Variant #0000814743 (NC_000005.9:g.176831232G>T, NM_000505.3:c.983C>A (F12))
Individual ID |
00385695 |
Chromosome |
5 |
Allele |
Unknown |
Affects function (as reported) |
Affects function |
Affects function (by curator) |
Affects function |
Classification method |
ACMG |
Clinical classification |
pathogenic |
DNA change (genomic) (Relative to hg19 / GRCh37) |
g.176831232G>T |
DNA change (hg38) |
g.177404231G>T |
Published as |
c.1032C>A |
ISCN |
- |
DB-ID |
F12_000008 See all 38 reported entries |
Variant remarks |
The first French pedigree affected by HAE-F12. Incomplete penetrance: 8/13 affected individuals. Haplotype analyses with use of SNPs at the F12 locus provided evidence that the French family and 3 of the German families reported by Dewald and Bork (2006) shared a common founder. Plasma displays a gain-of-function of kallikrein-kinin system; p.(Thr328Lys) exhibits a lower glycosylation, with subsequent increased autoactivation of zymogen F12. Thr to Lys transition has consequence on the protein’s folding and conformation, with an open or relaxed conformation facilitating the access of kallikrein and plasmin and exposing cryptic proteolytic targets for thrombin that are normally concealed and not accessible in the compact conformation of FXII. The c.983C>A variant meets the ACMG criteria to be characterized pathogenic PP1, PM1, PM5, PS3, PS4_Mod. |
Reference |
Journal: Martin 2001 Journal: Cichon 2006 Journal: Björkvist 2015 Journal: de Maat 2016 |
ClinVar ID |
ClinVar-VCV000001169.8 |
dbSNP ID |
rs118204456 |
Origin |
Germline |
Segregation |
yes |
Frequency |
0.000004 (1/234142, GnomAD_exome) |
Re-site |
- |
VIP |
- |
Methylation |
- |
Average frequency (gnomAD v.2.1.1) |
Retrieve |
Owner |
Christian Drouet |
Database submission license |
Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International |
Created by |
Christian Drouet |
Date created |
2021-10-14 12:37:09 +02:00 (CEST) |
Date last edited |
2025-02-06 11:19:16 +01:00 (CET) |

Variant on transcripts
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