A published R104Q variant that is likely pathogenic has been identified in the PRICKLE1 gene. The R104Q variant has been previously reported as a homozygous variant in multiple unrelated individuals with progressive myoclonus epilepsy (PME)-ataxia syndrome; individuals in these families who were heterozygous for the variant were not affected (Bassuk et al., 2008). Functional studies suggest that the R104Q variant impairs protein function (Bassuk et al., 2008). The R104Q variant is not observed at a significant frequency in large population cohorts (Lek et al., 2016; 1000 Genomes Consortium et al., 2015; Exome Variant Server). The R104Q variant is a semi-conservative amino acid substitution, which may impact secondary protein structure as these residues differ in some properties. In silico analysis predicts this variant is probably damaging to the protein structure/function. However, this substitution occurs at a position that is not conserved. Therefore, this variant is likely pathogenic; however, the possibility that it is benign cannot be excluded.
ClinVar Genomic variation as it relates to human health
NM_153026.3(PRICKLE1):c.311G>A (p.Arg104Gln)
Germline
Classification
Help
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.
(10)
Help
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/Likely pathogenic
10
criteria provided, multiple submitters, no conflicts
Somatic
No data submitted for somatic clinical impact
Somatic
No data submitted for oncogenicity
Variant Details
- Identifiers
-
NM_153026.3(PRICKLE1):c.311G>A (p.Arg104Gln)
Variation ID: 2283 Accession: VCV000002283.15
- Type and length
-
single nucleotide variant, 1 bp
- Location
-
Cytogenetic: 12q12 12: 42469523 (GRCh38) [ NCBI UCSC ] 12: 42863325 (GRCh37) [ NCBI UCSC ]
- Timeline in ClinVar
-
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 Apr 4, 2013 Sep 8, 2024 Apr 5, 2024 - HGVS
-
... more HGVS ... less HGVSNucleotide Protein Molecular
consequenceNM_153026.3:c.311G>A MANE Select Help Transcripts from the Matched Annotation from the NCBI and EMBL-EBI (MANE) collaboration.
NP_694571.2:p.Arg104Gln missense NM_001144881.2:c.311G>A NP_001138353.1:p.Arg104Gln missense NM_001144882.2:c.311G>A NP_001138354.1:p.Arg104Gln missense NM_001144883.2:c.311G>A NP_001138355.1:p.Arg104Gln missense NC_000012.12:g.42469523C>T NC_000012.11:g.42863325C>T NG_012965.1:g.125248G>A Q96MT3:p.Arg104Gln - Protein change
- R104Q
- Other names
- -
- Canonical SPDI
- NC_000012.12:42469522:C:T
-
Functional
consequence HelpThe effect of the variant on RNA or protein function, based on experimental evidence from submitters.
- -
-
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.
- -
-
Allele frequency
Help
The frequency of the allele represented by this VCV record.
-
Exome Aggregation Consortium (ExAC) 0.00001
The Genome Aggregation Database (gnomAD), exomes 0.00001
The Genome Aggregation Database (gnomAD) 0.00003
Trans-Omics for Precision Medicine (TOPMed) 0.00003
- 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 | ||
|---|---|---|---|---|---|---|
| HI score
Help
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. |
|||
| LOC130007700 | - | - | - | GRCh38 | - | 16 |
| PRICKLE1 | - | - |
GRCh38 GRCh37 |
480 | 603 | |
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. |
|---|---|---|---|---|
| Pathogenic/Likely pathogenic (9) |
criteria provided, multiple submitters, no conflicts
|
Apr 5, 2024 | RCV000002373.20 | |
| Likely pathogenic (1) |
criteria provided, single submitter
|
Jan 19, 2017 | RCV000431708.1 |
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. |
|
|---|---|---|---|---|---|
|
Likely pathogenic
(Jan 19, 2017)
|
criteria provided, single submitter
Method: clinical testing
|
Not Provided
Affected status: yes
Allele origin:
germline
|
GeneDx
Accession: SCV000520887.3
First in ClinVar: Mar 08, 2017 Last updated: Mar 08, 2017 |
Comment:
A published R104Q variant that is likely pathogenic has been identified in the PRICKLE1 gene. The R104Q variant has been previously reported as a homozygous … (more)
A published R104Q variant that is likely pathogenic has been identified in the PRICKLE1 gene. The R104Q variant has been previously reported as a homozygous variant in multiple unrelated individuals with progressive myoclonus epilepsy (PME)-ataxia syndrome; individuals in these families who were heterozygous for the variant were not affected (Bassuk et al., 2008). Functional studies suggest that the R104Q variant impairs protein function (Bassuk et al., 2008). The R104Q variant is not observed at a significant frequency in large population cohorts (Lek et al., 2016; 1000 Genomes Consortium et al., 2015; Exome Variant Server). The R104Q variant is a semi-conservative amino acid substitution, which may impact secondary protein structure as these residues differ in some properties. In silico analysis predicts this variant is probably damaging to the protein structure/function. However, this substitution occurs at a position that is not conserved. Therefore, this variant is likely pathogenic; however, the possibility that it is benign cannot be excluded. (less)
