| Literature DB >> 30908796 |
Andrey V Marakhonov1,2, Andreas Brodehl3, Roman P Myasnikov4, Peter A Sparber2, Anna V Kiseleva5, Olga V Kulikova4, Alexey N Meshkov6,5, Anastasia A Zharikova7,5, Serguey N Koretsky8, Maria S Kharlap9, Caroline Stanasiuk3, Elena A Mershina7,10, Valentin E Sinitsyn7,10, Alexey O Shevchenko11, Natalia P Mozheyko12, Oksana M Drapkina8, Sergey A Boytsov13, Hendrik Milting3, Mikhail Yu Skoblov14,2.
Abstract
Mutations in DES, encoding desmin protein, are associated with different kinds of skeletal and/or cardiac myopathies. However, it is unknown, whether DES mutations are associated with left ventricular hypertrabeculation (LVHT). Here, we performed a clinical examination and subsequent genetic analysis in a family, with two individuals presenting LVHT with conduction disease and skeletal myopathy. The genetic analysis revealed a novel small in-frame deletion within the DES gene, p.Q113_L115del, affecting the α-helical rod domain. Immunohistochemistry analysis of explanted myocardial tissue from the index patient revealed an abnormal cytoplasmic accumulation of desmin and a degraded sarcomeric structure. Cell transfection experiments with wild-type and mutant desmin verified the cytoplasmic aggregation and accumulation of mutant desmin. Cotransfection experiments were performed to model the heterozygous state of the patients and revealed a dominant negative effect of the mutant desmin on filament assembly. DES:p.Q113_L115del is classified as a pathogenic mutation associated with dilated cardiomyopathy with prominent LVHT.Entities:
Keywords: 1A coiled-coil rod segment; desmin; left ventricular noncompaction cardiomyopathy (LVNC); small in-frame deletion
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Year: 2019 PMID: 30908796 DOI: 10.1002/humu.23747
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878