View genomic variant #0000025362
Chromosome |
17 |
Allele |
Unknown |
Affects function (as reported) |
Not classified |
Affects function (by curator) |
Not classified |
Type |
- |
DNA change (genomic) (Relative to hg19 / GRCh37) |
g.7123478_7123479insGCCCT |
Published as |
- |
GERP |
- |
Segregation |
- |
DB-ID |
ACADVL_000243 |
MSCV |
- |
dbSNP ID |
- |
Frequency |
- |
Sources |
; clinvar; |
Reference |
- |
Variant remarks |
- |
Genetic origin |
- |
Variant_disease |
- |
Average frequency (large NGS studies) |
Variant not found in online data sets |
Owner |
Lishuang Shen |
Variant on transcripts
ClinVar @ MSeqDR | RCVaccession | RCV000795353; | Chromosome | 17:7123478..7123478 | Allele frequencies from ExAC | 0.00006 | ClinVar Allele ID | 646645 | Disease database name and identifier | MONDO:MONDO:0008723, MedGen:C3887523, OMIM:201475, Orphanet:26793 | ClinVar preferred disease name | Very long chain acyl-CoA dehydrogenase deficiency | HGVS variant names | NC 000017.10:g.7123478G>A | ClinVar review status | criteria provided, single submitter | Clinical Significance | Uncertain significance | Variant type | single nucleotide variant | Sequence Ontology for variant type | SO:0001483 | Gene symbol:Gene id. | ACADVL:37|LOC130060113:130060113 | Molecular consequence | SO:0001583|missense variant, SO:0001623|5 prime UTR variant | Allele origin | germline | dbSNP ID | 781061205 | Variant Flags | : |
ClinVar @ MSeqDR as full content XML tree
ClinVar @ MSeqDR | RCVaccession | RCV000665413; | Chromosome | 17:7123478..7123479 | ClinVar Allele ID | 548617 | Disease database name and identifier | MONDO:MONDO:0008723, MedGen:C3887523, OMIM:201475, Orphanet:26793 | ClinVar preferred disease name | Very long chain acyl-CoA dehydrogenase deficiency | HGVS variant names | NC 000017.10:g.7123483 7123487dup | ClinVar review status | criteria provided, conflicting interpretations | Clinical Significance | Conflicting interpretations of pathogenicity | Conflicting clinical significance | Pathogenic(2)|Likely pathogenic(3)|Uncertain significance(1) | Variant type | Duplication | Sequence Ontology for variant type | SO:1000035 | Gene symbol:Gene id. | ACADVL:37|LOC130060113:130060113 | Molecular consequence | SO:0001589|frameshift variant, SO:0001623|5 prime UTR variant | Allele origin | germline | dbSNP ID | 1555527532 | Variant Flags | : |
ClinVar @ MSeqDR as full content XML tree
ClinVar @ MSeqDR | RCVaccession | RCV003460259; | Chromosome | 17:7123479..7123483 | ClinVar Allele ID | 2838683 | Disease database name and identifier | MONDO:MONDO:0008723, MedGen:C3887523, OMIM:201475, Orphanet:26793 | ClinVar preferred disease name | Very long chain acyl-CoA dehydrogenase deficiency | HGVS variant names | NC 000017.10:g.7123483 7123487del | ClinVar review status | criteria provided, single submitter | Clinical Significance | Likely pathogenic | Variant type | Deletion | Sequence Ontology for variant type | SO:0000159 | Gene symbol:Gene id. | ACADVL:37|LOC130060113:130060113 | Molecular consequence | SO:0001589|frameshift variant, SO:0001623|5 prime UTR variant | Allele origin | unknown | Variant Flags | : |
ClinVar @ MSeqDR as full content XML tree
ClinVar @ MSeqDR | RCVaccession | RCV000652036; | Chromosome | 17:7123480..7123480 | ClinVar Allele ID | 531746 | Disease database name and identifier | MONDO:MONDO:0008723, MedGen:C3887523, OMIM:201475, Orphanet:26793 | ClinVar preferred disease name | Very long chain acyl-CoA dehydrogenase deficiency | HGVS variant names | NC 000017.10:g.7123482del | ClinVar review status | reviewed by expert panel | Clinical Significance | Pathogenic | Variant type | Deletion | Sequence Ontology for variant type | SO:0000159 | Variant clinical sources reported | ClinGen:CA624861220 | Gene symbol:Gene id. | ACADVL:37|LOC130060113:130060113 | Molecular consequence | SO:0001589|frameshift variant, SO:0001623|5 prime UTR variant | Allele origin | germline | dbSNP ID | 1443151475 | Variant Flags | : |
ClinVar @ MSeqDR as full content XML tree
MSeqDR View Variant at Gbrowse Mitomap Mitochondrial Variant Phenotype Information:
None Ensembl Variant Phenotype Information:
None
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