ClinVar Genomic variation as it relates to human health
NM_005236.3(ERCC4):c.2395C>T (p.Arg799Trp)
The aggregate germline classification for this variant, typically for a monogenic or Mendelian disorder as in the ACMG/AMP guidelines, or for response to a drug. This value is calculated by NCBI based on data from submitters. Read our rules for calculating the aggregate classification.
Stars represent the aggregate review status, or the level of review supporting the aggregate germline classification for this VCV record. This value is calculated by NCBI based on data from submitters. Read our rules for calculating the review status. The number of submissions which contribute to this review status is shown in parentheses.
Pathogenic(10); Likely pathogenic(4); Uncertain significance(5)
No data submitted for somatic clinical impact
No data submitted for oncogenicity
Variant Details
- Identifiers
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NM_005236.3(ERCC4):c.2395C>T (p.Arg799Trp)
Variation ID: 16580 Accession: VCV000016580.65
- Type and length
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single nucleotide variant, 1 bp
- Location
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Cytogenetic: 16p13.12 16: 13947991 (GRCh38) [ NCBI UCSC ] 16: 14041848 (GRCh37) [ NCBI UCSC ]
- Timeline in ClinVar
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First in ClinVar Help The date this variant first appeared in ClinVar with each type of classification.
Last submission Help The date of the most recent submission for each type of classification for this variant.
Last evaluated Help The most recent date that a submitter evaluated this variant for each type of classification.
Germline Jun 9, 2014 Nov 24, 2024 May 16, 2024 - HGVS
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Nucleotide Protein Molecular
consequenceNM_005236.3:c.2395C>T MANE Select Help Transcripts from the Matched Annotation from the NCBI and EMBL-EBI (MANE) collaboration.
NP_005227.1:p.Arg799Trp missense NC_000016.10:g.13947991C>T NC_000016.9:g.14041848C>T NG_011442.1:g.32835C>T LRG_463:g.32835C>T LRG_463t1:c.2395C>T LRG_463p1:p.Arg799Trp Q92889:p.Arg799Trp - Protein change
- R799W
- Other names
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R788W
- Canonical SPDI
- NC_000016.10:13947990:C:T
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Functional
consequence HelpThe effect of the variant on RNA or protein function, based on experimental evidence from submitters.
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Global minor allele
frequency (GMAF) HelpThe global minor allele frequency calculated by the 1000 Genomes Project. The minor allele at this location is indicated in parentheses and may be different from the allele represented by this VCV record.
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Allele frequency
Help
The frequency of the allele represented by this VCV record.
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The Genome Aggregation Database (gnomAD) 0.00013
The Genome Aggregation Database (gnomAD), exomes 0.00048
Exome Aggregation Consortium (ExAC) 0.00051
Trans-Omics for Precision Medicine (TOPMed) 0.00143
- Links
Genes
Gene | OMIM | ClinGen Gene Dosage Sensitivity Curation |
Variation Viewer
Help
Links to Variation Viewer, a genome browser to view variation data from NCBI databases. |
Related variants | ||
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HI score
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The haploinsufficiency score for the gene, curated by ClinGen’s Dosage Sensitivity Curation task team. |
TS score
Help
The triplosensitivity score for the gene, curated by ClinGen’s Dosage Sensitivity Curation task team. |
Within gene
Help
The number of variants in ClinVar that are contained within this gene, with a link to view the list of variants. |
All
Help
The number of variants in ClinVar for this gene, including smaller variants within the gene and larger CNVs that overlap or fully contain the gene. |
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ERCC4 | - | - |
GRCh38 GRCh37 |
771 | 865 |
Conditions - Germline
Condition
Help
The condition for this variant-condition (RCV) record in ClinVar. |
Classification
Help
The aggregate germline classification for this variant-condition (RCV) record in ClinVar. The number of submissions that contribute to this aggregate classification is shown in parentheses. (# of submissions) |
Review status
Help
The aggregate review status for this variant-condition (RCV) record in ClinVar. This value is calculated by NCBI based on data from submitters. Read our rules for calculating the review status. |
Last evaluated
Help
The most recent date that a submitter evaluated this variant for the condition. |
Variation/condition record
Help
The RCV accession number, with most recent version number, for the variant-condition record, with a link to the RCV web page. |
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Pathogenic/Likely pathogenic (8) |
criteria provided, multiple submitters, no conflicts
