Comprehensive Genetic Analysis Reveals Complexity of Monogenic Urinary Stone Disease

Cogal, Andrea G.; Arroyo, Jennifer; Shah, Ronak Jagdeep; Reese, Kalina J.; Walton, Brenna N.; Reynolds, Laura M.; Kennedy, Gabrielle N.; Seide, Barbara M.; Senum, Sarah R.; Baum, Michelle A.; Erickson, Stephen B.; Jagadeesh, Sujatha; Soliman, Neveen A.; Goldfarb, David S.; Beara-Lasić, Lada; Eðvarðsson, Viðar Örn; Pálsson, Runólfur; Milliner, Dawn S.; Sas, David J.; Lieske, John C.; Harris, Peter C.

doi:10.1016/j.ekir.2021.08.033

Cited by 20 publications

(14 citation statements)

References 95 publications

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“…Interestingly, identified molecular diagnoses pertained to only three distinct disorders: (a) cystinuria, (b) dRTA, and (c) renal phosphate wasting. Analogous to previous data on adult and adolescent cohorts, dominant genes predominated their recessive counterparts (Braun et al, 2016;Cogal et al, 2021;Halbritter et al, 2015). While in cystinuria both modes of inheritance were observed, we only found…”

Section: Discussionsupporting

confidence: 88%

“…However, the question of whom to subject to genetic testing is still unresolved. Most of the previous studies focused on childhood KSD (Braun et al, 2016; Cogal et al, 2021; Daga et al, 2018) and available prevalence data is difficult to interpret. A main limitation of most studies constitute their preselection of patients based on an upfront clinical suspicion of monogenic KSD (Cogal et al, 2021; Halbritter et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

“…Most of the previous studies focused on childhood KSD (Braun et al, 2016; Cogal et al, 2021; Daga et al, 2018) and available prevalence data is difficult to interpret. A main limitation of most studies constitute their preselection of patients based on an upfront clinical suspicion of monogenic KSD (Cogal et al, 2021; Halbritter et al, 2015). Lessons from the introduction of broad genetic testing in other medical fields, however, have taught us to expect genetic causes also in unsuspected clinical situations (Splinter et al, 2018; Sun et al, 2022).…”

Section: Introductionmentioning

confidence: 99%

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Systematic assessment of monogenic etiology in adult‐onset kidney stone formers undergoing urological intervention–evidence for genetic pretest probability

Schönauer

Scherer

Nemitz‐Kliemchen

et al. 2022

American J of Med Genetics Pt C

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Kidney stone disease (KSD) is a prevalent condition associated with high morbidity, frequent recurrence, and progression to chronic kidney disease (CKD). The etiology is multifactorial, depending on environmental and genetic factors. Although monogenic KSD is frequent in children, unbiased prevalence data of heritable forms in adults is scarce. Within 2 years of recruitment, all patients hospitalized for urological kidney stone intervention at our center were consecutively enrolled for targeted next generation sequencing (tNGS). Additionally, clinical and metabolic assessments were performed for genotype-phenotype analyses. The cohort comprised 155 (66%) males and 81 (34%) females, with a mean age at first stone of 47 years (4-86). The diagnostic yield of tNGS was 6.8% (16/236), with cystinuria (SLC3A1, SLC7A9), distal renal tubular acidosis (SLC4A1), and renal phosphate wasting (SLC34A1, SLC9A3R1) as underlying hereditary disorders. While metabolic syndrome traits were associated with late-onset KSD, hereditary KSD was associated with increased disease severity in terms of early-onset, frequent recurrence, mildly impaired kidney function, and common bilateral affection. By employing systematic genetic analysis to a less biased cohort of common adult kidney stone formers, we demonstrate its diagnostic value for establishing the underlying disorder in a distinct proportion. Factors determining pretest probability include age at first stone (<40 years), frequent recurrence, mild CKD, and bilateral KSD.

