Whole-Exome Sequencing in Adults With Chronic Kidney Disease

Sneh Lata(Columbia University), Maddalena Marasà(Columbia University), Yifu Li(Columbia University), David Fasel(Columbia University), Emily Groopman(Columbia University), Vaidehi Jobanputra(Columbia University), Hila Milo Rasouly(Columbia University), Adele Mitrotti(Columbia University), Rik Westland(Columbia University), Miguel Verbitsky(Columbia University), Jordan G. Nestor(Columbia University), Lindsey M. Slater, Vivette D. D’Agati(Columbia University), Marcin Zaniew, Anna Materna‐Kiryluk(Poznan University of Medical Sciences), Francesca Lugani(Istituto Giannina Gaslini), Gianluca Caridi(Istituto Giannina Gaslini), Luca Rampoldi(Istituti di Ricovero e Cura a Carattere Scientifico), Aditya Mattoo(New York University), Chad A. Newton(The University of Texas Southwestern Medical Center), Maya K. Rao(Columbia University), Jai Radhakrishnan(Columbia University), Wooin Ahn(Columbia University), Pietro A. Canetta(Columbia University), Andrew S. Bomback(Columbia University), Gerald B. Appel(Columbia University), Corinne Antignac(Sorbonne Paris Cité), Glen S. Markowitz(Columbia University), Christine Kim Garcia(The University of Texas Southwestern Medical Center), Krzysztof Kiryluk(Columbia University), Simone Sanna‐Cherchi(Columbia University), Ali G. Gharavi(Columbia University)
Annals of Internal Medicine
January 16, 2018
10.7326/m17-1319
Cited by 205

Abstract

Background: The utility of whole-exome sequencing (WES) for the diagnosis and management of adult-onset constitutional disorders has not been adequately studied. Genetic diagnostics may be advantageous in adults with chronic kidney disease (CKD), in whom the cause of kidney failure often remains unknown. Objective: To study the diagnostic utility of WES in a selected referral population of adults with CKD. Design: Observational cohort. Setting: A major academic medical center. Patients: 92 adults with CKD of unknown cause or familial nephropathy or hypertension. Measurements: The diagnostic yield of WES and its potential effect on clinical management. Results: Whole-exome sequencing provided a diagnosis in 22 of 92 patients (24%), including 9 probands with CKD of unknown cause and encompassing 13 distinct genetic disorders. Among these, loss-of-function mutations were identified in PARN in 2 probands with tubulointerstitial fibrosis. PARN mutations have been implicated in a short telomere syndrome characterized by lung, bone marrow, and liver fibrosis; these findings extend the phenotype of PARN mutations to renal fibrosis. In addition, review of the American College of Medical Genetics actionable genes identified a pathogenic BRCA2 mutation in a proband who was diagnosed with breast cancer on follow-up. The results affected clinical management in most identified cases, including initiation of targeted surveillance, familial screening to guide donor selection for transplantation, and changes in therapy. Limitation: The small sample size and recruitment at a tertiary care academic center limit generalizability of findings among the broader CKD population. Conclusion: Whole-exome sequencing identified diagnostic mutations in a substantial number of adults with CKD of many causes. Further study of the utility of WES in the evaluation and care of patients with CKD in additional settings is warranted. Primary Funding Source: New York State Empire Clinical Research Investigator Program, Renal Research Institute, and National Human Genome Research Institute of the National Institutes of Health.

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