| Literature DB >> 34003581 |
Gregory Webster1, Meredith Reynolds2, Nicoleta C Arva2, Lisa M Dellefave-Castillo3, Hilary S McElligott4, Amber Kofman1, Aleksandra Laboski1, Defne Magnetta1, Alfred L George5, Elizabeth M McNally3, Megan J Puckelwartz3,5.
Abstract
Patients with biallelic mutations in the nuclear-encoded mitochondrial gene C1QBP/p32 have been described with syndromic features and autosomal recessive cardiomyopathy. We describe the clinical course in two siblings who developed cardiomyopathy and ventricular fibrillation in infancy. We provide genomic analysis and clinical-pathologic correlation. Both siblings had profound cardiac failure with ventricular arrhythmia. One child died suddenly. The second sibling survived resuscitation but required extracorporeal cardiopulmonary support and died shortly afterward. On cardiac autopsy, the left ventricle was hypertrophied in both children. Histological examination revealed prominent cardiomyocyte cytoplasmic clearing, and electron microscopy confirmed abnormal mitochondrial structure within cardiomyocytes. DNA sequencing revealed compound heterozygous variants in C1QBP (p.Thr40Asnfs*45 and p.Phe204Leu) in both children. Family segregation analysis demonstrated each variant was inherited from an unaffected, heterozygous parent. Inherited loss of C1QBP/p32 is associated with recessive cardiomyopathy, ventricular fibrillation, and sudden death in early life. Ultrastructural mitochondrial evaluation in the second child was similar to findings in engineered C1qbp-deficient mice. Rapid trio analysis can define rare biallelic variants in genes that may be implicated in sudden death and facilitate medical management and family planning. (184/200).Entities:
Keywords: C1QBP; mitochondrial cardiomyopathy; p32; pediatrics; sudden death; ventricular fibrillation
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Year: 2021 PMID: 34003581 PMCID: PMC8924900 DOI: 10.1002/ajmg.a.62262
Source DB: PubMed Journal: Am J Med Genet A ISSN: 1552-4825 Impact factor: 2.578