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Section: Discussionsupporting

confidence: 88%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Systematic assessment of monogenic etiology in adult‐onset kidney stone formers undergoing urological intervention–evidence for genetic pretest probability

Schönauer

Scherer

Nemitz‐Kliemchen

et al. 2022

American J of Med Genetics Pt C

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“…Others identified that diagnosable phenocopy disorders may be more common, representing up to one in five genetic diagnoses in suspected hereditary kidney disease and that an approach rigidly applying very strictly targeted gene panels rather than broader or cascade panels does not identify such instances [ 30 ▪ ]. For complex phenotypes such as urinary stone disease, the evidence for broadened gene panels is further reflecting this concept that application of a very targeted gene panel approach will fail to identify a genetic diagnosis that is present and directly related to the patient phenotype in 10–20% of instances [ 31 ].…”

Section: New Indications For Genomic Testingmentioning

confidence: 99%

Which patients with CKD will benefit from genomic sequencing? Synthesizing progress to illuminate the future

Mallett

2022

Current Opinion in Nephrology &Amp; Hypertension

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Purpose of reviewThis review will summarize and synthesize recent findings in regard to monogenic kidney disorders, including how that evidence is being translated into practice. It will add to existing key knowledge to provide context for clinicians in consolidating existing practice and approaches.Recent findingsWhilst there are long established factors, which indicate increased likelihood of identifying a monogenic cause for kidney disease, these can now be framed in terms of the identification of new genes, new indications for genomic testing and new evidence for clinical utility of genomic testing in nephrology. Further, inherent in the use of genomics in nephrology are key concepts including robust informed consent, variant interpretation and return of results. Recent findings of variants in genes related to complex or broader kidney phenotypes are emerging in addition to understanding of de novo variants. Phenocopy phenomena are indicating a more pragmatic use of broader gene panels whilst evidence is emerging of a role in unexplained kidney disease. Clinical utility is evolving but is being successfully demonstrated across multiple domains of outcome and practice.SummaryWe provide an updated framework of evidence to guide application of genomic testing in chronic kidney disease (CKD), building upon existing principles and knowledge to indicate how the practice and implementation of this can be applied today. There are clearly established roles for genomic testing for some patients with CKD, largely those with suspected heritable forms, with these continuing to expand as new evidence emerges.

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“…Twenty-three patients were referred for molecular diagnosis to the Laboratory of histomorphology and molecular biology of the kidney (Italy) and 12 were referred to the Rare Kidney Stone Consortium (RKSC) in the USA. Sanger sequencing was used to determine and verify the pathogenic variants in OCRL in our cohort [16]. OCRL variants were classified as pathogenic or likely pathogenic according to American College of Medical Genetics and American College of Pathologists (ACMG/AMP) guidelines [17].…”

Section: Subjectsmentioning

confidence: 99%

Genotype Phenotype Correlation in Dent Disease 2 and Review of the Literature: OCRL Gene Pleiotropism or Extreme Phenotypic Variability of Lowe Syndrome?

Gianesello

Arroyo

Prete

et al. 2021

Genes

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Dent disease is a rare X-linked renal tubulopathy due to CLCN5 and OCRL (DD2) mutations. OCRL mutations also cause Lowe syndrome (LS) involving the eyes, brain and kidney. DD2 is frequently described as a mild form of LS because some patients may present with extra-renal symptoms (ESs). Since DD2 is a rare disease and there are a low number of reported cases, it is still unclear whether it has a clinical picture distinct from LS. We retrospectively analyzed the phenotype and genotype of our cohort of 35 DD2 males and reviewed all published DD2 cases. We analyzed the distribution of mutations along the OCRL gene and evaluated the type and frequency of ES according to the type of mutation and localization in OCRL protein domains. The frequency of patients with at least one ES was 39%. Muscle findings are the most common ES (52%), while ocular findings are less common (11%). Analysis of the distribution of mutations revealed (1) truncating mutations map in the PH and linker domain, while missense mutations map in the 5-phosphatase domain, and only occasionally in the ASH-RhoGAP module; (2) five OCRL mutations cause both DD2 and LS phenotypes; (3) codon 318 is a DD2 mutational hot spot; (4) a correlation was found between the presence of ES and the position of the mutations along OCRL domains. DD2 is distinct from LS. The mutation site and the mutation type largely determine the DD2 phenotype.

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Comprehensive Genetic Analysis Reveals Complexity of Monogenic Urinary Stone Disease

Cited by 20 publications

References 95 publications

Systematic assessment of monogenic etiology in adult‐onset kidney stone formers undergoing urological intervention–evidence for genetic pretest probability

Systematic assessment of monogenic etiology in adult‐onset kidney stone formers undergoing urological intervention–evidence for genetic pretest probability

Which patients with CKD will benefit from genomic sequencing? Synthesizing progress to illuminate the future

Genotype Phenotype Correlation in Dent Disease 2 and Review of the Literature: OCRL Gene Pleiotropism or Extreme Phenotypic Variability of Lowe Syndrome?

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