Clinical and genetic data of 22 new patients with <i>SMAD3</i> pathogenic variants and review of the literature

Chesneau, Bertrand; Edouard, Thomas; Dulac, Yves; Colineaux, Hélène; Langeois, Maud; Hanna, Nadine; Boileau, Cathérine; Arnaud, Pauline; Chassaing, Nicolas; Julia, Sophie; Jondeau, Guillaume; Plancke, Aurélie; Kien, Philippe Khau Van; Plaisancié, Julie

doi:10.1002/mgg3.1132

Cited by 13 publications

(17 citation statements)

References 29 publications

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“…In particular, Loeys-Dietz syndrome type 3 (LDS3), originally named aneurysms-osteoarthritis syndrome because of the striking findings of early-onset osteoarthritis in the fourth decade of life and the presence of aortic and other vascular aneurysms, is typically considered milder than LDS1/2. While similar systemic manifestations can be present in LDS3 patients as compared to LDS1/2 patients, the of age of onset of vascular pathology is usually later (Chesneau et al, 2020;Schepers et al, 2018;van de Laar et al, 2011) and 34.8 years, respectively, which is nearly a decade before the onset of aortic events in LDS3 individuals (Jondeau et al, 2016). And although not seen in the MAC, aortic dilation necessitating surgical repair has been described in pediatric patients with SMAD3-related Loeys-Dietz syndrome (Chesneau et al, 2020;Fitzgerald, Bhat, Conard, Hyland, & Pizarro, 2014), with the youngest reported age of aneurysm repair at 12 months old (Wischmeijer et al, 2013).…”

Section: Discussionmentioning

confidence: 86%

“…In particular, Loeys‐Dietz syndrome type 3 (LDS3), originally named aneurysms‐osteoarthritis syndrome because of the striking findings of early‐onset osteoarthritis in the fourth decade of life and the presence of aortic and other vascular aneurysms, is typically considered milder than LDS1/2. While similar systemic manifestations can be present in LDS3 patients as compared to LDS1/2 patients, the of age of onset of vascular pathology is usually later (Chesneau et al, 2020; Schepers et al, 2018; van de Laar et al, 2011). Hostetler et al (2019) reported data from the Montalcino Aortic Consortium (MAC) indicating that of 212 individuals with SMAD3 mutations, only 37% had ever experienced an aortic event (defined as elective aortic aneurysm repair, aortic dissection, or aortic rupture) with a median age at first aortic event of 47 years.…”

Section: Discussionmentioning

confidence: 96%

“…This is in contrast to the outcomes of 441 affected individuals in the MAC with TGFBR1 or TGFBR2 variants, who had a median age of death of 28.4 and 34.8 years, respectively, which is nearly a decade before the onset of aortic events in LDS3 individuals (Jondeau et al, 2016). And although not seen in the MAC, aortic dilation necessitating surgical repair has been described in pediatric patients with SMAD3 ‐related Loeys‐Dietz syndrome (Chesneau et al, 2020; Fitzgerald, Bhat, Conard, Hyland, & Pizarro, 2014), with the youngest reported age of aneurysm repair at 12 months old (Wischmeijer et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

“…LDS3 was initially named aneurysms-osteoarthritis syndrome due to striking presence of both aortic aneurysms and early-onset osteoarthritis, the latter of which distinguishes LDS3 from other subtypes of LDS (van de Laar et al, 2011). The phenotype of LDS3 can be milder than that caused by TGFBR1 and TGFBR2 mutations, with lower prevalence of skeletal manifestations and later onset of aortic and arterial disease, although a spectrum of disease has been reported (Chesneau et al, 2020;Hostetler et al, 2019;Schepers et al, 2018). Until 2020, all described cases of LDS were the result of heterozygous pathogenic variants in one of the six aforementioned genes of the TGF-β signaling pathway (Marsili et al, 2020;Mégarbané et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

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The first reported case of Loeys‐Dietz syndrome in a patient with biallelic SMAD3 variants

Baskin

Morris

Vara

et al. 2020

American J of Med Genetics Pt A

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Loeys-Dietz syndrome (LDS), a connective tissue disorder characterized by its vascular, skeletal, craniofacial, and cutaneous manifestations is caused by mutations in one of six genes (TGFBR1, TGFBR2, SMAD2, SMAD3, TGFB2, and TGFB3). Until recently, all reported cases of LDS have been attributed to heterozygous pathogenic variants in these genes. Here, we report the first case of Loeys-Dietz syndrome due to SMAD3 biallelic likely pathogenic variants in a 15-year-old male with classic Loeys-Dietz features, including dysmorphic facial features, significant scoliosis, and pectus excavatum, arachnodactyly, severe aortic root dilation, and diffuse arterial tortuosity. His parents are each heterozygous for the likely pathogenic variant and are more mildly affected. To our knowledge, this represents the first reported case of biallelic SMAD3-related Loeys-Dietz syndrome and the third case in the literature of biallelic LDS, indicating that there are multiple genetic modes of inheritance underlying this disorder.

