Rescue of cardiomyopathy through U7sn<scp>RNA</scp>‐mediated exon skipping in <i>Mybpc3</i>‐targeted knock‐in mice

Gedicke‐Hornung, Christina; Behrens-Gawlik, Verena; Reischmann, Silke; Geertz, Birgit; Stimpel, Doreen; Weinberger, Florian; Schlossarek, Saskia; Précigout, Guillaume; Braren, Ingke; Eschenhagen, Thomas; Mearini, Giulia; Lorain, Stéphanie; Voït, Thomas; Dreyfus, Patrick A.; Garcı́a, Luis; Carrier, Lucie

doi:10.1002/emmm.201202168

Cited by 82 publications

(77 citation statements)

References 64 publications

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“…Classical treatments of HCM target symptoms and LV outflow tract obstruction with pharmacological and/or surgical treatments, but do not address the cause of the disease 29,30 . New strategies targeting the endogenous mutant pre-mRNA or RNA such as exon skipping, exon inclusion, trans-splicing and ARTICLE RNA silencing, opened the perspective for a causal therapy for patients with HCM 2,21,22,31,32 . These proof-of-concept studies still have major limitations.…”

Section: Discussionmentioning

confidence: 99%

“…We previously showed that a 5 0 -transsplicing approach corrects the mutation in cardiac myocytes and in vivo in HCM KI mice, but its efficiency was too low to prevent or rescue the disease phenotype 22 . In-frame skipping of mutated exons by antisense oligonucleotides inserted in U7snRNA produced a stable functional protein and transiently rescued the cardiac phenotype in KI mice 21 . In both cases, however, the amount of repaired protein remained very low 21,22 .…”

Section: Discussionmentioning

confidence: 99%

“…In-frame skipping of mutated exons by antisense oligonucleotides inserted in U7snRNA produced a stable functional protein and transiently rescued the cardiac phenotype in KI mice 21 . In both cases, however, the amount of repaired protein remained very low 21,22 . Another RNA-targeting approach, the allele-specific silencing using oligonucleotides has been recently evaluated in another HCM mouse model carrying a mutation in Myh6 encoding a-myosin heavy chain showing disease prevention until 25 wks of age, which, in this model, needs to be revealed by application of cyclosporine 31 .…”

Section: Discussionmentioning

confidence: 99%

“…Long-term expression of cMyBP-C in the heart was achieved by a single intravenous injection in 1-day-old KI mice using a combination of AAV9, which is the most cardiotropic serotype in rodents 21,36 and a cardiomyocyte-specific promoter 36,37 . Previous data indicated that combining AAV9 and a chicken minimal truncated TNNT2 promoter gave 4640-fold higher expression in the heart than in other organs in mice 37 .…”

Section: Discussionmentioning

confidence: 99%

“…Some of these infants have homozygous or compound heterozygous frameshift MYBPC3 mutations 14,[16][17][18][19][20] , expected to result in low level or absence of mutant cMyBP-C. Here we tested the easily generalizable idea to prevent the disease phenotype by adding full-length Mybpc3 by gene therapy in a Mybpc3-targeted knock-in (KI) mouse model 21,22 that genetically mimics the severe neonatal HCM cases 21,22 . These mice carry at the homozygous state the human c.772G4A MYBPC3 transition, which is one of the most frequent HCM mutations (13% in a large Italian cohort) 23 and is associated with a bad prognosis 19 .…”