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Feb 22, 2022 | RCV000018048.44 | |
Uncertain significance (2) |
criteria provided, single submitter
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Mar 29, 2016 | RCV000120808.6 | |
Conflicting interpretations of pathogenicity (4) |
criteria provided, conflicting classifications
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May 1, 2024 | RCV000415873.30 | |
Pathogenic (2) |
criteria provided, single submitter
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Dec 30, 2023 | RCV000467658.13 | |
Uncertain significance (1) |
criteria provided, single submitter
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Mar 30, 2021 | RCV000768209.3 | |
Pathogenic (1) |
no assertion criteria provided
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Apr 4, 2019 | RCV000766208.2 | |
Likely pathogenic (1) |
no assertion criteria provided
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- | RCV001034542.2 | |
Uncertain significance (1) |
criteria provided, single submitter
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Jan 1, 2019 | RCV001262417.2 | |
Likely pathogenic (1) |
no assertion criteria provided
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Mar 4, 2021 | RCV001391196.2 | |
Conflicting interpretations of pathogenicity (2) |
criteria provided, conflicting classifications
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May 16, 2024 | RCV001787804.3 | |
Likely pathogenic (2) |
criteria provided, multiple submitters, no conflicts
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May 21, 2022 | RCV002257360.4 | |
ERCC4-related disorder
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Likely pathogenic (1) |
no assertion criteria provided
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Feb 22, 2024 | RCV003924841.3 |
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Submissions - Germline
Classification
Help
The submitted germline classification for each SCV record. (Last evaluated) |
Review status
Help
Stars represent the review status, or the level of review supporting the submitted (SCV) record. This value is calculated by NCBI based on data from the submitter. Read our rules for calculating the review status. This column also includes a link to the submitter’s assertion criteria if provided, and the collection method. (Assertion criteria) |
Condition
Help
The condition for the classification, provided by the submitter for this submitted (SCV) record. This column also includes the affected status and allele origin of individuals observed with this variant. |
Submitter
Help
The submitting organization for this submitted (SCV) record. This column also includes the SCV accession and version number, the date this SCV first appeared in ClinVar, and the date that this SCV was last updated in ClinVar. |
More information
Help
This column includes more information supporting the classification, including citations, the comment on classification, and detailed evidence provided as observations of the variant by the submitter. |
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Pathogenic
(Feb 21, 2021)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
(Autosomal recessive inheritance)
Affected status: yes
Allele origin:
maternal
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Undiagnosed Diseases Network, NIH
Study: Undiagnosed Diseases Network (NIH), UDN
Accession: SCV001499824.1 First in ClinVar: Mar 07, 2021 Last updated: Mar 07, 2021 |
Number of individuals with the variant: 2
Clinical Features:
Renal cyst (present) , Sensorineural hearing loss disorder (present) , Cerebellar ataxia (present) , Dysarthria (present) , Pes cavus (present) , Anemia (present) , Chorea … (more)
Renal cyst (present) , Sensorineural hearing loss disorder (present) , Cerebellar ataxia (present) , Dysarthria (present) , Pes cavus (present) , Anemia (present) , Chorea (present) , Cerebral cortical atrophy (present) , Abnormal brainstem morphology (present) , Hypoplasia of the brainstem (present) , Hand tremor (present) , Abnormal cerebral cortex morphology (present) , Frontal cortical atrophy (present) , Temporal cortical atrophy (present) , Sensorimotor neuropathy (present) , Hand muscle atrophy (present) , Parietal cortical atrophy (present) , Occipital cortical atrophy (present) , Cognitive impairment (present) (less)
Age: 50-59 years
Sex: male
Ethnicity/Population group: Caucasians
Tissue: blood
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Uncertain significance
(Mar 04, 2021)
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criteria provided, single submitter
Method: clinical testing
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Fanconi anemia complementation group Q
Affected status: yes
Allele origin:
unknown
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Baylor Genetics
Study: CSER-TexasKidsCanSeq
Accession: SCV002030262.1 First in ClinVar: Dec 12, 2021 Last updated: Dec 12, 2021 |
Comment:
This variant was determined to be of uncertain significance according to ACMG Guidelines, 2015 [PMID:25741868].