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Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

The first reported case of Loeys‐Dietz syndrome in a patient with biallelic SMAD3 variants

Baskin

Morris

Vara

et al. 2020

American J of Med Genetics Pt A

View full text Add to dashboard Cite

show abstract

“…As a result, it is generally accepted that SMAD3 variants are characterized by inter‐ and intra‐familial variability in phenotypic expression in addition to incomplete penetrance. Moreover, some patients present vascular aneurysms or dissections of small arteries without an aortic phenotype (Chesneau et al., 2020; Hostetler et al, 2019). The absence of complete arterial tree imaging in some of our patients makes characterization of a definitive clinical phenotype rather difficult.…”

Section: Discussionmentioning

confidence: 99%

Identification of novel splice mutation in SMAD3 in two Cypriot families with nonsyndromic thoracic aortic aneurysm. Two case reports

Keravnou

Bashiardes

Barberis

et al. 2020

Molec Gen & Gen Med

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Background Thoracic aortic aneurysm and dissection (TAA/D) represents a potentially lethal disease group characterized by an increased risk of dissection or rupture. Only a small percentage (approximately 30%) of individuals with nonsyndromic familial TAA/D have a pathogenic variant in one of the genes that have been found to be associated with the disease. Methods A targeted sequencing panel and direct sequencing approach were used to identify causative mutations in the index patients and other family members. Results In this study we report two apparently unrelated Cypriot families with nonsyndromic familial TAA/D. The proband A is a female patient diagnosed with TAA/D and intracranial aneurysm and opted for an elective intervention. The proband B is a male patient who was diagnosed with TAA/D and underwent cardiac surgery. Sequencing analysis identified a novel splice site variant (c.871+1G>A) in SMAD3 which is shown to be associated with the disease. Analysis of mRNA from the patient's tissue confirmed aberrant splicing and exon 6 skipping. Conclusion Our findings expand the mutation spectrum of variants that have been shown to be associated with nonsyndromic familial TAA/D. This study demonstrates the importance of a comprehensive clinical and genetic evaluation aiming at early diagnosis and intervention.

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Heterozygous variants in SPTBN1 cause intellectual disability and autism

Rosenfeld

Xiao

Bekheirnia

et al. 2021

American J of Med Genetics Pt A

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Spectrins are common components of cytoskeletons, binding to cytoskeletal elements and the plasma membrane, allowing proper localization of essential membrane proteins, signal transduction, and cellular scaffolding. Spectrins are assembled from α and β subunits, encoded by SPTA1 and SPTAN1 (α) and SPTB, SPTBN1, SPTBN2, SPTBN4, and SPTBN5 (β). Pathogenic variants in various spectrin genes are associated with erythroid cell disorders (SPTA1, SPTB) and neurologic disorders (SPTAN1, SPTBN2, and SPTBN4), but no phenotypes have been definitively associated with variants in SPTBN1 or SPTBN5. Through exome sequencing and case matching, we identified seven unrelated individuals with heterozygous SPTBN1 variants: two with de novo missense variants and five with predicted loss‐of‐function variants (found to be de novo in two, while one was inherited from a mother with a history of learning disabilities). Common features include global developmental delays, intellectual disability, and behavioral disturbances. Autistic features (4/6) and epilepsy (2/7) or abnormal electroencephalogram without overt seizures (1/7) were present in a subset. Identification of loss‐of‐function variants suggests a haploinsufficiency mechanism, but additional functional studies are required to fully elucidate disease pathogenesis. Our findings support the essential roles of SPTBN1 in human neurodevelopment and expand the knowledge of human spectrinopathy disorders.

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Clinical and genetic data of 22 new patients with SMAD3 pathogenic variants and review of the literature

Cited by 13 publications

References 29 publications

The first reported case of Loeys‐Dietz syndrome in a patient with biallelic SMAD3 variants

The first reported case of Loeys‐Dietz syndrome in a patient with biallelic SMAD3 variants

Identification of novel splice mutation in SMAD3 in two Cypriot families with nonsyndromic thoracic aortic aneurysm. Two case reports

Heterozygous variants in SPTBN1 cause intellectual disability and autism

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