nsv7097869
- Organism: Homo sapiens
- Study:nstd102 (Clinical Structural Variants)
- Variant Type:copy number variation
- Method Type:Multiple
- Submitted on:GRCh37
- Variant Calls:1
- Validation:Not tested
- Clinical Assertions: Yes
- Region Size:31,879
- Description:NC_000007.13:g.(?_144288496)_(144320374_?)del AND Childhood encephalopathy due to thiamine pyrophosphokinase deficiency
- Genome View
- Variant Region Details and Evidence
- Validation Information
- Clinical Assertions
- Genotype Information
Genome View
Select assembly:Overlapping variant regions from other studies: 159 SVs from 38 studies. See in: genome view
Overlapping variant regions from other studies: 52 SVs from 21 studies. See in: genome view
Overlapping variant regions from other studies: 159 SVs from 38 studies. See in: genome view
Variant Region Placement Information
| Variant Region ID | Placement Type | Score | Assembly | Assembly Unit | Reciprocity | Sequence ID | Chr | Inner Start | Inner Stop |
|---|---|---|---|---|---|---|---|---|---|
| nsv7097869 | Remapped | Perfect | GRCh38.p12 | Primary Assembly | First Pass | NC_000007.14 | Chr7 | 144,591,403 | 144,623,281 |
| nsv7097869 | Remapped | Perfect | GRCh38.p12 | PATCHES | Second Pass | NW_018654715.1 | Chr7|NW_01 8654715.1 | 641,134 | 673,012 |
| nsv7097869 | Submitted genomic | GRCh37 (hg19) | Primary Assembly | NC_000007.13 | Chr7 | 144,288,496 | 144,320,374 |
Variant Call Information
| Variant Call ID | Type | Method | Analysis | Subject Phenotype | Clinical Interpretation | Source of Interpretation | ClinVar ID |
|---|---|---|---|---|---|---|---|
| nssv18789442 | deletion | Multiple | Multiple | Childhood encephalopathy due to thiamine pyrophosphokinase deficiency; THIAMINE METABOLISM DYSFUNCTION SYNDROME 5 (EPISODIC ENCEPHALOPATHY TYPE); THMD5; Thiamine metabolism dysfunction syndrome 5 (episodic encephalopathy type) | Pathogenic | ClinVar | RCV003111487.2, VCV002426751.2 |
Variant Call Placement Information
| Variant Call ID | Placement Type | Score | HGVS | Assembly | Reciprocity | Sequence ID | Chr | Inner Start | Inner Stop |
|---|---|---|---|---|---|---|---|---|---|
| nssv18789442 | Remapped | Perfect | NW_018654715.1:g.( ?_641134)_(673012_ ?)del | GRCh38.p12 | Second Pass | NW_018654715.1 | Chr7|NW_01 8654715.1 | 641,134 | 673,012 |
| nssv18789442 | Remapped | Perfect | NC_000007.14:g.(?_ 144591403)_(144623 281_?)del | GRCh38.p12 | First Pass | NC_000007.14 | Chr7 | 144,591,403 | 144,623,281 |
| nssv18789442 | Submitted genomic | NC_000007.13:g.(?_ 144288496)_(144320 374_?)del | GRCh37 (hg19) | NC_000007.13 | Chr7 | 144,288,496 | 144,320,374 |
No validation data were submitted for this variant
Clinical Assertions
| Variant Call ID | HGVS | Type | Allele Origin | Subject Phenotype | Clinical Interpretation | Source of Interpretation | ClinVar ID |
|---|---|---|---|---|---|---|---|
| nssv18789442 | GRCh37: NC_000007.13:g.(?_144288496)_(144320374_?)del | deletion | germline | Childhood encephalopathy due to thiamine pyrophosphokinase deficiency; THIAMINE METABOLISM DYSFUNCTION SYNDROME 5 (EPISODIC ENCEPHALOPATHY TYPE); THMD5; Thiamine metabolism dysfunction syndrome 5 (episodic encephalopathy type) | Pathogenic | ClinVar | RCV003111487.2, VCV002426751.2 |