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Likely pathogenic
(Feb 22, 2022)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
Affected status: yes
Allele origin:
germline
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MGZ Medical Genetics Center
Accession: SCV002580798.1
First in ClinVar: Oct 15, 2022 Last updated: Oct 15, 2022
Comment:
ACMG criteria applied: PM3_STR, PS3_MOD, PP4
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Number of individuals with the variant: 1
Sex: male
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Pathogenic
(May 25, 2022)
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criteria provided, single submitter
Method: clinical testing
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Not Provided
Affected status: yes
Allele origin:
germline
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GeneDx
Accession: SCV002522019.2
First in ClinVar: Jun 05, 2022 Last updated: Mar 04, 2023 |
Comment:
Published functional studies demonstrate R799W decreased activity compared to wild-type (Ahmad et al., 2010).; This variant is associated with the following publications: (PMID: 26074087, 20221251, … (more)
Published functional studies demonstrate R799W decreased activity compared to wild-type (Ahmad et al., 2010).; This variant is associated with the following publications: (PMID: 26074087, 20221251, 24728327, 9579555, 22941649, 23623386, 21612988, 23623389, 18628313, 28678401, 27356891, 29376097, 28376890, 8797827, 28767289, 28431612, 29403087, 27528516, 21228398, 29105242, 34426522, 30665703, 31692161, 31980526, 31871297, 29892709) (less)
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Pathogenic
(-)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
Affected status: unknown
Allele origin:
unknown
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Baylor Genetics
Accession: SCV003841218.1
First in ClinVar: Mar 18, 2023 Last updated: Mar 18, 2023 |
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Uncertain significance
(Nov 03, 2021)
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criteria provided, single submitter
Method: clinical testing
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not provided
Affected status: not provided
Allele origin:
germline
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Institute for Clinical Genetics, University Hospital TU Dresden, University Hospital TU Dresden
Accession: SCV002009697.3
First in ClinVar: Nov 06, 2021 Last updated: Jul 16, 2023 |
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Uncertain significance
(Mar 29, 2016)
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criteria provided, single submitter
Method: clinical testing
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not specified
Affected status: unknown
Allele origin:
germline
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Laboratory for Molecular Medicine, Mass General Brigham Personalized Medicine
Accession: SCV000539115.1
First in ClinVar: Jun 09, 2014 Last updated: Jun 09, 2014 |
Comment:
Variant identified in a genome or exome case(s) and assessed due to predicted null impact of the variant or pathogenic assertions in the literature or … (more)
Variant identified in a genome or exome case(s) and assessed due to predicted null impact of the variant or pathogenic assertions in the literature or databases. Disclaimer: This variant has not undergone full assessment. The following are preliminary notes: Present in 1/908 alleles in the other population and in 55/66734 European alleles of ExAC. Reported by Sijbers_1996 in a compound heterozygous individual with XP group F. (less)
Method: Genome/Exome Filtration
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Pathogenic
(Dec 19, 2018)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
Affected status: unknown
Allele origin:
germline
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Illumina Laboratory Services, Illumina
Accession: SCV000914705.1
First in ClinVar: May 27, 2019 Last updated: May 27, 2019 |
Comment:
Across a selection of the available literature, the ERCC4 c.2395C>T (p.Arg799Trp) variant has been identified in 11 probands with xeroderma pigmentosum including five in a … (more)
Across a selection of the available literature, the ERCC4 c.2395C>T (p.Arg799Trp) variant has been identified in 11 probands with xeroderma pigmentosum including five in a homozygous state, four in a heterozygous state and two in a compound heterozygous state (Sijbers et al. 1996; Sijbers et al. 1998; Gregg et al. 2011). The p.Arg799Trp variant is reported at a frequency of 0.001 in the European American population of the Exome Sequencing Project. Functional rescue studies showed that the variant could only partially rescue the nuclear excision repair defect and that the variant protein mislocalized to the cytoplasm (Sijbers et al. 1998; Ahmad et al. 2010). Based on the collective evidence, the p.Arg799Trp variant is classified as pathogenic for xeroderma pigmentosum. This variant was observed by ICSL as part of a predisposition screen in an ostensibly healthy population. (less)
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Uncertain significance
(Jan 01, 2019)
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criteria provided, single submitter
Method: clinical testing
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Breast carcinoma
Affected status: yes
Allele origin:
unknown
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Institute of Human Genetics, University of Leipzig Medical Center
Accession: SCV001440280.1
First in ClinVar: Oct 31, 2020 Last updated: Oct 31, 2020 |
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Likely pathogenic
(Oct 23, 2020)
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criteria provided, single submitter
Method: clinical testing
