Biallelic PKP2 loss of function variants are associated with a lethal perinatal-onset biventricular dilated cardiomyopathy with excessive trabeculations and ventricular septal defects

Gibb, Jack ✉; Wall, Elizabeth*; Fields, Ella; Seale, Anna; Armstrong, Catherine; Bamber, Andrew; Daubeney, Piers; Jacobs-Pearson, Makaela; Marton, Tamas [Marton, Tamás (Perinatális patol...), szerző] Szülészeti és Nőgyógyászati Klinika Baross utca... (SE / AOK / K / SZSZNK); Stals, Karen; Low, Karen; Kaski, Juan Pablo; Spentzou, Georgia

Angol nyelvű Szakcikk (Folyóiratcikk) Tudományos

Megjelent: JOURNAL OF MEDICAL GENETICS 0022-2593 1468-6244 61 (4) pp. 405-409 2024

SJR Scopus - Genetics (clinical): Q1

Azonosítók

MTMT: 34428271
DOI: 10.1136/jmg-2023-109493
WoS: 001111133100001
Scopus: 85178576802
PubMed: 38050058

Homozygous plakophilin-2 ( PKP2 ) variants have been identified as a cause of a lethal form of dilated cardiomyopathy with excessive trabeculations (DCM-ET) in three cases. We report three more cases from two families with homozygous pathogenic PKP2 variants and perinatal-onset, lethal DCM-ET. Identification of the genetic abnormalities played a key role in decision-making and family counselling in these cases. This case series supports the published evidence that biallelic loss of function PKP2 variants cause a lethal, perinatal-onset cardiomyopathy.

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Biallelic PKP2 loss of function variants are associated with a lethal perinatal-onset biventricular dilated cardiomyopathy with excessive trabeculations and ventricular septal defects

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