A postnatal role for embryonic myosin revealed by MYH3 mutations that alter TGFβ signaling and cause autosomal dominant spondylocarpotarsal synostosis

Zieba, Jennifer; Zhang, Wenjuan; Chong, Jessica X.; Forlenza, Kimberly N.; Martı́n, Jorge; Heard, Kelly J.; Grange, Dorothy K.; Butler, Merlin G.; Kleefstra, Tjitske; Lachman, Ralph S.; Nickerson, Deborah A.; Regnier, Michael; Cohn, Daniel H.; Bamshad, Michael J.; Krakow, Deborah

doi:10.1038/srep41803

Cited by 32 publications

(46 citation statements)

References 31 publications

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“…Given the recent implication of monoallelic MYH3 variants in some cases of SCTS 6,7 and the suspicion that recessive inheritance underpins SCTS in the families in this study, the maternally transmitted haplotypes in individuals 1 and 2 were also examined. This showed that the top maternally transmitted haplotype that individuals 1 and 2 shared with individual 5 was also inclusive of the MYH3 locus (a 9 cM segment encompassing 28 annotated genes; Figure 2B).…”

Section: Analysis Of Shared Haplotypesmentioning

confidence: 99%

“…The wider cohort of SCTS-affected individuals without pathogenic variants in FLNB (n ¼ 16) had significantly more MYH3 truncating variants than presumptively healthy control individuals from publicly available databases (Supplemental Data). In the Genome Aggregation Database (gnomAD), 13 Our observations that individuals 1, 2, and 5 carry the same MYH3 splice-site variant on a shared paternal haplotype and also share a maternal haplotype in the context of 6 Zieba et al 7 Chong et al sibling recurrence suggest that a maternally derived pathogenic variant remains to be defined. We therefore performed WGS on individuals 1-3 and then prioritized and filtered MYH3 variants for high impact (SnpEff).…”

Section: Analysis Of Shared Haplotypesmentioning

confidence: 99%

“…5 FLNB was the sole identified locus for SCTS until recent reports of monoallelic variants in MYH3 (MIM: 160720) in families affected by vertical transmission of a SCTS phenotype. 6 An unrelated individual with simplex SCTS and affected members of a three-generation family have also been reported to be heterozygous for protein-altering MYH3 mutations, 7 including an in-frame deletion of a single amino acid and a frameshift variant leading to a presumptive premature termination of protein translation. Before these observations, monoallelic missense MYH3 mutations transmitted in a dominant fashion were also shown to underlie cases of distal arthrogryposis type 8 (DA8, otherwise known as autosomal-dominant multiple pterygium syndrome [MIM: 178110]).…”

Section: Introductionmentioning

confidence: 99%

“…The implication of MYH3 in the etiopathogenesis of SCTS suggests functions that extend to osteogenesis, and indeed, Zieba et al have recently demonstrated its role in the regulation of TGFß activity in the scleromyotome; this role is reminiscent of the mechanism that underpins the FLNB-deficient form of the condition. 7 Here, we investigated the molecular basis of SCTS in a cohort of individuals with no FLNB variants accounting for their phenotypes. These individuals were phenotypically similar to those with SCTS caused by mutations in FLNB but with the notable exception of the presence of contractures that were often clinically prominent at birth.…”

Section: Introductionmentioning

confidence: 99%

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Recessive Spondylocarpotarsal Synostosis Syndrome Due to Compound Heterozygosity for Variants in MYH3

