Mouse genetics reveals Barttin as a genetic modifier of Joubert syndrome

Author:

Ramsbottom Simon A.ORCID,Thelwall Peter E.,Wood Katrina M.,Clowry Gavin J.,Devlin Laura A.,Silbermann Flora,Spiewak Helena L.ORCID,Shril Shirlee,Molinari Elisa,Hildebrandt Friedhelm,Gunay-Aygun Meral,Saunier Sophie,Cordell Heather J.,Sayer John A.ORCID,Miles Colin G.

Abstract

Genetic and phenotypic heterogeneity and the lack of sufficiently large patient cohorts pose a significant challenge to understanding genetic associations in rare disease. Here we identify Bsnd (alias Barttin) as a genetic modifier of cystic kidney disease in Joubert syndrome, using a Cep290-deficient mouse model to recapitulate the phenotypic variability observed in patients by mixing genetic backgrounds in a controlled manner and performing genome-wide analysis of these mice. Experimental down-regulation of Bsnd in the parental mouse strain phenocopied the severe cystic kidney phenotype. A common polymorphism within human BSND significantly associates with kidney disease severity in a patient cohort with CEP290 mutations. The striking phenotypic modifications we describe are a timely reminder of the value of mouse models and highlight the significant contribution of genetic background. Furthermore, if appropriately managed, this can be exploited as a powerful tool to elucidate mechanisms underlying human disease heterogeneity.

Funder

RCUK | Medical Research Council

Kidney Research UK

Northern Counties Kidney Research UK

HHS | NIH | NIH Clinical Center

Fondation pour la Recherche Médicale

Agence Nationale de la Recherche

Rosetrees Trust

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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