Clinical and Genetic Characterization of Patients with Bartter and Gitelman Syndrome

Palazzo, Viviana; Raglianti, Valentina; Landini, Samuela; Cirillo, Luigi; Errichiello, Carmela; Buti, Elisa; Artuso, Rosangela; Tiberi, Lucia; Vergani, Debora; Romagnani, Paola; Mazzinghi, Benedetta; Becherucci, Francesca

doi:10.3390/ijms23105641

Cited by 5 publications

(5 citation statements)

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“…These authors also detected CKD ≥ stage 2 in 5/12 patients (41.7%) with a molecular diagnosis of BS type 1, while smaller percentage of 2/12 (16.7%), 1/12 (8.3%), and 4/12 (33.3%) showed causative variants in genes responsible for BS types 3, 4a, and GS, respectively. However, there is no mention about the type of the variants in each group [45]. In this Brazilian cohort, we were able to demonstrate that the presence of homozygous 1–20 del in CLCNKB was related to CKD progression characterized by decreasing in eGFR, changing in CKD status and higher proteinuria levels.…”

Section: Discussionmentioning

confidence: 66%

“…Furthermore, unexpectedly, we identified a novel likely pathogenic variant in SLC12A3 diagnosing GS in two siblings with antenatal/neonatal disease onset. Early GS manifestation has been rarely reported in literature [44, 45]; however, to the best of our knowledge, an antenatal clinical picture is described for the 1st time in this current Brazilian cohort.…”

Section: Discussionmentioning

confidence: 68%

“…Studies on the CKD progression of these patients have been scarce in the literature. CKD stages 2-5 have been reported in patients with BS with extremely variable rates (0-27%), but some studies did not perform genetic testing confirmation or did not include BS type 3 patients [45]. Palazzo et al [45], by studying BS and GS patients, reported a significantly higher frequency of CKD ≥stage 2 (defined as eGFR <90 mL/min/1.73 m 2 ) in patients with BS than in those affected by GS.…”

Section: Discussionmentioning

confidence: 99%

“…CKD stages 2–5 have been reported in patients with BS with extremely variable rates (0–27%), but some studies did not perform genetic testing confirmation or did not include BS type 3 patients [45]. Palazzo et al [45], by studying BS and GS patients, reported a significantly higher frequency of CKD ≥stage 2 (defined as eGFR <90 mL/min/1.73 m 2 ) in patients with BS than in those affected by GS. These authors also detected CKD ≥ stage 2 in 5/12 patients (41.7%) with a molecular diagnosis of BS type 1, while smaller percentage of 2/12 (16.7%), 1/12 (8.3%), and 4/12 (33.3%) showed causative variants in genes responsible for BS types 3, 4a, and GS, respectively.…”

Section: Discussionmentioning

confidence: 99%

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Bartter Syndrome-Related Variants Distribution: Brazilian Data and Its Comparison with Worldwide Cohorts

Vaisbich

Messa

Rangel-Santos

et al. 2023

Nephron

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Background: Genetic testing is recommended for accurate diagnosis of Bartter syndrome (BS) and serves as a basis for implementing specific target therapies. However, populations other than Europeans and North Americans are underrepresented in most databases and there are uncertainties in the genotype-phenotype correlation. We studied Brazilian BS patients, an admixed population with diverse ancestry. Methods: We evaluated the clinical and mutational profile of this cohort and performed a systematic review of BS mutations from worldwide cohorts. Results: Twenty-two patients were included; Gitelman syndrome was diagnosed in 2 siblings with antenatal BS and congenital chloride diarrhea in 1 girl. BS was confirmed in 19 patients: BS type 1 in 1 boy (antenatal BS); BS type 4a in 1 girl and BS type 4b in 1 girl, both of them with antenatal BS and neurosensorial deafness; BS type 3 (CLCNKB mutations): 16 cases. The deletion of the entire CLCNKB (1–20 del) was the most frequent variant. Patients carrying the 1–20 del presented earlier manifestations than those with other CLCNKB-mutations and the presence of homozygous 1–20 del was correlated with progressive chronic kidney disease. The prevalence of the 1–20 del in this BS Brazilian cohort was similar to that of Chinese cohorts and individuals of African and Middle Eastern descent from other cohorts. Conclusion: This study expands the genetic spectrum of BS patients with different ethnics, reveals some genotype/phenotype correlations, compares the findings with other cohorts, and provides a systematic review of the literature on the distribution of BS-related variants worldwide.

