Updated Genetic Testing of Italian Patients Referred with a Clinical Diagnosis of Primary Hyperoxaluria

Overview

Journal J Nephrol

Publisher Springer

Specialty Nephrology

Date 2016 Mar 7

PMID 26946417

Citations 7

Authors

Alessandra Pelle

Alessandra Cuccurullo

Cecilia Mancini

Regina Sebastiano

Giovanni Stallone

Susanna Negrisolo

Elisa Benetti

Licia Peruzzi

Michele Petrarulo

Mario De Marchi

Martino Marangella

Antonio Amoroso

Daniela Giachino

Giorgia Mandrile

Affiliations

Soon will be listed here.

Abstract

Background: Primary hyperoxaluria (PH) is a rare autosomal recessive disease commonly arising in childhood and presenting with nephrolithiasis, nephrocalcinosis and/or chronic renal failure. Three genes are currently known as responsible: alanine-glyoxylate aminotransferase (AGXT, PH type 1), glyoxylate reductase/hydroxypyruvate reductase (GRHPR, PH type 2), and 4-hydroxy-2-oxoglutarate aldolase (HOGA1, PH type 3). In our Centre, at the end of 2014 molecular diagnosis of PH1 had been performed in 80 patients, while one patient received a PH2 diagnosis.

Materials And Methods: Fifteen patients referred to our Centre and suspected to have PH on clinical grounds were negative for pathogenic variants in the entire coding sequence and exon-intron boundaries of the AGXT gene. Therefore, we extended the analysis to the AGXT promoter region and the GRHPR and HOGA1 genes.

Results: Two patients were heterozygous for two novel AGXT-promoter variants (c.-647C > T, c.-424C > T) that were probably non pathogenic. One patient was homozygous for a novel HOGA1 variant of intron 2 (c.341-81delT), whose pathogenicity predicted by in silico splicing tools was not confirmed by a minigene splicing assay in COS-7 and HEK293T cells.

Conclusion: New genetic subtypes of PH can be hypothesized in our patients, that may be caused by mutations in other gene encoding proteins of glyoxylate metabolism. Alternatively, some kind of mutations (e.g., deletions/duplications, deep intronic splicing regulatory variants) could be missed in a few cases, similarly to other genetic diseases.

Citing Articles

HOGA1 variants in Chinese patients with primary hyperoxaluria type 3: genetic features and genotype-phenotype relationships.

Ge Y, Liu Y, Zhan R, Zhao Z, Li J, Wang W World J Urol. 2023; 41(8):2141-2148.

PMID: 37318624 DOI: 10.1007/s00345-023-04461-5.

Primary hyperoxaluria in Italy: the past 30 years and the near future of a (not so) rare disease.

Mandrile G, Pelle A, Sciannameo V, Benetti E, DAlessandro M, Emma F J Nephrol. 2022; 35(3):841-850.

PMID: 35218550 PMC: 8995259. DOI: 10.1007/s40620-022-01258-4.

A novel nonsense variant of the AGXT identified in a Chinese family: special variant research in the Chinese reference genome.

Xu C, Zhou X, Xu H, Zhao Y, Zhao X, Liu D BMC Nephrol. 2021; 22(1):83.

PMID: 33691640 PMC: 7945658. DOI: 10.1186/s12882-021-02276-3.

Meeting report of the "Symposium on kidney stones and mineral metabolism: calcium kidney stones in 2017".

Pozdzik A, Maalouf N, Letavernier E, Brocheriou I, Body J, Vervaet B J Nephrol. 2019; 32(5):681-698.

PMID: 30680550 DOI: 10.1007/s40620-019-00587-1.

Updated Genetic Testing of Primary Hyperoxaluria Type 1 in a Chinese Population: Results from a Single Center Study and a Systematic Review.

Du D, Li Q, Chen C, Shi S, Zhao Y, Jiang J Curr Med Sci. 2018; 38(5):749-757.

PMID: 30341509 DOI: 10.1007/s11596-018-1941-y.

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