|
|
|
Likely pathogenic
(Aug 18, 2020)
|
criteria provided, single submitter
Method: clinical testing
|
Epilepsy, progressive myoclonic, 1B
Affected status: yes
Allele origin:
germline
|
Al Jalila Children’s Genomics Center, Al Jalila Childrens Speciality Hospital
Accession: SCV001984660.1
First in ClinVar: Oct 30, 2021 Last updated: Oct 30, 2021
Comment:
The p. Arg104Gln missense variant in PRICKLE1 has been previously reported in the homozygous in at least 3 unrelated families with progressive myoclonus epilepsy-ataxia (PME) … (more)
The p. Arg104Gln missense variant in PRICKLE1 has been previously reported in the homozygous in at least 3 unrelated families with progressive myoclonus epilepsy-ataxia (PME) syndrome (PMID: 18976727). Functional studies suggest that this variant disrupts protein function and subcellular localization (PMID: 18976727). The p.Arg104Gln variant was also identified in 5/282818 (0.0018% 0 homozygotes) total alleles in the Genome Aggregation Database. Computational prediction tools and conservation analysis suggest an impact to protein function. In summary this variant meets our criteria to be classified as likely pathogenic. (less)
|
|
|
|
Pathogenic
(-)
|
criteria provided, single submitter
Method: clinical testing
|
Epilepsy, progressive myoclonic, 1B
(Autosomal recessive inheritance)
Affected status: yes
Allele origin:
germline
|
Lifecell International Pvt. Ltd
Accession: SCV003924042.1
First in ClinVar: May 13, 2023 Last updated: May 13, 2023 |
Comment:
A Heterozygous Missense variant c.311G>A in Exon 4 of the PRICKLE1 gene that results in the amino acid substitution p.Arg104Gln was identified. The observed variant … (more)
A Heterozygous Missense variant c.311G>A in Exon 4 of the PRICKLE1 gene that results in the amino acid substitution p.Arg104Gln was identified. The observed variant has a maximum allele frequency of 0.00001/0.00006% in gnomAD exomes and genomes, respectively. The severity of the impact of this variant on the protein is medium, based on the effect of the protein and REVEL score . Rare Exome Variant Ensemble Learner (REVEL) is an ensembl method for predicting the pathogenicity of missense variants based on a combination of scores from 13 individual tools: MutPred, FATHMM v2.3, VEST 3.0, PolyPhen-2, SIFT, PROVEAN, MutationAssessor, MutationTaster, LRT, GERP++, SiPhy, phyloP, and phastCons. The REVEL score for an individual missense variant can range from 0 to 1, with higher scores reflecting greater likelihood that the variant is disease-causing. ClinVar has also classified this variant as LikelyPathogenic. The p. Arg104Gln missense variant in PRICKLE1 has been previously reported in the homozygous in at least 3 unrelated families with progressive myoclonus epilepsy-ataxia (PME) syndrome. Functional studies suggest that this variant disrupts protein function and subcellular localization (Bassuk AG et al., 2008). Based on the above evidence this variant has been classified as Pathogenic according to the ACMG guidelines. (less)
Ethnicity/Population group: Asian
Geographic origin: India
|
|
|
Pathogenic
(Nov 29, 2023)
|
criteria provided, single submitter
Method: clinical testing
|
Epilepsy, progressive myoclonic, 1B
Affected status: unknown
Allele origin:
germline
|
Women's Health and Genetics/Laboratory Corporation of America, LabCorp
Accession: SCV004223247.1
First in ClinVar: Jan 06, 2024 Last updated: Jan 06, 2024 |
Comment:
Variant summary: PRICKLE1 c.311G>A (p.Arg104Gln) results in a conservative amino acid change located in the PET domain (IPR010442) of the encoded protein sequence. Four of … (more)
Variant summary: PRICKLE1 c.311G>A (p.Arg104Gln) results in a conservative amino acid change located in the PET domain (IPR010442) 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 1.2e-05 in 251416 control chromosomes. c.311G>A has been reported in the literature in multiple individuals affected with Epilepsy, progressive myoclonic, 1B (Bassuk_2008). 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 suggesting it impacts protein function (Bassuk_2008). The following publications have been ascertained in the context of this evaluation (PMID: 18976727, 32214227, 35040250). Four submitters have cited clinical-significance assessments for this variant to ClinVar after 2014. All submitters classified the variant as pathogenic/likely pathogenic. Based on the evidence outlined above, the variant was classified as pathogenic. (less)
|
|
|
Pathogenic
(Sep 14, 2022)
|
criteria provided, single submitter
Method: clinical testing
|
Epilepsy, progressive myoclonic, 1B
Affected status: unknown
Allele origin:
germline
|
Labcorp Genetics (formerly Invitae), Labcorp
Accession: SCV003481216.2
First in ClinVar: Feb 07, 2023 Last updated: Feb 14, 2024 |
Comment:
