Variant #0000987827 (NC_000001.10:g.100696460_100696462del, NM_001918.2:c.263_265del (DBT))
| Individual ID |
00451662 |
| Chromosome |
1 |
| Allele |
Both (homozygous) |
| Affects function (as reported) |
Probably affects function |
| Affects function (by curator) |
Not classified |
| Classification method |
ACMG |
| Clinical classification |
likely pathogenic (recessive) |
| DNA change (genomic) (Relative to hg19 / GRCh37) |
g.100696460_100696462del |
| DNA change (hg38) |
g.100230904_100230906del |
| Published as |
- |
| ISCN |
- |
| DB-ID |
DBT_000041 |
| Variant remarks |
This variant was classified as per ACMG guidelines (Richards et al 2015) and the recently developed ACMG scoring system (Tavtigian et al 2020). Nguyen et al 2020 reported a Vietnamese pediatric patient with maple sirup who presents this same variant in homozygous state (PMID:32515140). In silico analysis shows that the microdeletion occurs in the functional domain PLN02528 (2-oxoisovalerate dehydrogenase E2 component). The MutPred-indel program predicts it as deleterious: sp P11182 ODB2_HUMAN Lipoamide acyltransferase component: 0.7621 (>0.5 = deleterious) NA - The CADD program predicts it as also as deleterious: 21.0 (score "threshold" for deleterious >20). The Glu at position 88 of the DBT protein is evolutionarily conserved from human to C.elegans; Adhikari 2020:32778825, |
| Reference |
- |
| ClinVar ID |
ClinVar-527136 |
| dbSNP ID |
rs1217050849 |
| Origin |
Germline |
| Segregation |
yes |
| Frequency |
- |
| Re-site |
- |
| VIP |
- |
| Methylation |
- |
| Average frequency (gnomAD v.2.1.1) |
Retrieve |
| Owner |
Miriam Erandi Reyna-Fabián |
| Database submission license |
Creative Commons Attribution-ShareAlike 4.0 International |
| Created by |
Miriam Erandi Reyna-Fabián |
| Date created |
2024-06-24 04:35:36 +02:00 (CEST) |
| Date last edited |
2024-06-28 09:37:48 +02:00 (CEST) |

Variant on transcripts
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