Synergistic effects of rare variants of ARHGAP31 and FBLN1 in vitro in terminal transverse limb defects

Hong, Tao; Chu, Fan; Li, Yingjie; Xu, Mengmeng; Li, Wenjiao; Li, Chuanzhou

doi:10.3389/fgene.2022.946854

Cited by 3 publications

(2 citation statements)

References 20 publications

(38 reference statements)

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“…To our knowledge, missense variants of ARHGAP31 that contribute to the development of dominant forms of AOS have not been described, yet. However, the synergic effect of two rare missense variants of the ARHGAP31 and FBLN1 genes was recently demonstrated in a patient with terminal transverse limb defects [19]. A heterozygous individual carrying one of these variants did not show the phenotype [19].…”

Section: Discussionmentioning

confidence: 99%

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Characterization of a New Variant in ARHGAP31 Probably Involved in Adams–Oliver Syndrome in a Family with a Variable Phenotypic Spectrum

Santaniello,

Faversani,

Corsaro

et al. 2024

Genes

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Adams–Oliver syndrome is a rare inherited condition characterized by scalp defects and limb abnormalities. It is caused by variants in different genes such as ARHGAP31. Here, we used an interdisciplinary approach to study a family with lower limb anomalies. We identified a novel variant in the ARHGAP31 gene that is predicted to result in a truncated protein with a constitutively activated catalytic site due to the loss of 688 amino acids involved in the C-terminal domain, essential for protein auto-inhibition. Pathogenic variants in ARHGAP31 exon 12, leading to a premature protein termination, are associated with Adams–Oliver syndrome. Bioinformatic analysis was useful to elucidate the impact of the identified genetic variant on protein structure. To better understand the impact of the identified variant, 3D protein models were predicted for the ARHGAP31 wild type, the newly discovered variant, and other pathogenetic alterations already reported. Our study identified a novel variant probably involved in Adams–Oliver syndrome and increased the evidence on the phenotypic variability in patients affected by this syndrome, underlining the importance of translational research, including experimental and bioinformatics analyses. This strategy represents a successful model to investigate molecular mechanisms involved in syndrome occurrence.

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Section: Discussionmentioning

confidence: 99%

“…However, the synergic effect of two rare missense variants of the ARHGAP31 and FBLN1 genes was recently demonstrated in a patient with terminal transverse limb defects [19]. A heterozygous individual carrying one of these variants did not show the phenotype [19].…”

Section: Discussionmentioning

confidence: 99%