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not provided
(Unknown mechanism)
Affected status: yes
Allele origin:
germline
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Institute of Medical Genetics and Applied Genomics, University Hospital Tübingen
Accession: SCV001447559.1
First in ClinVar: Nov 28, 2020 Last updated: Nov 28, 2020 |
Clinical Features:
Cerebellar ataxia (present)
Sex: female
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Likely pathogenic
(Nov 02, 2021)
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criteria provided, single submitter
Method: curation
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Xeroderma pigmentosum
Affected status: unknown
Allele origin:
germline
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Sema4, Sema4
Accession: SCV002537945.1
First in ClinVar: Jun 24, 2022 Last updated: Jun 24, 2022
Comment:
The ERCC4 c.2395C>T (p.R799W) variant has been reported as homozygous or compound heterozygous in at least 8 individuals with xeroderma pigmentosum (XP) or ERCC4 releated … (more)
The ERCC4 c.2395C>T (p.R799W) variant has been reported as homozygous or compound heterozygous in at least 8 individuals with xeroderma pigmentosum (XP) or ERCC4 releated neurological (ataxia) or progeroid syndromes (PMID: 8797827, 9579555, 21612988, 27528516, 29105242). It was also reported in 2 individuals with head and neck squamous cell carcinoma and sporadic pancreatic ductal adenocarcinoma (zygosity not specified, PMID: 28678401, 28767289). It is also known as R788W in the literature. In silico predictions of the variant's effect on protein function are inconclusive. However, cultured fibroblasts in patients with both compound heterozygous and homozygous mutations show deficits of nucleotide excision repair and reduced cell survival (PMID: 9579555, 29105242). It was observed in 105/129048 chromosomes of the Non-Finnish European subpopulation, with no homozygotes, in the Genome Aggregation Database (http://gnomad.broadinstitute.org, PMID: 32461654). The variant has been reported in ClinVar (Variation ID 16580). Based on the current evidence available, this variant is interpreted as likely pathogenic. (less)
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Likely pathogenic
(May 21, 2022)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum
Affected status: unknown
Allele origin:
germline
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Women's Health and Genetics/Laboratory Corporation of America, LabCorp
Accession: SCV002548369.1
First in ClinVar: Jul 18, 2022 Last updated: Jul 18, 2022 |
Comment:
Variant summary: ERCC4 c.2395C>T (p.Arg799Trp) results in a non-conservative amino acid change located in the ERCC4 domain (IPR006166) of the encoded protein sequence. Four of … (more)
Variant summary: ERCC4 c.2395C>T (p.Arg799Trp) results in a non-conservative amino acid change located in the ERCC4 domain (IPR006166) of the encoded protein sequence. Four of five in-silico tools predict a damaging effect of the variant on protein function. The variant allele was found at a frequency of 0.00048 in 251312 control chromosomes, predominantly at a frequency of 0.00089 within the Non-Finnish European subpopulation in the gnomAD database. The observed variant frequency within Non-Finnish European control individuals in the gnomAD database is approximately 5 fold of the estimated maximal expected allele frequency for a pathogenic variant in ERCC4 causing Xeroderma Pigmentosum phenotype (0.00019), suggesting that the variant is a benign polymorphism found primarily in populations of Non-Finnish European origin, although this could represent a higher carrier frequency in this population. c.2395C>T has been widely reported in the literature as homozygous and compound heterozygous genotypes in multiple individuals affected with mild features of Xeroderma Pigmentosum associated with later onset neurodegeneration/ataxia/chorea/variant forms of Cockayne syndrome/XP-F complementation group (example, Sijbers_1998, Ahmad_2010, Marelli_2016, Carre_2017, Ngo_2020, Kashiyama_2013, Shanbag_2018, Doi_2018, Mori_2018). These data indicate that the variant is very likely to be associated with disease. At least one publication reports experimental evidence evaluating an impact on protein function (example, Sijbers_1998, Ahmad_2010). The most pronounced variant effect results in approximately 20% of normal Nucleotide Excision Repair (NER) activity. Multiple clinical diagnostic laboratories have submitted clinical-significance assessments for this variant to ClinVar after 2014 without evidence for independent evaluation. Multiple laboratories reported the variant with conflicting assessments (Pathogenic/Likely Pathogenic, n=8; VUS, n=5). Based on the evidence outlined above, the variant was classified as likely pathogenic. (less)
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Pathogenic
(-)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
(Autosomal recessive inheritance)
Affected status: yes
Allele origin:
unknown
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Wangler Lab, Baylor College of Medicine
Accession: SCV002587792.1
First in ClinVar: Oct 29, 2022 Last updated: Oct 29, 2022 |
Comment:
This missense ERCC4 variant at c.2395C>T (p.R799W) was seen on exome through the Texome project (R01HG011795). This variant has been described in individuals with ERCC4-related … (more)
This missense ERCC4 variant at c.2395C>T (p.R799W) was seen on exome through the Texome project (R01HG011795). This variant has been described in individuals with ERCC4-related conditions (PMID: 8797827, 9579555, 20221251, 27528516). It has been observed in gnomAD with a frequency of 0.040% in the heterozygous state and has not been observed in the homozygous state (PM2). Functional studies suggest this variant is functionally defective (PMID: 9579555, 20221251) (PS3).This variant is predicted to be deleterious (CADD: 31.000) (PP3). The evolutionary conservation of this residue is high. We classify this variant as pathogenic. (less)
