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Expanding the genetic spectrum of the pyruvate carboxylase deficiency with novel missense, deep intronic and structural variants

Title:	Expanding the genetic spectrum of the pyruvate carboxylase deficiency with novel missense, deep intronic and structural variants
Authors:	Polina Tsygankova; Igor Bychkov; Marina Minzhenkova; Natalia Pechatnikova; Lyudmila Bessonova; Galina Buyanova; Irina Naumchik; Nikita Beskorovainiy; Vyacheslav Tabakov; Yulia Itkis; Nadezhda Shilova; Ekaterina Zakharova
Source:	Molecular Genetics and Metabolism Reports, Vol 32, Iss , Pp 100889- (2022)
Publisher Information:	Elsevier
Publication Year:	2022
Collection:	Directory of Open Access Journals: DOAJ Articles
Subject Terms:	Pyruvate carboxylase deficiency; Reciprocal translocations; Deep intronic variants; WES; WGS; Medicine (General); R5-920; Biology (General); QH301-705.5
Description:	Introduction: Pathogenic variants in the pyruvate carboxylase (PC) gene cause a wide spectrum of recessive phenotypes, ranging from the early-onset fatal encephalopathy to the adult-onset benign form. Results: Patient 1 is a 6 y.o. boy with ataxia, hypoglycemia and episodes of lactic acidosis. WGS revealed the novel heterozygous missense variant c.1372A > G (p.Asn458Asp) in the PC gene. Additional analysis revealed discordant reads mapped to chromosomes 11 and 1, so a reciprocal translocation disrupted the PC gene was suspected. The translocation was validated via FISH-analysis and Sanger sequencing of its boundaries.Patient 2 is a 13 y.o. girl with psychomotor delay, episodes of lactic acidosis and ketonuria. WES revealed the novel homozygous intronic variant c.1983-116C > T. The PC's mRNA analysis demonstrated the exonization of several intron 16 sequences and some residual amount of WT mRNA isoform.Two other patients had more severe course of the disease. Their genotype represents missense variants in compound heterozygous and homozygous state (c.1876C > T (p.Arg626Trp), c.2606G > C (p.Gly869Ala), c.2435C > A (p.Ala812Asp). Conclusion: In patients with metabolic crises, lactic acidosis and hypoglycemia analysis of PC gene is recommended. WGS with deep bioinformatic analysis should be taken into consideration when none or the only one pathogenic variant in the PC gene is found.
Document Type:	article in journal/newspaper
Language:	English
ISBN:	978-2-214-42692-0; 2-214-42692-2
Relation:	http://www.sciencedirect.com/science/article/pii/S2214426922000490; https://doaj.org/toc/2214-4269; https://doaj.org/article/3b023d91c24c4a228d7b9d0076ffc9e3
DOI:	10.1016/j.ymgmr.2022.100889
Availability:	https://doi.org/10.1016/j.ymgmr.2022.100889; https://doaj.org/article/3b023d91c24c4a228d7b9d0076ffc9e3
Accession Number:	edsbas.9D49C137
Database:	BASE