Genes (Jul 2024)

In Silico Analysis of the Missense Variants of Uncertain Significance of <i>CTNNB1</i> Gene Reported in GnomAD Database

  • Arturo Caballero-Avendaño,
  • Melva Gutiérrez-Angulo,
  • María de la Luz Ayala-Madrigal,
  • José Miguel Moreno-Ortiz,
  • Anahí González-Mercado,
  • Jorge Peregrina-Sandoval

DOI
https://doi.org/10.3390/genes15080972
Journal volume & issue
Vol. 15, no. 8
p. 972

Abstract

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CTNNB1 pathogenic variants are related to the improper functioning of the WNT/β-catenin pathway, promoting the development of different types of cancer of somatic origin. Bioinformatics analyses of genetic variation are a great tool to understand the possible consequences of these variants on protein structure and function and their probable implication in pathologies. The objective of this study is to describe the impact of the missense variants of uncertain significance (VUS) of the CTNNB1 gene on structure and function of the β-catenin protein. The CTNNB1 variants were obtained from the GnomAD v2.1.1 database; subsequently, a bioinformatic analysis was performed using the VarSome, UCSC Genome Browser, UniProt, the Kinase Library database, and DynaMut2 platforms to evaluate clinical significance, gene conservation, consensus sites for post-translational modifications, and the dynamics and stability of proteins. The GnomAD v2.1.1 database included 826 variants of the CTNNB1 gene, of which 385 were in exons and exon/intron boundaries. Among these variants, 214 were identified as missense, of which 146 were classified as VUS. Notably, 12 variants were in proximity to consensus sites for post-translational modifications (PTMs). The in silico analysis showed a slight tendency towards probably pathogenic for c.59C>T (p.Ala20Val) and c.983T>C (p.Met328Thr) missense VUS. These findings provide possible functional implications of these variants in some types of cancer.

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