Table 2.
Pathogenic or likely pathogenic variants based on the ACMG guidelines
| Variant information | Database | Frequency | |||||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Gene | OMIM number | Chr: pos | Variant | AA change | dbSNP | ACMG interpretation result | Criteria | Disease‐associated | EmVClass | Clinvitae | M‐CAP score | ClinVar | HGMD | VarSome | InterVar | Maximum minor Allele frequency | Frequency in Taiwan |
| MSH6 | 120435 | 2:48026566 | NM_000179.2:c.1444C>T | R482X | rs63750909 | P | PVS1 PM1 PM2 PP3 | Lynch syndrome | NA | P | PP | P | DM | P | P | 0.0006 | NA |
| TSC2 | 613254 | 16:2100489 | NM_000548.5:c.225+2T>C | NA | LP | PVS1 PM2 PP3 | Tuberous sclerosis syndrome | NA | NA | NA | LP | NA | P | NA | NA | NA | |
| SCN5A | 603830 | 3:38645439 | NM_000335.5:c.1654G>C | G552R | rs3918389 | LP | PS1 PM1 PM2 PP3 | Brugada syndrome | NA | NA | PP | NA | NA | LP | LP | 0.0002 | NA |
| ATP7B | 277900 | 13:52511739 | NM_000053.4:c.3775_3776insAAAG | G1259Efs*14 | NA | P | PVS1 PM1 PM2 PP3 | Wilson disease | NA | NA | NA | NA | NA | P | NA | NA | NA |
| ATP7B | 277900 | 13:52523835 | NM_000053.4:c.2828G>A | G943D | rs779323689 | LP | PS1 PM1 PM2 PP3 | Wilson disease | NA | P/LP | PP | P/LP | DM | LP | LP | 0.0019 | 0.00066 |
| ATP7B | 277900 | 13:52523859 | NM_000053.4:c.2804C>T a | T935M | rs750019452 | LP | PS1 PM1 PM2 PP3 | Wilson disease | NA | P/LP | PP | P/LP | DM | LP | LP | 0.0024 | 0.00198 |
| ATP7B | 277900 | 13:52532469 | NM_000053.4:c.2333G>T | R778L | rs28942074 | P | PS1 PS3 PM1 PM2 PP3 | Wilson disease | P | P | PP | P | DM | P | LP | 0.0023 | 0.00165 |
Abbreviations: DM, disease‐causing mutation; LB, likely benign; LP, likely pathogenic; NA, not available; P, pathogenic; PP, possibly pathogenic; VUS, variant of uncertain significance.
a
ATP7B c.2804C>T was identified in two individuals.