View genomic variant #0000018208

Chromosome	17
Allele	Unknown
Affects function (as reported)	Affects function
Affects function (by curator)	Affects function
Type	-
DNA change (genomic) (Relative to hg19 / GRCh37)	g.12898101del
Published as	-
GERP	-
Segregation	-
DB-ID	ELAC2_000034
MSCV	MSCV_0018208
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	LOVD

Variant on transcripts

Legend

Please note that a short description of a certain column can be displayed when you move your mouse cursor over the column's header and hold it still. Below, a more detailed description is shown per column.

Affects function: The variant's effect on the protein's function, in the format 'R/C' where R is the value reported by the source and C is the value concluded by the curator; '+' indicating the variant affects function, '+?' probably affects function, '+*' affects function, not associated with individual's disease phenotype, '#' affects function, not associated with any known disease phenotype, '-' does not affect function, '-?' probably does not affect function, '?' effect unknown, '.' effect not classified.

Location: Location of variant at DNA level; note that the variant location can also be derived from the variant description.
All options:

5' gene flanking
5' UTR
Exon
Intron
3' UTR
3' gene flanking

Exon: Number of exon/intron containing variant; 2 = exon 2, 12i = intron 12, 2i_7i = exons 3 to 7, 8i_9 = border intron 8/exon 9.

DNA change (cDNA): Description of variant at DNA level, based on a coding DNA reference sequence (following HGVS recommendations); e.g. c.123C>T, c.123_145del, c.123_126dup.

Protein: Description of variant at protein level (following HGVS recommendations).

p.(Arg345Pro) = change predicted from DNA (RNA not analysed)
p.Arg345Pro = change derived from RNA analysis
p.? = unknown effect
p.0? = probably no protein produced

PolyPhen: Effect of variant, predicted by PolyPhen.
All options:

benign = Benign
possiblyDamaging = Possibly damaging
probablyDamaging = Probably damaging
noPrediction = No prediction

GVS function: The functional annotation of this position from the Genome Variation Server.
All options:

intergenic
near-gene-5
utr-5
coding
coding-near-splice
coding-synonymous
coding-synonymous-near-splice
codingComplex
codingComplex-near-splice
frameshift
frameshift-near-splice
missense
missense-near-splice
splice-5
intron
splice-3
stop-gained
stop-gained-near-splice
stop-lost
stop-lost-near-splice
utr-3
near-gene-3

Splice distance: The distance to the nearest splice site.

SIFT: SIFT Annotation

3 entries on 1 page. Showing entries 1 - 3.

Legend

Gene	Transcript ID	Transcript	Variant ID	Affects function	Location	Exon	DNA change (cDNA)	Protein	PolyPhen	GVS function	Splice distance	SIFT
ELAC2	00001869	NM_001165962.1	0000018208	./.	-	-	c.1889del	p.(Cys630Serfs*14)	-	-	-	-
ELAC2	00001871	NM_018127.6	0000018208	./.	-	-	c.2009del	p.(Cys670Serfs*14)	-	-	-	-
ELAC2	00001870	NM_173717.1	0000018208	./.	-	-	c.2006del	p.(Cys669Serfs*14)	-	-	-	-

Legend

ClinVar @ MSeqDR
RCVaccession	RCV001866962;
Chromosome	17:12898100..12898100
ClinVar Allele ID	1509283
Disease database name and identifier	MONDO:MONDO:0014190, MedGen:C3809526, OMIM:615440, Orphanet:369913
ClinVar preferred disease name	Combined oxidative phosphorylation defect type 17
HGVS variant names	NC 000017.10:g.12898100G>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.	ELAC2:60528
Molecular consequence	SO:0001819\|synonymous variant
Allele origin	germline
dbSNP ID	1598197387
Variant Flags	:

ClinVar @ MSeqDR as full content XML tree

ClinVar @ MSeqDR
RCVaccession RCV000578466; RCV002529038;
Chromosome 17:12898101..12898101
Allele frequencies from ExAC 0.00002
ClinVar Allele ID 481370
Disease database name and identifier MONDO:MONDO:0014190, MedGen:C3809526, OMIM:615440, Orphanet:369913|MeSH:D030342, MedGen:C0950123
ClinVar preferred disease name Combined oxidative phosphorylation defect type 17|Inborn genetic diseases
HGVS variant names NC 000017.10:g.12898101del
ClinVar review status criteria provided, multiple submitters, no conflicts
Clinical Significance Pathogenic
Variant type Deletion
Sequence Ontology for variant type SO:0000159
Variant clinical sources reported ClinGen:CA8400980
Gene symbol:Gene id. ELAC2:60528
Molecular consequence SO:0001589|frameshift variant
Allele origin
dbSNP ID 761385155
For included Variant: Tag-value pairs of disease database name and identifier, e.g. OMIM:NNNNNN MONDO:MONDO:0014190, MedGen:C3809526, OMIM:615440, Orphanet:369913
For included Variant : ClinVar preferred disease name for the concept specified by disease identifiers in CLNDISDB Combined oxidative phosphorylation defect type 17
Clinical significance for a haplotype or genotype that includes this variant. Reported as pairs of VariationID:clinical significance. 828177:Pathogenic
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