt kidney development and result in CAKUT.*
Article Abstract
Background: About 40 disease genes have been described to date for isolated CAKUT, the most common cause of childhood CKD. However, these genes account for only 20% of cases. ARHGEF6, a guanine nucleotide exchange factor that is implicated in biologic processes such as cell migration and focal adhesion, acts downstream of integrin-linked kinase (ILK) and parvin proteins. A genetic variant of ILK that causes murine renal agenesis abrogates the interaction of ILK with a murine focal adhesion protein encoded by Parva , leading to CAKUT in mice with this variant.
Methods: To identify novel genes that, when mutated, result in CAKUT, we performed exome sequencing in an international cohort of 1265 families with CAKUT. We also assessed the effects in vitro of wild-type and mutant ARHGEF6 proteins, and the effects of Arhgef6 deficiency in mouse and frog models.
Results: We detected six different hemizygous variants in the gene ARHGEF6 (which is located on the X chromosome in humans) in eight individuals from six families with CAKUT. In kidney cells, overexpression of wild-type ARHGEF6 -but not proband-derived mutant ARHGEF6 -increased active levels of CDC42/RAC1, induced lamellipodia formation, and stimulated PARVA-dependent cell spreading. ARHGEF6-mutant proteins showed loss of interaction with PARVA. Three-dimensional Madin-Darby canine kidney cell cultures expressing ARHGEF6-mutant proteins exhibited reduced lumen formation and polarity defects. Arhgef6 deficiency in mouse and frog models recapitulated features of human CAKUT.
Conclusions: Deleterious variants in ARHGEF6 may cause dysregulation of integrin-parvin-RAC1/CDC42 signaling, thereby leading to X-linked CAKUT.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10103091 | PMC |
| http://dx.doi.org/10.1681/ASN.2022010050 | DOI Listing |
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