A new case of SMABF2 diagnosed in stillbirth expands the prenatal presentation and mutational spectrum of <i>ASCC1</i>

Giuffrida, Maria Grazia; Mastromoro, Gioia; Guida, Valentina; Truglio, Mauro; Fabbretti, Maria; Torres, Bárbara; Mazza, Tommaso; Luca, Alessandro De; Roggini, Mario; Bernardini, Laura; Pizzuti, Antonio

doi:10.1002/ajmg.a.61431

Cited by 11 publications

(14 citation statements)

References 15 publications

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“…Our proband was found to have biallelic variants in ASCC1 and her clinical phenotype is consistent with SMABF2 as reported in 11 other infants (Table 1). (Bohm et al, 2019;Giuffrida et al, 2020;Knierim et al, 2016;Lu et al, 2020;Oliveira et al, 2017) The findings in our proband confirm the association of biallelic variants in ASCC1 with SMABF2 characterized by severe diffuse hypotonia and congenital fractures and extends the phenotypic spectrum with her unique features of cleft palate, small spleen, transverse liver, cardiac abnormalities, and pulmonary vasculature with thromboemboli with chondroid appearance. The muscle histology findings of fiber atrophy, myofibrillar disorganization, and enlarged Z-bands are typical for SMABF2.…”

Section: Discussionsupporting

confidence: 82%

“…Biallelic variants in ASCC1 (MIM# 616867) have been recently identified as the underlying cause of a rare form of AMC known as spinal muscular atrophy with congenital bone fractures 2 (SMABF2) (Bamshad et al, 2009; Giuffrida et al, 2020; Knierim et al, 2016; Lu et al, 2020; Oliveira et al, 2017). ASCC1 encodes a subunit of the tetrameric ASC‐1 transcriptional co‐integrator complex that includes ASCC1, ASCC2, ASCC3, and TRIP4 (Jung et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

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Biallelic ASCC1 variants including a novel intronic variant result in expanded phenotypic spectrum of spinal muscular atrophy with congenital bone fractures 2 (SMABF2)

Rosano

Wegner

Shinawi

et al. 2021

American J of Med Genetics Pt A

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Spinal muscular atrophy with congenital bone fractures 2 (SMABF2), a type of arthrogryposis multiplex congenita (AMC), is characterized by congenital joint contractures, prenatal fractures of long bones, and respiratory distress and results from biallelic variants in ASCC1. Here, we describe an infant with severe, diffuse hypotonia, congenital contractures, and pulmonary hypoplasia characteristic of SMABF2, with the unique features of cleft palate, small spleen, transverse liver, and pulmonary thromboemboli with chondroid appearance. This infant also had impaired coagulation with diffuse petechiae and ecchymoses which has only been reported in one other infant with AMC. Using trio whole genome sequencing, our proband was identified to have biallelic variants in ASCC1. Using deep next generation sequencing of parental cDNA, we characterized alteration of splicing encoded by the novel, maternally inherited ASCC1 variant (c.297‐8 T > G) which provides a mechanism for functional pathogenicity. The paternally inherited ASCC1 variant is a rare nonsense variant (c.466C > T; p.Arg156*) that has been previously identified in one other infant with AMC. This report extends the phenotypic characteristics of ASCC1‐associated AMC (SMABF2) and describes a novel intronic variant that partially disrupts RNA splicing.

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Section: Discussionsupporting

confidence: 82%

Section: Introductionmentioning

confidence: 99%

Biallelic ASCC1 variants including a novel intronic variant result in expanded phenotypic spectrum of spinal muscular atrophy with congenital bone fractures 2 (SMABF2)

Rosano

Wegner

Shinawi

et al. 2021

American J of Med Genetics Pt A

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“…The question of primary motor neuron versus muscle involvement has not been clarified by more recent reports of three other patients with 5 novel ASCC1 mutations. Their clinical presentation was consistent with the lethal perinatal phenotype described above, including congenital bone fractures [ 33 , 34 , 35 ], mild brain ventricle dilatation abnormalities in one patient [ 35 ] and one stillbirth [ 24 ]. The muscle biopsy from one of them was reported as atrophic with no further description [ 33 ] and no muscle biopsies were performed in the remaining two cases.…”

