Table 1.
The FOXL2 mutations identified in the current study.
| DNA sequence variation | Amino acid change | Predicted protein change | Inheritance | Allele Frequency | Polyphen-2 | Mutation Taster | ACMG | Reference |
|---|---|---|---|---|---|---|---|---|
| c.173_175dup | p. Ser58dup | Insertion mutation | Sporadic | 0 | – | Disease causing | LP | Current study |
| c.188T>A | p. Ile63Asn | Missense mutation | Familial | 0 | Probably damaging | Disease causing | LP | (20) |
| c.316C>T | p. Leu106Phe | Missense mutation | Familial | 0 | Possibly damaging | Disease causing | LP | (5, 21) |
| c.382T>G | p. Trp128Gly | Missense mutation | Familial | 0 | Probably damaging | Disease causing | LP | (22) |
| c.383G>A | p. Trp128* | Nonsense mutation | Familial | 0 | – | Disease causing | P | (22, 23) |
| c.481C>T | p. Gln161* | Nonsense mutation | Sporadic | 0 | – | Disease causing | LP | Current study |
| c.576del | p. Lys193Serfs*78 | Frameshift mutation | Sporadic | 0 | – | Disease causing | LP | Current study |
| c.586C>T | p. Gln196* | Nonsense mutation | Sporadic | 0 | – | Disease causing | P | (24) |
| c.655C>T | p. Gln219* | Nonsense mutation | Familial | 0 | – | Disease causing | P | (25, 26) |
| c.672_701dup | p. Ala225_Ala234dup | Extended polyalanine tract | Familial | 4.28E-05 | – | Disease causing | P | (27, 28) |
| c.675_714del | p. Ala226Leufs*32 | Frameshift mutation | Sporadic | 0 | – | Disease causing | P | Current study |
| c.804dupC | p. Gly269Argfs*263 | Frameshift mutation | Sporadic | 0 | – | Disease causing | P | (27, 29) |
| c.843_859dup | p. Pro287Argfs*75 | Frameshift mutation | Sporadic | 0 | – | Disease causing | P | (27) |
ACMG, American College of Medical Genetics; LP, likely pathogenic; P, pathogenic.