2. Academic Validation
  3. Novel frameshift variant in MYL2 reveals molecular differences between dominant and recessive forms of hypertrophic cardiomyopathy

Novel frameshift variant in MYL2 reveals molecular differences between dominant and recessive forms of hypertrophic cardiomyopathy

  • PLoS Genet. 2020 May 26;16(5):e1008639. doi: 10.1371/journal.pgen.1008639.
Sathiya N Manivannan 1 2 Sihem Darouich 3 Aida Masmoudi 4 David Gordon 5 Gloria Zender 1 Zhe Han 6 Sara Fitzgerald-Butt 1 2 7 Peter White 5 7 Kim L McBride 1 2 7 Maher Kharrat 3 Vidu Garg 1 2 7 8
Affiliations

Affiliations

  • 1 Center for Cardiovascular Research, Abigail Wexner Research Institute at Nationwide Children's Hospital, Columbus, Ohio, United States of America.
  • 2 Heart Center, Nationwide Children's Hospital, Columbus, Ohio, United States of America.
  • 3 University of Tunis El Manar, Faculty of Medicine of Tunis, LR99ES10 Laboratory of Human Genetics, Tunis, Tunisia.
  • 4 University of Tunis El Manar, Faculty of Medicine of Tunis, Department of Embryo-Fetopathology, Maternity and Neonatology Center, Tunis, Tunisia.
  • 5 Institute for Genomic Medicine at Nationwide Children's Hospital, Columbus, Ohio, United States of America.
  • 6 Department of Medicine, University of Maryland School of Medicine, Baltimore, Maryland, United States of America.
  • 7 Department of Pediatrics, The Ohio State University, Columbus, Ohio, United States of America.
  • 8 Department of Molecular Genetics, The Ohio State University, Columbus, Ohio, United States of America.
PMID: 32453731 DOI: 10.1371/journal.pgen.1008639
Abstract

Hypertrophic cardiomyopathy (HCM) is characterized by thickening of the ventricular muscle without dilation and is often associated with dominant pathogenic variants in cardiac sarcomeric protein genes. Here, we report a family with two infants diagnosed with infantile-onset HCM and mitral valve dysplasia that led to death before one year of age. Using exome Sequencing, we discovered that one of the affected children had a homozygous frameshift variant in Myosin light chain 2 (MYL2:NM_000432.3:c.431_432delCT: p.Pro144Argfs*57;MYL2-fs), which alters the last 20 Amino acids of the protein and is predicted to impact the most C-terminal of the three EF-hand domains in MYL2. The parents are unaffected heterozygous carriers of the variant and the variant is absent in control cohorts from gnomAD. The absence of the phenotype in carriers and the infantile presentation of severe HCM is in contrast to HCM associated with dominant MYL2 variants. Immunohistochemical analysis of the ventricular muscle of the deceased patient with the MYL2-fs variant showed a marked reduction of MYL2 expression compared to an unaffected control. In vitro overexpression studies further indicate that the MYL2-fs variant is actively degraded. In contrast, an HCM-associated missense variant (MYL2:p.Gly162Arg) and three Other MYL2 stop-gain variants (p.E22*, p.K62*, p.E97*) that result in loss of the EF domains are stably expressed but show impaired localization. The degradation of the MYL2-fs can be rescued by inhibiting the cell's Proteasome function supporting a post-translational effect of the variant. In vivo rescue experiments with a Drosophila MYL2-homolog (Mlc2) knockdown model indicate that neither the MYL2-fs nor the MYL2:p.Gly162Arg variant supports normal cardiac function. The tools that we have generated provide a rapid screening platform for functional assessment of variants of unknown significance in MYL2. Our study supports an autosomal recessive model of inheritance for MYL2 loss-of-function variants in infantile HCM and highlights the variant-specific molecular differences found in MYL2-associated cardiomyopathy.

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