Introduction: Focal segmental glomerulosclerosis (FSGS) is a histopathologically defined kidney lesion. FSGS can be observed with various underlying causes, including highly penetrant monogenic renal disease. We recently identified pathogenic variants of , a gene encoding the tubular protein uromodulin, in 8 families with suspected glomerular disease.
Methods: To validate pathogenic variants of , we reviewed the clinical and pathology reports of members of 8 families identified to have variants of . Clinical, laboratory, and pathologic data were collected, and genetic confirmation for was performed by Sanger sequencing.
Results: Biopsy-proven cases of FSGS were verified in 21% (7 of 34) of patients with variants. The variants seen in 7 families were mutations previously reported in autosomal dominant tubulointerstitial kidney disease-uromodulin (ADTKD-UMOD). For one family with 3 generations affected, we identified p.R79G in a noncanonical transcript variant of co-segregating with disease. Consistent with ADTKD, most patients in our study presented with autosomal dominant inheritance, subnephrotic range proteinuria, minimal hematuria, and renal impairment. Kidney biopsies showed histologic features of glomerular injury consistent with secondary FSGS, including focal sclerosis and partial podocyte foot process effacement.
Conclusion: Our study demonstrates that with the use of standard clinical testing and kidney biopsy, clinicians were unable to make the diagnosis of ADTKD-UMOD; patients were often labeled with a clinical diagnosis of FSGS. We show that genetic testing can establish the diagnosis of ADTKD-UMOD with secondary FSGS. Genetic testing in individuals with FSGS histology should not be limited to genes that directly impair podocyte function.
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| http://dx.doi.org/10.1016/j.ekir.2019.12.016 | DOI Listing |
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