Cameron-Christie

Wells

Simon

et al. 2018

The American Journal of Human Genetics

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Spondylocarpotarsal synostosis syndrome (SCTS) is characterized by intervertebral fusions and fusion of the carpal and tarsal bones. Biallelic mutations in FLNB cause this condition in some families, whereas monoallelic variants in MYH3, encoding embryonic heavy chain myosin 3, have been implicated in dominantly inherited forms of the disorder. Here, five individuals without FLNB mutations from three families were hypothesized to be affected by recessive SCTS on account of sibling recurrence of the phenotype. Initial whole-exome sequencing (WES) showed that all five were heterozygous for one of two independent splice-site variants in MYH3. Despite evidence indicating that three of the five individuals shared two allelic haplotypes encompassing MYH3, no second variant could be located in the WES datasets. Subsequent genome sequencing of these three individuals demonstrated a variant altering a 5' UTR splice donor site (rs557849165 in MYH3) not represented by exome-capture platforms. When the cohort was expanded to 16 SCTS-affected individuals without FLNB mutations, nine had truncating mutations transmitted by unaffected parents, and six inherited the rs557849165 variant in trans, an observation at odds with the population allele frequency for this variant. The rs557849165 variant disrupts splicing in the 5' UTR but is still permissive of MYH3 translational initiation, albeit with reduced efficiency. Although some MYH3 variants cause dominant SCTS, these data indicate that others (notably truncating variants) do not, except in the context of compound heterozygosity for a second hypomorphic allele. These observations make genetic diagnosis challenging in the context of simplex presentations of the disorder.

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Section: Analysis Of Shared Haplotypesmentioning

confidence: 99%

Section: Analysis Of Shared Haplotypesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Recessive Spondylocarpotarsal Synostosis Syndrome Due to Compound Heterozygosity for Variants in MYH3

Cameron-Christie

Wells

Simon

et al. 2018

The American Journal of Human Genetics

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“…2 Mutations in MYH3, which encodes embryonic myosin heavy chain 3, have been detected in some families with autosomal dominant SCT. 3 However, in some cases, the specific genetic mutation remains unknown. 2 Our patient underwent genetic study, with testing for mutation of the FLNB gene, but no specific genetic mutation could be demonstrated.…”

mentioning

confidence: 99%

Spondylocarpotarsal synostosis syndrome: “Bat wings” spinal fusions and “ladybug” carpal coalitions

Bazzocchi

Spinnato

Gómez

et al. 2019

Pediatrics & Neonatology

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A novel pathogenic MYH3 mutation in a child with Sheldon–Hall syndrome and vertebral fusions

Scala

Accogli

Grandis

et al. 2018

American J of Med Genetics Pt A

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Sheldon-Hall syndrome (SHS) is the most common of the distal arthrogryposes (DAs), a group of disorders characterized by congenital non-progressive contractures. Patients with SHS present with contractures of the limbs and a distinctive triangular facies with prominent nasolabial folds. Calcaneovalgus deformity is frequent, as well as camptodactyly and ulnar deviation. Causative mutations in at least four different genes have been reported (MYH3, TNNI2, TPM2, and TNNT3). MYH3 plays a pivotal role in fetal muscle development and mutations in this gene are associated with Freeman-Sheldon syndrome, distal arthrogryposis 8 (DA8), and autosomal dominant spondylocarpotarsal synostosis. The last two disorders are characterized by skeletal abnormalities, in particular bony fusions. The observation that MYH3 may be mutated in these syndromes has suggested the involvement of this gene in bone development. We report the case of a boy with a novel pathogenic MYH3 mutation, presenting with the classical clinical features of SHS in association with unilateral carpal bone fusion and multiple vertebral fusions. This distinctive phenotype has never been reported in the literature so far and expands the phenotypic spectrum of SHS, endorsing the clinical variability of patients with MYH3-related disorders. Our findings also support a role for MYH3 in both muscle and bone development, suggesting a phenotypic continuum in MYH3-related disorders.

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A postnatal role for embryonic myosin revealed by MYH3 mutations that alter TGFβ signaling and cause autosomal dominant spondylocarpotarsal synostosis

Cited by 32 publications

References 31 publications

Recessive Spondylocarpotarsal Synostosis Syndrome Due to Compound Heterozygosity for Variants in MYH3

Recessive Spondylocarpotarsal Synostosis Syndrome Due to Compound Heterozygosity for Variants in MYH3

Spondylocarpotarsal synostosis syndrome: “Bat wings” spinal fusions and “ladybug” carpal coalitions

A novel pathogenic MYH3 mutation in a child with Sheldon–Hall syndrome and vertebral fusions

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