Table 1.
Disease-causing heterozygous PPARG variants in subjects with FPLD3
| Patients (n) | Variant cDNA level | Variant protein level | rs number | Clinvar prediction | Functional score [7] | References |
|---|---|---|---|---|---|---|
| 1 | c.282delG | p.K94Nfs*4 | NA | NA | — | — |
| 1 | c.421G>C | p.V141L | NA | NA | −3.5 | — |
| 1 | c.452C>G | p.Y151C | rs1354592503 | Pathogenic | −4.2 | [10, 11] |
| 1 | c.480+120G>C | (?) | NA | NA | — | — |
| 1 | c.580C>T | p.R194W | rs121909146 | Pathogenic | −5.4 | [12] |
| 2 | c.641C>T | p.P214L | NA | NA | −0.48 | — |
| 3 | c.670G>T | p.E224* | NA | NA | — | — |
| 1 | c.971T>C | p.I324T | rs1378972597 | Pathogenic | −2.57 | — |
| 1 | c.1154G>A | p.R385Q | rs140204299 | Uncertain significance | −1.4 | [7] |
| 3 | c.1159C>T | p.P387S | NA | NA | −4.2 | [7, 9] |
| 2 | c.1184A>G | p.K395R | NA | NA | −1.16 | [7, 9] |
| 6 | c.1273C>T | p.R425C | rs72551364 | Pathogenic | −5.37 | [5] |
| 1 | c.1313A>C | p.Q438P | NA | Uncertain significance | −4.9 | [7, 9] |
| 2 | c.1393C>T | p.Q465* | NA | NA | — | — |
| 1 | c.1480+1G>A | (?) | NA | NA | — | — |
| 4 | c.1484C>T | p.P495L | rs121909244 | Pathogenic | −5.58 | [13–15] |
| 1 | c.1495delG | p.E499Rfs*12 | NA | NA | — | — |
Five variants were null or splice site variants. Eleven were missense variants, of which 5 were classified as “pathogenic” and 2 of “uncertain significance” by Clinvar. The 2 variants with “uncertain significance” have been published before. One variant is a novel intronic variant not present in the gnomAD database. For the 4 missense variants that had no information in Clinvar, we looked at the functional score according to Majithia et al [7]. All had negative scores. Two of them had functional scores ≤3.5, which has increased probability of lipodystrophy, and 1 of them, p.P387S, has been previously published by 2 groups. There was evidence of segregation in 3 family members for p.K395R and in 2 family members for p.P214L.
Abbreviation: NA, not available.