LAMA2 and LOXL4 are candidate FSGS genes.

Poornima VijayanSaidah HackTony YaoMohammad Azfar QureshiAndrew D PatersonRohan JohnBernard DavenportRachel LennonYork PeiMoumita Barua

Published in: BMC nephrology (2021)

Based on our findings, we postulate that the additive effect of digenic inheritance of heterozygous variants in LAMA2 and LOXL4 leads to adult-onset FSGS. Limitations to our study includes the absence of functional characterization to support pathogenicity. Alternatively, identification of additional FSGS cases with suspected deleterious variants in LAMA2 and LOXL4 will provide more evidence for disease causality. Thus, our report will be of benefit to the renal community as sequencing in renal disease becomes more widespread.

Keyphrases

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