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NM_014363.6(SACS):c.11100dup (p.Trp3701fs) AND Autosomal recessive spastic ataxia

Germline classification:
Likely pathogenic (1 submission)
Last evaluated:
Apr 15, 2019
Review status:
1 star out of maximum of 4 stars
criteria provided, single submitter
Somatic classification
of clinical impact:
None
Review status:
(0/4) 0 stars out of maximum of 4 stars
no assertion criteria provided
Somatic classification
of oncogenicity:
None
Review status:
(0/4) 0 stars out of maximum of 4 stars
no assertion criteria provided
Record status:
current
Accession:
RCV001195303.5

Allele description [Variation Report for NM_014363.6(SACS):c.11100dup (p.Trp3701fs)]

NM_014363.6(SACS):c.11100dup (p.Trp3701fs)

Gene:
SACS:sacsin molecular chaperone [Gene - OMIM - HGNC]
Variant type:
Duplication
Cytogenetic location:
13q12.12
Genomic location:
Preferred name:
NM_014363.6(SACS):c.11100dup (p.Trp3701fs)
HGVS:
  • NC_000013.11:g.23332775_23332776insT
  • NC_000013.11:g.23332776dup
  • NG_012342.1:g.105927dup
  • NM_001278055.2:c.10659dup
  • NM_014363.6:c.11100dupMANE SELECT
  • NP_001264984.1:p.Trp3554fs
  • NP_055178.3:p.Trp3701fs
  • NC_000013.10:g.23906914_23906915insT
  • NC_000013.10:g.23906915dup
Protein change:
W3554fs
Links:
dbSNP: rs1883571351
NCBI 1000 Genomes Browser:
rs1883571351
Molecular consequence:
  • NM_001278055.2:c.10659dup - frameshift variant - [Sequence Ontology: SO:0001589]
  • NM_014363.6:c.11100dup - frameshift variant - [Sequence Ontology: SO:0001589]
Observations:
1

Condition(s)

Name:
Autosomal recessive spastic ataxia
Identifiers:
MONDO: MONDO:0017847; MedGen: C5679900

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Assertion and evidence details

Help
Submission AccessionSubmitterReview Status
(Assertion method)		Clinical Significance
(Last evaluated)		OriginMethodCitations
SCV001365625Laboratory for Molecular Medicine, Mass General Brigham Personalized Medicine
criteria provided, single submitter

(LMM Criteria)		Likely pathogenic
(Apr 15, 2019) 		germlineclinical testing

PubMed (1)
[See all records that cite this PMID]

Help

Summary from all submissions

EthnicityOriginAffectedIndividualsFamiliesChromosomes testedNumber TestedFamily historyMethod
not providedgermlineunknown11not providednot providednot providedclinical testing

Citations

PubMed

A systematic approach to assessing the clinical significance of genetic variants.

Duzkale H, Shen J, McLaughlin H, Alfares A, Kelly MA, Pugh TJ, Funke BH, Rehm HL, Lebo MS.

Clin Genet. 2013 Nov;84(5):453-63. doi: 10.1111/cge.12257.

PubMed [citation]
PMID:
24033266
PMCID:
PMC3995020

Details of each submission

From Laboratory for Molecular Medicine, Mass General Brigham Personalized Medicine, SCV001365625.1

#EthnicityIndividualsChromosomes TestedFamily HistoryMethodCitations
1not provided1not providednot providedclinical testing PubMed (1)

Description

The p.Trp3701MetfsX17 variant in SACS has not been previously reported in individuals with spastic ataxia and was absent from large population studies. This variant is predicted to cause a frameshift, which alters the protein’s amino acid sequence beginning at position 3701 and leads to a premature termination codon 17 amino acids downstream. This termination codon occurs within the last exon and is, therefore, likely to escape nonsense mediated decay (NMD) and result in a protein truncated by 860 amino acids (representing 19% of the full protein length). Notably, many other truncating variants in this region have been reported in the homozygous or compound heterozygous state in individuals with ARSACS. In summary, although additional studies are required to fully establish its clinical significance, this variant meets criteria to be classified as likely pathogenic for autosomal recessive spastic ataxia, Charlevoix-Saguenay type. ACMG/AMP Criteria applied: PVS1_Strong, PM2.

#SampleMethodObservation
OriginAffectedNumber testedTissuePurposeMethodIndividualsAllele frequencyFamiliesCo-occurrences
1germlineunknownnot providednot providednot provided1not provided1not provided

Last Updated: Jun 23, 2024