Whole-exome sequencing as a diagnostic tool for distal renal tubular acidosis

Pereira, Paula Cristina Barros; Melo, Flávia Medeiros; De Marco, Luiz Armando Cunha; Oliveira, Eduardo Araújo; Miranda, Débora Marques; Silva, Ana Cristina Simões e

doi:10.1016/j.jped.2015.02.002

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Sumário

• J. Pediatr. (Rio J.) 91 (6) • Nov-Dec 2015 • https://doi.org/10.1016/j.jped.2015.02.002 copy

Whole-exome sequencing as a diagnostic tool for distal renal tubular acidosis^☆ ☆ Please cite this article as: Pereira PC, Melo FM, De Marco LA, Oliveira EA, Miranda DM, Simões e Silva AC. Whole-exome sequencing as a diagnostic tool for distal renal tubular acidosis. J Pediatr (Rio J). 2015;91:583-9.

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Objective

Distal renal tubular acidosis (dRTA) is characterized by metabolic acidosis due to impaired renal acid excretion. The aim of this study was to demonstrate the genetic diagnosis of four children with dRTA through use of whole-exome sequencing.

Methods

Two unrelated families were selected; a total of four children with dRTA and their parents, in order to perform whole-exome sequencing. Hearing was preserved in both children from the first family, but not in the second, wherein a twin pair had severe deafness. Whole-exome sequencing was performed in two pooled samples and findings were confirmed with Sanger sequencing method.

Results

Two mutations were identified in the ATP6V0A4 and ATP6V1B1 genes. In the first family, a novel mutation in the exon 13 of the ATP6V0A4 gene with a single nucleotide change GAC → TAC (c.1232G>T) was found, which caused a substitution of aspartic acid to tyrosine in position 411. In the second family, a homozygous recurrent mutation with one base-pair insertion (c.1149_1155insC) in exon 12 of the ATP6V1B1 gene was detected.

Conclusion

These results confirm the value of whole-exome sequencing for the study of rare and complex genetic nephropathies, allowing the identification of novel and recurrent mutations. Furthermore, for the first time the application of this molecular method in renal tubular diseases has been clearly demonstrated.

KEYWORDS
ATP6V0A4; ATP6V1B1; Children; Distal renal tubular acidosis; Genetics; Whole-exome sequencing

Findings/patients	II2 – Family 1	II3 – Family 1	II1 – Family 2	II2 – Family 2
Age	4 months	1 month	2 years	2 years
Sex	Female	Male	Female	Female
Deafness/SNHL	Absent	Absent	Present	Present
Birth weight (g)	Not available	3450	2340	2300
Weight (g)	3960	3760	8250	8300
WAZ	<−3	0	<−3	<−3
Height (cm)	54.5	50.0	73.5	74.0
HAZ	<−3	−2	<−3	<−3
Nephrocalcinosis	Present	Present	Absent	Absent
Initial manifestations	Failure to thrive, dehydration	Vomiting and dehydration	Rickets, failure to thrive, growth retardation	Rickets, failure to thrive, growth retardation
Serum creatinine (mg/dL)	0.4	1.7	0.5	0.5
Blood venous pH	7.36	7.16	7.23	7.12
Serum bicarbonate (mmol/L)	19.0	8.0	15.9	13.7
Serum potassium (mEq/L)	3.8	2.0	4.0	4.1
Serum chloride (mmol/L)	109	118	117	123
Urinary pH	7.5	7.1	7.0	7.0

Parameters	Family 1	Family 2
	Number of variants	Number of variants
Total variants	3993	6791
Intergenic, intronic, and UTR regions and synonymous mutations were excluded	1445	1912
Quality score <20 were excluded	879	1012
PhyloP <3 were excluded	131	215
Selection by function	15	14
PolyPhen <0.7 were excluded	10	6
Selection using cross-reference gene database and IGV	1	1
Candidate gene	1	1

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[1] * Corresponding author. E-mail: acssilva@hotmail.com (A.C. Simões e Silva).