Variant #0000735262 (NC_000001.10:g.160252826G>A, NM_002857.3:c.254C>T (PEX19))
Individual ID |
00334927 |
Chromosome |
1 |
Allele |
Both (homozygous) |
Affects function (as reported) |
Effect unknown |
Affects function (by curator) |
Not classified |
Classification method |
ACMG |
Clinical classification |
VUS |
DNA change (genomic) (Relative to hg19 / GRCh37) |
g.160252826G>A |
DNA change (hg38) |
- |
Published as |
- |
ISCN |
- |
DB-ID |
PEX19_000006 See all 3 reported entries |
Variant remarks |
ACMG PM2, PP3, PP4, BP1; The sib-pair's electroclinical phenotype is different to the previously reported phenotype in a single case, with childhood onset, no dysmorphic features and a less rapidly progressive clinical course. However, the same predicted damaging missense variant is homozygous in four unrelated families (two reported here) with similar presentation from Malta; the same haplotype was confirmed supporting a founder effect. The variant was not present in the Maltese human genome project (n=400). It is therefore with high confidence we expand the PEX19 clinical spectrum to PME. |
Reference |
PubMed: Courage 2021, Journal: Courage 2021 |
ClinVar ID |
- |
dbSNP ID |
- |
Origin |
Germline |
Segregation |
- |
Frequency |
- |
Re-site |
- |
VIP |
- |
Methylation |
- |
Average frequency (gnomAD v.2.1.1) |
0.00051 View details |
Owner |
Carolina Courage |
Database submission license |
No license selected |
Created by |
Carolina Courage |
Date created |
2021-03-02 13:37:42 +01:00 (CET) |
Date last edited |
2021-04-14 10:21:27 +02:00 (CEST) |

Variant on transcripts
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