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Section: Discussionmentioning

confidence: 66%

Section: Discussionmentioning

confidence: 68%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Bartter Syndrome-Related Variants Distribution: Brazilian Data and Its Comparison with Worldwide Cohorts

Vaisbich

Messa

Rangel-Santos

et al. 2023

Nephron

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“…Selection criteria were usually stringent and phenotype-centered. 15,[19][20][21][22][23][24][25][26][27] However, genetic testing can provide diagnostic certainty also in less well-defined settings such as in advanced CKD where biopsy is usually no longer performed or only reveals nonspecific features of kidney atrophy (CKD of unknown origin [CKDu]). 3,28 Recently, testing with WES in a large cross-section cohort of unselected patients with kidney diseases across all age groups showed an overall diagnostic yield of approximately 10%, 29 questioning cost-effectiveness for health care systems and hence a broader implementation into daily clinical practice in unselected cohorts of patients.…”

Section: Introductionmentioning

confidence: 99%

A Clinical Workflow for Cost-Saving High-Rate Diagnosis of Genetic Kidney Diseases

Becherucci

Landini

Palazzo

et al. 2023

JASN

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Significance Statement To optimize the diagnosis of genetic kidney disorders in a cost-effective manner, we developed a workflow based on referral criteria for in-person evaluation at a tertiary center, whole-exome sequencing, reverse phenotyping, and multidisciplinary board analysis. This workflow reached a diagnostic rate of 67%, with 48% confirming and 19% modifying the suspected clinical diagnosis. We obtained a genetic diagnosis in 64% of children and 70% of adults. A modeled cost analysis demonstrated that early genetic testing saves 20% of costs per patient. Real cost analysis on a representative sample of 66 patients demonstrated an actual cost reduction of 41%. This workflow demonstrates feasibility, performance, and economic effect for the diagnosis of genetic kidney diseases in a real-world setting. Background Whole-exome sequencing (WES) increases the diagnostic rate of genetic kidney disorders, but accessibility, interpretation of results, and costs limit use in daily practice. Methods Univariable analysis of a historical cohort of 392 patients who underwent WES for kidney diseases showed that resistance to treatments, familial history of kidney disease, extrarenal involvement, congenital abnormalities of the kidney and urinary tract and CKD stage ≥G2, two or more cysts per kidney on ultrasound, persistent hyperechoic kidneys or nephrocalcinosis on ultrasound, and persistent metabolic abnormalities were most predictive for genetic diagnosis. We prospectively applied these criteria to select patients in a network of nephrology centers, followed by centralized genetic diagnosis by WES, reverse phenotyping, and multidisciplinary board discussion. Results We applied this multistep workflow to 476 patients with eight clinical categories (podocytopathies, collagenopathies, CKD of unknown origin, tubulopathies, ciliopathies, congenital anomalies of the kidney and urinary tract, syndromic CKD, metabolic kidney disorders), obtaining genetic diagnosis for 319 of 476 patients (67.0%) (95% in 21 patients with disease onset during the fetal period or at birth, 64% in 298 pediatric patients, and 70% in 156 adult patients). The suspected clinical diagnosis was confirmed in 48% of the 476 patients and modified in 19%. A modeled cost analysis showed that application of this workflow saved 20% of costs per patient when performed at the beginning of the diagnostic process. Real cost analysis of 66 patients randomly selected from all categories showed actual cost reduction of 41%. Conclusions A diagnostic workflow for genetic kidney diseases that includes WES is cost-saving, especially if implemented early, and is feasible in a real-world setting. Podcast This article contains a podcast at https://dts.podtrac.com/redirect.mp3/www.asn-online.org/media/podcast/JASN/2023_04_03_JASN2022060725.mp3

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40 años de experiencia en síndrome de Bartter

García Espinosa,

Zarauza Santoveña,

Bravo Feito

et al. 2023

Nefrología

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Clinical and Genetic Characterization of Patients with Bartter and Gitelman Syndrome

Cited by 5 publications

References 46 publications

Bartter Syndrome-Related Variants Distribution: Brazilian Data and Its Comparison with Worldwide Cohorts

Bartter Syndrome-Related Variants Distribution: Brazilian Data and Its Comparison with Worldwide Cohorts

A Clinical Workflow for Cost-Saving High-Rate Diagnosis of Genetic Kidney Diseases

40 años de experiencia en síndrome de Bartter

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