Clinical Features:
Neoplasm of the skin (present) , Chorea (present) , Tremor (present) , Myoclonus (present) , Dysarthria (present) , Dementia (present) , Hearing impairment (present) , … (more)
Neoplasm of the skin (present) , Chorea (present) , Tremor (present) , Myoclonus (present) , Dysarthria (present) , Dementia (present) , Hearing impairment (present) , Slurred speech (present) (less)
Age: 60-69 years
Sex: male
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Pathogenic
(Aug 17, 2020)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
(Autosomal recessive inheritance)
Affected status: yes
Allele origin:
germline
|
Institute of Human Genetics Munich, Klinikum Rechts Der Isar, TU München
Accession: SCV002764685.1
First in ClinVar: Dec 24, 2022 Last updated: Dec 24, 2022 |
Number of individuals with the variant: 1
Clinical Features:
Chorea (present) , Tremor (present) , Dystonic disorder (present)
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Pathogenic
(Oct 28, 2021)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
Affected status: unknown
Allele origin:
germline
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St. Jude Molecular Pathology, St. Jude Children's Research Hospital
Accession: SCV002012437.2
First in ClinVar: Nov 11, 2021 Last updated: Dec 24, 2022 |
Comment:
The ERCC4 c.2395C>T (p.Arg799Trp) missense change has a maximum subpopulation frequency of 0.081% in gnomAD v2.1.1 (https://gnomad.broadinstitute.org/variant/16-14041848-C-T). Six of seven in silico tools predict a … (more)
The ERCC4 c.2395C>T (p.Arg799Trp) missense change has a maximum subpopulation frequency of 0.081% in gnomAD v2.1.1 (https://gnomad.broadinstitute.org/variant/16-14041848-C-T). Six of seven in silico tools predict a deleterious effect of this variant on protein function (PP3), and in vitro functional assays in LCLs (Epstein–Barr virus transformed lymphoblastoid cell lines) and fibroblasts have shown that this variant causes reduced protein expression of nuclear ERCC4 which is attributed to protein mislocalization and can result in decreased cell survival and DNA replication after ultraviolet light exposure (PS3; PMID: 20221251, 29105242, 9579555). This variant has been reported in over ten individuals affected with xeroderma pigmentosum (PS4, PM3; PMID: 8797827, 9579555, 23623389, 21228398, 28431612, 29892709). In addition, it has been reported in three individuals with autosomal recessive cerebellar ataxia with mild pigmentation of exposed skin areas and/or an equivocal history of pathological sunburn (PMID: 29403087), one individual with sporadic ataxia (PMID: 31692161), two individuals with head and neck squamous cell carcinoma (PMID: 28678401), one individual with sporadic pancreatic adenocarcinoma (PMID: 28767289), one individual with Cockayne syndrome (PMID: 29105242), and one individual with colorectal cancer (PMID: 31871297). This variant is also known as p.Arg788Trp in the literature. In summary, this variant meets criteria to be classified as pathogenic based on the ACMG/AMP criteria applied: PS3, PS4, PM3, PP3. (less)
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Uncertain significance
(Mar 30, 2021)
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criteria provided, single submitter
Method: clinical testing
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Xeroderma pigmentosum, group F
XFE progeroid syndrome Fanconi anemia complementation group Q
Affected status: unknown
Allele origin:
germline
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Center for Genomics, Ann and Robert H. Lurie Children's Hospital of Chicago
Accession: SCV000898673.2
First in ClinVar: Apr 25, 2019 Last updated: May 06, 2023 |
Comment:
ERCC4 NM_005236 exon 11 p.Arg799Trp (c.2395C>T): This variant has been reported in the literature in at least 5 individuals with features or a diagnosis of … (more)
ERCC4 NM_005236 exon 11 p.Arg799Trp (c.2395C>T): This variant has been reported in the literature in at least 5 individuals with features or a diagnosis of Xeroderma Pigmentosum-F as compound heterozygous or homozygous (Sijbers 1996 PMID: 8797827, Sijbers 1998 PMID:9579555, Kashiyama 2013 PMID:23623389, Marelli 2016 PMID:27528516, Carre 2017 PMID:28431612). This variant is present in 103/126562 Caucasian individuals in the Genome Aggregation Database (http://gnomad.broadinstitute.org/rs121913049). Please note, disease causing variants may be present in control databases at low frequencies, reflective of the general population and/or variable expressivity. This variant is present in ClinVar (Variation ID:16580). Evolutionary conservation and computational predictive tools suggest that this variant may impact the protein. In addition, functional studies have shown a deleterious effect of this variant (Sijbers 1998 PMID:9579555, de Laat 1998 PMID:9722633). However, these studies may not accurately represent in vivo biological function. In summary, data on this variant is insufficient for disease classification. Therefore, the clinical significance of this variant is uncertain. (less)
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Pathogenic
(Dec 30, 2023)
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criteria provided, single submitter
Method: clinical testing
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Fanconi anemia complementation group Q
Xeroderma pigmentosum, group F Cockayne syndrome
Explanation for multiple conditions: Uncertain.
The variant was classified for several related diseases, possibly a spectrum of disease; the variant may be associated with one or more the diseases.
