Table 1.
Exon | Nucleotide Change | Amino Acid Change | Domain | Mutation Group | Subjects | Origin | MetaSVMa | CADD phreda | REVELa | ACMG |
---|---|---|---|---|---|---|---|---|---|---|
1 | c.62T>C | p.Ile21Thr | α1 | III | 1 | de novo | 0.3729 | 27.1 | 0.901 | pathogenic |
1 | c.68A>G | p.Tyr23Cys | α1 | III | 2 | de novo | 0.7752 | 27.1 | 0.937 | pathogenic |
3 | c.191A>G | p.Tyr64Cys | switch II | I | 3 | de novo | 0.7976 | 23.4 | 0.834 | pathogenic |
3 | c.196A>G | p.Arg66Gly | switch II | I | 4, 5 | de novo | 0.5326 | 26.9 | 0.836 | pathogenic |
3 | c.203G>A | p.Arg68Gln | switch II | I | 6, 7 | de novo | 0.6586 | 26.3 | 0.827 | pathogenic |
3 | c.242G>T | p.Cys81Phe | β4 | II | 8 | de novo | 0.6280 | 30.0 | 0.840 | pathogenic |
3 | c.247T>C | p.Ser83Pro | β4 | II | 9, 10 | de novo | 0.8283 | 27.8 | 0.853 | pathogenic |
4 | c.476C>T | p.Ala159Val | NBP | II | 11 | de novo | 1.0179 | 34.0 | 0.916 | pathogenic |
5 | c.511G>Ab | p.Glu171Lys | CBR | III | 12, 13–15 | 1 de novo, 1 familial | 0.0158 | 24.7 | 0.768 | pathogenic |
Nucleotide numbering reflects cDNA numbering with 1 corresponding to the A of the ATG translation initiation codon in the CDC42 reference sequence (GenBank: NM_001791.3). No variants were reported in the public databases ExAC and GnomAD. All variants were predicted to be “deleterious” by Combined Annotation Dependent Depletion (CADD) v.1.3, Database for Nonsynonymous SNPs’ Functional Predictions (dbNSFP) Support Vector Machine (SVM) v.3.0, and REVEL algorithms.16, 17, 18 All changes satisfied the necessary criteria to be classified as pathogenic according to the American College of Medical Genetics guidelines.19 Abbreviations: NBP, nucleotide binding pocket; CBR, CRIB motif binding region.
Scores > 0 (MetaSVM), > 15 (CADDphred) or > 0.5 (REVEL) predict that the sequence change has a significant impact on protein structure and function.
This change affects transcript variant 1 (GenBank: NM_001791.3) and isoform 1 (GenBank: NP_001782.1), while it does not affect transcript variant 2 (GenBank: NM_044472.2) and isoform 2 (GenBank: NP_426359.1). The two isoforms have the same amino acid length but are characterized by a different C terminus.