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confidence: 99%

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Mybpc3 gene therapy for neonatal cardiomyopathy enables long-term disease prevention in mice

et al. 2014

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Homozygous or compound heterozygous frameshift mutations in MYBPC3 encoding cardiac myosin-binding protein C (cMyBP-C) cause neonatal hypertrophic cardiomyopathy (HCM), which rapidly evolves into systolic heart failure and death within the first year of life. Here we show successful long-term Mybpc3 gene therapy in homozygous Mybpc3-targeted knock-in (KI) mice, which genetically mimic these human neonatal cardiomyopathies. A single systemic administration of adeno-associated virus (AAV9)-Mybpc3 in 1-day-old KI mice prevents the development of cardiac hypertrophy and dysfunction for the observation period of 34 weeks and increases Mybpc3 messenger RNA (mRNA) and cMyBP-C protein levels in a dose-dependent manner. Importantly, Mybpc3 gene therapy unexpectedly also suppresses accumulation of mutant mRNAs. This study reports the first successful long-term gene therapy of HCM with correction of both haploinsufficiency and production of poison peptides. In the absence of alternative treatment options except heart transplantation, gene therapy could become a realistic treatment option for severe neonatal HCM.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Mybpc3 gene therapy for neonatal cardiomyopathy enables long-term disease prevention in mice

et al. 2014

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The mechanics of the heart: zooming in on hypertrophic cardiomyopathy and cMyBP‐C

Suay-Corredera

Alegre-Cebollada

2022

FEBS Letters

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Hypertrophic cardiomyopathy (HCM), a disease characterized by cardiac muscle hypertrophy and hypercontractility, is the most frequently inherited disorder of the heart. HCM is mainly caused by variants in genes encoding proteins of the sarcomere, the basic contractile unit of cardiomyocytes. The most frequently mutated among them is MYBPC3, which encodes cardiac myosin-binding protein C (cMyBP-C), a key regulator of sarcomere contraction. In this review, we summarize clinical and genetic aspects of HCM and provide updated information on the function of the healthy and HCM sarcomere, as well as on emerging therapeutic options targeting sarcomere mechanical activity. Building on what is known about cMyBP-C activity, we examine different pathogenicity drivers by which MYBPC3 variants can cause disease, focussing on protein haploinsufficiency as a common pathomechanism also in nontruncating variants. Finally, we discuss recent evidence correlating altered cMyBP-C mechanical properties with HCM development.

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In Vitro Correction of a Pseudoexon-Generating Deep Intronic Mutation in LGMD2A by Antisense Oligonucleotides and Modified Small Nuclear RNAs

et al. 2013

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Limb-girdle muscular dystrophy type 2A (LGMD2A) is the most frequent autosomal recessive muscular dystrophy. It is caused by mutations in the calpain-3 (CAPN3) gene. The majority of the mutations described to date are located in the coding sequence of the gene. However, it is estimated that 25% of the mutations are present at exon-intron boundaries and modify the pre-mRNA splicing of the CAPN3 transcript. We have previously described the first deep intronic mutation in the CAPN3 gene: c.1782+1072G>C mutation. This mutation causes the pseudoexonization of an intronic sequence of the CAPN3 gene in the mature mRNA. In the present work, we show that the point mutation generates the inclusion of the pseudoexon in the mRNA using a minigene assay. In search of a treatment that restores normal splicing, splicing modulation was induced by RNA-based strategies, which included antisense oligonucleotides and modified small-nuclear RNAs. The best effect was observed with antisense sequences, which induced pseudoexon skipping in both HeLa cells cotransfected with mutant minigene and in fibroblasts from patients. Finally, transfection of antisense sequences and siRNA downregulation of serine/arginine-rich splicing factor 1 (SRSF1) indicate that binding of this factor to splicing enhancer sequences is involved in pseudoexon activation.

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Rescue of cardiomyopathy through U7snRNA‐mediated exon skipping in Mybpc3‐targeted knock‐in mice

Cited by 82 publications

References 64 publications

Mybpc3 gene therapy for neonatal cardiomyopathy enables long-term disease prevention in mice

Mybpc3 gene therapy for neonatal cardiomyopathy enables long-term disease prevention in mice

The mechanics of the heart: zooming in on hypertrophic cardiomyopathy and cMyBP‐C

In Vitro Correction of a Pseudoexon-Generating Deep Intronic Mutation in LGMD2A by Antisense Oligonucleotides and Modified Small Nuclear RNAs

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