Affected status: unknown
Allele origin:
germline
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Labcorp Genetics (formerly Invitae), Labcorp
Accession: SCV000548332.9
First in ClinVar: Apr 17, 2017 Last updated: Feb 28, 2024 |
Comment:
This sequence change replaces arginine, which is basic and polar, with tryptophan, which is neutral and slightly polar, at codon 799 of the ERCC4 protein … (more)
This sequence change replaces arginine, which is basic and polar, with tryptophan, which is neutral and slightly polar, at codon 799 of the ERCC4 protein (p.Arg799Trp). This variant is present in population databases (rs121913049, gnomAD 0.08%), and has an allele count higher than expected for a pathogenic variant. This missense change has been observed in individual(s) with clinical features of ERCC4-related conditions (PMID: 8797827, 20221251, 23623389, 26074087, 27356891, 27528516, 28431612, 28678401, 28767289, 29105242, 29403087, 29892709). In at least one individual the data is consistent with being in trans (on the opposite chromosome) from a pathogenic variant. This variant is also known as c.2377C>T, p.Arg788Trp. ClinVar contains an entry for this variant (Variation ID: 16580). Advanced modeling of protein sequence and biophysical properties (such as structural, functional, and spatial information, amino acid conservation, physicochemical variation, residue mobility, and thermodynamic stability) performed at Invitae indicates that this missense variant is expected to disrupt ERCC4 protein function with a positive predictive value of 80%. Experimental studies have shown that this missense change affects ERCC4 function (PMID: 9579555, 20221251). For these reasons, this variant has been classified as Pathogenic. (less)
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Pathogenic
(May 01, 2024)
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criteria provided, single submitter
Method: clinical testing
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not provided
Affected status: yes
Allele origin:
germline
|
CeGaT Center for Human Genetics Tuebingen
Accession: SCV000493482.33
First in ClinVar: Jan 30, 2017 Last updated: Oct 20, 2024 |
Comment:
ERCC4: PM3:Very Strong, PM2, PS3:Supporting
Number of individuals with the variant: 12
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Pathogenic
(May 16, 2024)
|
criteria provided, single submitter
Method: clinical testing
|
Fanconi anemia complementation group Q
Affected status: unknown
Allele origin:
germline
|
St. Jude Molecular Pathology, St. Jude Children's Research Hospital
Accession: SCV005402101.1
First in ClinVar: Nov 24, 2024 Last updated: Nov 24, 2024 |
Comment:
The ERCC4 c.2395C>T (p.Arg799Trp) missense change has a maximum subpopulation frequency of 0.081% in gnomAD v2.1.1 (https://gnomad.broadinstitute.org/). The in silico tool REVEL is inconclusive about … (more)
The ERCC4 c.2395C>T (p.Arg799Trp) missense change has a maximum subpopulation frequency of 0.081% in gnomAD v2.1.1 (https://gnomad.broadinstitute.org/). The in silico tool REVEL is inconclusive about a pathogenic or benign effect of this variant on protein function, however in vitro functional assays in LCLs (Epstein–Barr virus transformed lymphoblastoid cell lines) and fibroblasts have shown that this variant causes reduced protein expression of nuclear ERCC4 which is attributed to protein mislocalization and can result in decreased cell survival and DNA replication after ultraviolet light exposure (PMID: 20221251, 29105242, 9579555). This variant has been reported in over ten individuals affected with xeroderma pigmentosum (PMID: 8797827, 9579555, 23623389, 21228398, 28431612, 29892709). In addition, it has been reported in three individuals with autosomal recessive cerebellar ataxia with mild pigmentation of exposed skin areas and/or an equivocal history of pathological sunburn (PMID: 29403087), one individual with sporadic ataxia (PMID: 31692161), two individuals with head and neck squamous cell carcinoma (PMID: 28678401), one individual with sporadic pancreatic adenocarcinoma (PMID: 28767289), one individual with Cockayne syndrome (PMID: 29105242), and one individual with colorectal cancer (PMID: 31871297). This variant is also known as p.Arg788Trp in the literature. In summary, this variant meets criteria to be classified as pathogenic. (less)
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Pathogenic
(May 01, 1998)
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no assertion criteria provided
Method: literature only
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XERODERMA PIGMENTOSUM, TYPE F
Affected status: not provided
Allele origin:
germline
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OMIM
Accession: SCV000038327.3
First in ClinVar: Apr 04, 2013 Last updated: Apr 07, 2019 |
Comment on evidence:
For discussion of the arg788-to-trp (R788W) mutation in the ERCC4 gene that was found in compound heterozygous state in a patient with xeroderma pigmentosum type … (more)
For discussion of the arg788-to-trp (R788W) mutation in the ERCC4 gene that was found in compound heterozygous state in a patient with xeroderma pigmentosum type F (XPF; 278760) by Sijbers et al. (1996), see 133520.0001. Sijbers et al. (1998) found the R788W mutation in homozygous state in a second Caucasian patient with XPF. Mild ocular photophobia had been present from childhood, and acute skin reactions occurred upon exposure to sunlight. Basal and squamous cell carcinomas developed after his twenty-seventh year. In his late forties, progressive neurologic symptoms emerged, which included intellectual decline, mild chorea and ataxia, and marked cerebral and cerebellar atrophy. Sijbers et al. (1998) stated that such neurologic abnormalities were unusual in XPF, having been described in only 1 of 17 other XPF individuals. The patient's 5-fold reduced activity of nucleotide excision repair in cultured cells, combined with moderately affected cell survival and DNA replication after UV exposure, was typical of XPF. Biochemical, genetic, and clinical data indicated the presence of considerable residual repair activity, strongly suggesting that the R788W mutation is leaky. The 2 Caucasian patients carrying this mutation were not known to be related. (less)