Section: Ascc1 Mutations: Lethal Involvement Of Central Nervous System Skeletal Muscles and Bonessupporting

confidence: 63%

“…Congenital bone fractures, present in only two families with TRIP4 mutations [ 23 ], are part of the clinical phenotype in all the ASCC1 -mutated patients [ 24 , 33 , 34 , 35 ]. Although prenatal fractures have been non-specifically reported in other forms of congenital muscle disease [ 54 , 55 , 56 ], their frequency in ASCC1 -mutant cases suggests that, in this context, they are not an unspecific consequence of fetal immobility but directly linked to a role of ASCC1 in bone.…”

Section: Discussionmentioning

confidence: 99%

Inherited Defects of the ASC-1 Complex in Congenital Neuromuscular Diseases

Meunier

Villar-Quiles

Duband-Goulet

et al. 2021

IJMS

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Defects in transcriptional and cell cycle regulation have emerged as novel pathophysiological mechanisms in congenital neuromuscular disease with the recent identification of mutations in the TRIP4 and ASCC1 genes, encoding, respectively, ASC-1 and ASCC1, two subunits of the ASC-1 (Activating Signal Cointegrator-1) complex. This complex is a poorly known transcriptional coregulator involved in transcriptional, post-transcriptional or translational activities. Inherited defects in components of the ASC-1 complex have been associated with several autosomal recessive phenotypes, including severe and mild forms of striated muscle disease (congenital myopathy with or without myocardial involvement), but also cases diagnosed of motor neuron disease (spinal muscular atrophy). Additionally, antenatal bone fractures were present in the reported patients with ASCC1 mutations. Functional studies revealed that the ASC-1 subunit is a novel regulator of cell cycle, proliferation and growth in muscle and non-muscular cells. In this review, we summarize and discuss the available data on the clinical and histopathological phenotypes associated with inherited defects of the ASC-1 complex proteins, the known genotype–phenotype correlations, the ASC-1 pathophysiological role, the puzzling question of motoneuron versus primary muscle involvement and potential future research avenues, illustrating the study of rare monogenic disorders as an interesting model paradigm to understand major physiological processes.

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“…SMABF2 is characterized by intrauterine onset of fetal hypotonia and hypokinesia resulting in arthrogryposis multiplex along with intrauterine fracture of long bones. To date, only six families with SMABF2 have been reported in the literature, with NIHF reported as a presenting feature in a single case 38 . The fetus in the present study harbored two protein truncating variants –p.Arg138Ter, a known variant reported in a patient from Sri Lanka, 31 and p.Phe155SerfsTer15, a novel variant.…”

Section: Discussionmentioning

confidence: 53%

Utility of fetal whole exome sequencing in the etiological evaluation and outcome of nonimmune hydrops fetalis

et al. 2021

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Introduction Nonimmune hydrops fetalis (NIHF) has varied etiology. We assessed the etiological spectrum and evaluated the utility of fetal whole exome sequencing (fWES) for the diagnosis of NIHF. Methods In this prospective cohort study, we evaluated antenatally diagnosed fetuses with NIHF between July 2018 and December 2019 according to the routine diagnostic algorithm. Fetuses that remained undiagnosed after routine NIHF workup were subjected to fetal chromosomal microarray and/or WES. Pregnancies were followed up for clinical outcomes. Results Of the 45 fetuses, consanguinity and recurrent hydrops fetalis were observed in 13.3% (6/45) and 28.8% (13/45), respectively. Overall, an etiological diagnosis was possible in 75.5% (34/45) of fetuses, while the cause remained unknown in 24.4% (11/45). A genetic etiology was identified in 46.6% (21/45): aneuploidy and monogenic disorders in 28.8% (13/45) and 17.8% (8/45), respectively. fWES on 19 fetuses detected disease‐causing variants in 42.1% (8/19). Nine novel variants were detected in RAPSN, ASCC1, NEB, PKD1L1, GUSB, and PIEZO1. Only 8.8% (4/45) of the cohort survived without morbidity. Conclusions This study describes the etiological spectrum and the disease‐causing variants in an Indian cohort of hydropic fetuses.

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A new case of SMABF2 diagnosed in stillbirth expands the prenatal presentation and mutational spectrum of ASCC1

Cited by 11 publications

References 15 publications

Biallelic ASCC1 variants including a novel intronic variant result in expanded phenotypic spectrum of spinal muscular atrophy with congenital bone fractures 2 (SMABF2)

Biallelic ASCC1 variants including a novel intronic variant result in expanded phenotypic spectrum of spinal muscular atrophy with congenital bone fractures 2 (SMABF2)

Inherited Defects of the ASC-1 Complex in Congenital Neuromuscular Diseases

Utility of fetal whole exome sequencing in the etiological evaluation and outcome of nonimmune hydrops fetalis

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