Past, present and future of genomics for kidney stone disease

Author:

Jahrreiss Victoria12,Özsoy Mehmet23,Seitz Christian12,Somani Bhaskar234

Affiliation:

1. Department of Urology, Comprehensive Cancer Center, Medical University of Vienna, Vienna, Austria

2. EAU Section on Urolithiasis (EULIS)

3. Uromed Competence Center for Urology, Vienna Austria

4. University Hospital Southampton NHS Trust, Southampton, UK

Abstract

Purpose of review To summarize the latest findings and developments in genomics for kidney stone disease (KSD) that help to understand hereditary pathomechanisms, identify high risk stone formers, provide early treatment and prevent recurrent kidney stone formation. Recent findings Several gene loci associated to KSD have presently been discovered in large Genome-wide association studies. Monogenic causes are rare, but are thought to have higher penetrance, while polygenic causes are more frequent with less penetrance. Although there is a great effort identifying genetic causes of KSD, targeted therapies are scarce. Summary There have been great advancements in genetic research in identifying genetic variants associated with KSD. Identifying these variants and understanding the underlying pathophysiology will not only provide individual risk assessment but open the way for new treatment targets and preventive care strategies.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Urology

Reference22 articles.

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2. Epidemiology of stone disease across the world;Sorokin;World J Urol,2017

3. Epidemiology of urolithiasis in Asia;Liu;Asian J Urol,2018

4. Genetic predisposition to formation of calcium oxalate renal calculi;Resnick;N Engl J Med,1968

5. Familial aggregation of renal calcium stone disease;Trinchieri;J Urol,1988

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