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Pathogenic
(Apr 04, 2019)
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no assertion criteria provided
Method: literature only
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XFE PROGEROID SYNDROME
Affected status: not provided
Allele origin:
germline
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OMIM
Accession: SCV000897688.1
First in ClinVar: Apr 08, 2019 Last updated: Apr 08, 2019 |
Comment on evidence:
In a 35-year-old woman with XFE progeroid syndrome (XFEPS; 610965), Mori et al. (2018) identified compound heterozygosity for 2 mutations in the ERCC4 gene: a … (more)
In a 35-year-old woman with XFE progeroid syndrome (XFEPS; 610965), Mori et al. (2018) identified compound heterozygosity for 2 mutations in the ERCC4 gene: a c.2395C-T transition (c.2395C-T, NM_005236.2), resulting in an arg799-to-trp (R799W) substitution, and a 5,656-bp deletion (c.388+1164_792+795del; 133520.0012), resulting in a frameshift and a premature termination codon (Gly130AspfsTer18). (less)
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Likely pathogenic
(-)
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no assertion criteria provided
Method: research
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Atypical Werner Syndrome
Affected status: yes
Allele origin:
unknown
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University of Washington Center for Mendelian Genomics, University of Washington
Accession: SCV001197907.1
First in ClinVar: Apr 15, 2020 Last updated: Apr 15, 2020 |
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Likely pathogenic
(Mar 04, 2021)
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no assertion criteria provided
Method: case-control
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Carcinoma of pancreas
Affected status: yes
Allele origin:
germline
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CZECANCA consortium
Accession: SCV001593122.1
First in ClinVar: May 14, 2021 Last updated: May 14, 2021 |
Number of individuals with the variant: 4
Ethnicity/Population group: Slavic
Geographic origin: Czech Republic
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Likely pathogenic
(Feb 22, 2024)
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no assertion criteria provided
Method: clinical testing
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ERCC4-related condition
Affected status: unknown
Allele origin:
germline
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PreventionGenetics, part of Exact Sciences
Accession: SCV004740866.2
First in ClinVar: Mar 16, 2024 Last updated: Oct 08, 2024 |
Comment:
The ERCC4 c.2395C>T variant is predicted to result in the amino acid substitution p.Arg799Trp. This variant has been reported in the compound heterozygous and homozygous … (more)
The ERCC4 c.2395C>T variant is predicted to result in the amino acid substitution p.Arg799Trp. This variant has been reported in the compound heterozygous and homozygous state in patients affected with xeroderma pigmentosum (F) (reported as R788W in Sijbers et al. 1996. PubMed ID: 8797827 and Sijbers et al. 1998. PubMed ID: 9579555; HGMD# CM960516 in Table S9 in Bell et al. 2011. PubMed ID: 21228398; Doi et al. 2018. PubMed ID: 29403087; Shanbhag et al. 2018. PubMed ID: 29892709; Marelli et al. 2016. PubMed ID: 27528516; Kashiyama et al. 2013. PubMed ID: 23623389). This variant has also been identified in individuals with pancreatic adenocarcinoma (Shindo et al. 2017. PubMed ID: 28767289), head and neck squamous cell carcinoma (Chandrasekharappa et al. 2017. PubMed ID: 28678401), and colorectal cancer (Goldstein et al. 2020. PubMed ID: 31871297), but was also found in healthy control individuals (Table 2, Dobbins et al. 2016. PubMed ID: 27356891; Bodian et al. 2014. PubMed ID: 24728327). In Dobbins et al. 2016 paper the authors conclude that they did not observe a significant difference in the frequency of pathogenic variants between cases and controls in their cohort. This variant is reported in 0.081% of alleles in individuals of European (non-Finnish) descent in gnomAD. Based on the available evidence, this variant is interpreted as likely pathogenic for autosomal recessive ERCC4-related disease. (less)
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not provided
(Sep 19, 2013)
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no classification provided
Method: reference population
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AllHighlyPenetrant
Affected status: unknown
Allele origin:
germline
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ITMI
Accession: SCV000084973.1
First in ClinVar: Jun 09, 2014 Last updated: Jun 09, 2014
Comment:
Please see associated publication for description of ethnicities
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Observation 1:
Ethnicity/Population group: Whole_cohort
Observation 2:
Ethnicity/Population group: African
Observation 3:
Ethnicity/Population group: African_European
Observation 4:
Ethnicity/Population group: Central_Asian
Observation 5:
Ethnicity/Population group: East_Asian
Observation 6:
Ethnicity/Population group: European
Observation 7:
Ethnicity/Population group: Hispanic
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not provided
(-)
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no classification provided
Method: phenotyping only
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Fanconi anemia complementation group Q
Xeroderma pigmentosum, group F Cockayne syndrome
Explanation for multiple conditions: Uncertain.
