Litcius/Paper detail

The Desmin (DES) Mutation p.A337P Is Associated with Left-Ventricular Non-Compaction Cardiomyopathy

О. В. Куликова, Andreas Brodehl, А. В. Киселева, R. P. Myasnikov, А. Н. Мешков, Caroline Stanasiuk, Anna Gärtner, М.Г. Дивашук, Е. А. Сотникова, Sergey Koretskiy, М. С. Харлап, V. A. Kozlova, Е. А. Мершина, Polina Pilus, В. Е. Синицын, Hendrik Milting, S. А. Boytsov, Oxana M. Drapkina

2021Genes39 citationsDOIOpen Access PDF

Abstract

Here, we present a small Russian family, where the index patient received a diagnosis of left-ventricular non-compaction cardiomyopathy (LVNC) in combination with a skeletal myopathy. Clinical follow-up analysis revealed a LVNC phenotype also in her son. Therefore, we applied a broad next-generation sequencing gene panel approach for the identification of the underlying mutation. Interestingly, DES-p.A337P was identified in the genomes of both patients, whereas only the index patient carried DSP-p.L1348X. DES encodes the muscle-specific intermediate filament protein desmin and DSP encodes desmoplakin, which is a cytolinker protein connecting desmosomes with the intermediate filaments. Because the majority of DES mutations cause severe filament assembly defects and because this mutation was found in both affected patients, we analyzed this DES mutation in vitro by cell transfection experiments in combination with confocal microscopy. Of note, desmin-p.A337P forms cytoplasmic aggregates in transfected SW-13 cells and in cardiomyocytes derived from induced pluripotent stem cells underlining its pathogenicity. In conclusion, we suggest including the DES gene in the genetic analysis for LVNC patients in the future, especially if clinical involvement of the skeletal muscle is present.

Topics & Concepts

DesminBiologyMutationIntermediate filamentDesmoplakinCardiomyopathyMyopathyTransfectionMolecular biologyDilated cardiomyopathyCell biologyPathologyGeneCancer researchGeneticsInternal medicineHeart failureCytoskeletonMedicineCellImmunologyImmunohistochemistryVimentinCardiomyopathy and Myosin StudiesSkin and Cellular Biology ResearchNuclear Structure and Function
The Desmin (DES) Mutation p.A337P Is Associated with Left-Ventricular Non-Compaction Cardiomyopathy | Litcius