Functional characterization of the novel DES mutation p.L136P associated with dilated cardiomyopathy reveals a dominant filament assembly defect

Article ID	Journal	Published Year	Pages	File Type
8473973	Journal of Molecular and Cellular Cardiology	2016	36 Pages	PDF

Abstract

In vitro analysis demonstrated that desmin-p.L136P is unable to form regular filaments and accumulate instead within the cytoplasm. Therefore, we classified DES-p.L136P as a likely pathogenic mutation. In conclusion, the functional characterization of DES-p.L136P might have relevance for the genetic counseling of affected families with similar DES mutations and could contribute to distinguish pathogenic mutations from benign rare variants.

Keywords

desmosomes Desmin Intermediate filaments Myofibrillar myopathy Dilated cardiomyopathy

Related Topics

Life Sciences Biochemistry, Genetics and Molecular Biology Cell Biology

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Functional characterization of the novel DES mutation p.L136P associated with dilated cardiomyopathy reveals a dominant filament assembly defect

Authors

Andreas Brodehl, Mareike Dieding, Niklas Biere, Andreas Unger, Bärbel Klauke, Volker Walhorn, Jan Gummert, Uwe Schulz, Wolfgang A. Linke, Brenda Gerull, Matthias Vorgert, Dario Anselmetti, Hendrik Milting,