The variant was classified for several related diseases, possibly a spectrum of disease; the variant may be associated with one or more the diseases.
Affected status: unknown
Allele origin:
unknown
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GenomeConnect - Invitae Patient Insights Network
Accession: SCV001749397.2
First in ClinVar: Jul 18, 2021 Last updated: Jun 17, 2024 |
Comment:
Variant interpreted as Pathogenic and reported on 12-16-2019 by Invitae. GenomeConnect-Invitae Patient Insights Network assertions are reported exactly as they appear on the patient-provided report … (more)
Variant interpreted as Pathogenic and reported on 12-16-2019 by Invitae. GenomeConnect-Invitae Patient Insights Network assertions are reported exactly as they appear on the patient-provided report from the testing laboratory. Registry team members make no attempt to reinterpret the clinical significance of the variant. Phenotypic details are available under supporting information. (less)
Clinical Features:
Skin basal cell carcinoma (present)
Indication for testing: Diagnostic
Age: 50-59 years
Sex: female
Testing laboratory: Invitae
Date variant was reported to submitter: 2019-12-16
Testing laboratory interpretation: Pathogenic
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Germline Functional Evidence
There is no functional evidence in ClinVar for this variation. If you have generated functional data for this variation, please consider submitting that data to ClinVar. |
Citations for germline classification of this variant
HelpTitle | Author | Journal | Year | Link |
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A diagnostic ceiling for exome sequencing in cerebellar ataxia and related neurological disorders. | Ngo KJ | Human mutation | 2020 | PMID: 31692161 |
Neurodegeneration as the presenting symptom in 2 adults with xeroderma pigmentosum complementation group F. | Shanbhag NM | Neurology. Genetics | 2018 | PMID: 29892709 |
Cerebellar ataxia-dominant phenotype in patients with ERCC4 mutations. | Doi H | Journal of human genetics | 2018 | PMID: 29403087 |
ERCC4 variants identified in a cohort of patients with segmental progeroid syndromes. | Mori T | Human mutation | 2018 | PMID: 29105242 |
Deleterious Germline Mutations in Patients With Apparently Sporadic Pancreatic Adenocarcinoma. | Shindo K | Journal of clinical oncology : official journal of the American Society of Clinical Oncology | 2017 | PMID: 28767289 |
Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50. | Chandrasekharappa SC | Cancer | 2017 | PMID: 28678401 |
Xeroderma pigmentosum complementation group F: A rare cause of cerebellar ataxia with chorea. | Carré G | Journal of the neurological sciences | 2017 | PMID: 28431612 |
Mini-Exome Coupled to Read-Depth Based Copy Number Variation Analysis in Patients with Inherited Ataxias. | Marelli C | Human mutation | 2016 | PMID: 27528516 |
Undefined familial colorectal cancer and the role of pleiotropism in cancer susceptibility genes. | Dobbins SE | Familial cancer | 2016 | PMID: 27356891 |
The ERCC1 and ERCC4 (XPF) genes and gene products. | Manandhar M | Gene | 2015 | PMID: 26074087 |
Germline variation in cancer-susceptibility genes in a healthy, ancestrally diverse cohort: implications for individual genome sequencing. | Bodian DL | PloS one | 2014 | PMID: 24728327 |
Malfunction of nuclease ERCC1-XPF results in diverse clinical manifestations and causes Cockayne syndrome, xeroderma pigmentosum, and Fanconi anemia. | Kashiyama K | American journal of human genetics | 2013 | PMID: 23623389 |
Physiological consequences of defects in ERCC1-XPF DNA repair endonuclease. | Gregg SQ | DNA repair | 2011 | PMID: 21612988 |
Carrier testing for severe childhood recessive diseases by next-generation sequencing. | Bell CJ | Science translational medicine | 2011 | PMID: 21228398 |
Mislocalization of XPF-ERCC1 nuclease contributes to reduced DNA repair in XP-F patients. | Ahmad A | PLoS genetics | 2010 | PMID: 20221251 |
Homozygous R788W point mutation in the XPF gene of a patient with xeroderma pigmentosum and late-onset neurologic disease. | Sijbers AM | The Journal of investigative dermatology | 1998 | PMID: 9579555 |
Xeroderma pigmentosum group F caused by a defect in a structure-specific DNA repair endonuclease. | Sijbers AM | Cell | 1996 | PMID: 8797827 |
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Text-mined citations for rs121913049 ...
HelpRecord last updated Nov 25, 2024
This date represents the last time this VCV record was updated. The update may be due to an update to one of the included submitted records (SCVs), or due to an update that ClinVar made to the variant such as adding HGVS expressions or a rs number. So this date may be different from the date of the “most recent submission” reported at the top of this page.