For these reasons, this variant has been classified as Pathogenic. Experimental studies have shown that this missense change affects PRICKLE1 function (PMID: 18976727). Advanced modeling … (more)
For these reasons, this variant has been classified as Pathogenic. Experimental studies have shown that this missense change affects PRICKLE1 function (PMID: 18976727). 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 PRICKLE1 protein function. ClinVar contains an entry for this variant (Variation ID: 2283). This missense change has been observed in individuals with progressive myoclonic epilepsy (PMID: 18976727, 32214227). It has also been observed to segregate with disease in related individuals. This variant is present in population databases (rs113994140, gnomAD 0.005%). This sequence change replaces arginine, which is basic and polar, with glutamine, which is neutral and polar, at codon 104 of the PRICKLE1 protein (p.Arg104Gln). (less)
|
|
|
Pathogenic
(Mar 29, 2024)
|
criteria provided, single submitter
Method: clinical testing
|
Epilepsy, progressive myoclonic, 1B
Affected status: unknown
Allele origin:
germline
|
Center for Genomic Medicine, King Faisal Specialist Hospital and Research Center
Accession: SCV004807497.1
First in ClinVar: Apr 06, 2024 Last updated: Apr 06, 2024 |
|
|
|
Likely pathogenic
(Apr 05, 2024)
|
criteria provided, single submitter
Method: clinical testing
|
Epilepsy, progressive myoclonic, 1B
Affected status: yes
Allele origin:
germline
|
Greenwood Genetic Center Diagnostic Laboratories, Greenwood Genetic Center
Accession: SCV005200845.1
First in ClinVar: Sep 08, 2024 Last updated: Sep 08, 2024 |
Comment:
PS3, PM2, PM3, PP1
|
|
|
Pathogenic
(Nov 01, 2008)
|
no assertion criteria provided
Method: literature only
|
EPILEPSY, PROGRESSIVE MYOCLONIC, 1B
Affected status: not provided
Allele origin:
germline
|
OMIM
Accession: SCV000022531.3
First in ClinVar: Apr 04, 2013 Last updated: Sep 25, 2019 |
Comment on evidence:
In affected members of 3 unrelated consanguineous families with progressive myoclonic epilepsy-1B (EPM1B; 612437), Bassuk et al. (2008) identified a homozygous 311G-A transition in the … (more)
In affected members of 3 unrelated consanguineous families with progressive myoclonic epilepsy-1B (EPM1B; 612437), Bassuk et al. (2008) identified a homozygous 311G-A transition in the PRICKLE1 gene, resulting in an arg104-to-gln (R104Q) substitution in a highly conserved region. The mutation was not detected in 1,354 control individuals. In vitro functional expression studies showed that mutant PRICKLE1 failed to bind REST (600571) and blocked transport of REST out of the nucleus, resulting in constitutive activation of REST and inappropriate downregulation of REST target genes. (less)
|
|
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Likely pathogenic
(Aug 01, 2019)
|
no assertion criteria provided
Method: research
|
Epilepsy, progressive myoclonic, 1B
Affected status: yes
Allele origin:
germline
|
Section for Clinical Neurogenetics, University of Tübingen
Accession: SCV001156099.1
First in ClinVar: Apr 06, 2020 Last updated: Apr 06, 2020 |
|
|
|
not provided
(-)
|
no classification provided
Method: literature only
|
Epilepsy, progressive myoclonic, 1B
Affected status: not provided
Allele origin:
unknown
|
GeneReviews
Accession: SCV000041601.2
First in ClinVar: Apr 04, 2013 Last updated: Oct 01, 2022 |
|
Comment:
Comment:
A Heterozygous Missense variant c.311G>A in Exon 4 of the PRICKLE1 gene that results in the amino acid substitution p.Arg104Gln was identified. The observed variant has a maximum allele frequency of 0.00001/0.00006% in gnomAD exomes and genomes, respectively. The severity of the impact of this variant on the protein is medium, based on the effect of the protein and REVEL score . Rare Exome Variant Ensemble Learner (REVEL) is an ensembl method for predicting the pathogenicity of missense variants based on a combination of scores from 13 individual tools: MutPred, FATHMM v2.3, VEST 3.0, PolyPhen-2, SIFT, PROVEAN, MutationAssessor, MutationTaster, LRT, GERP++, SiPhy, phyloP, and phastCons. The REVEL score for an individual missense variant can range from 0 to 1, with higher scores reflecting greater likelihood that the variant is disease-causing. ClinVar has also classified this variant as LikelyPathogenic. The p. Arg104Gln missense variant in PRICKLE1 has been previously reported in the homozygous in at least 3 unrelated families with progressive myoclonus epilepsy-ataxia (PME) syndrome. Functional studies suggest that this variant disrupts protein function and subcellular localization (Bassuk AG et al., 2008). Based on the above evidence this variant has been classified as Pathogenic according to the ACMG guidelines.
Comment:
Variant summary: PRICKLE1 c.311G>A (p.Arg104Gln) results in a conservative amino acid change located in the PET domain (IPR010442) 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 1.2e-05 in 251416 control chromosomes. c.311G>A has been reported in the literature in multiple individuals affected with Epilepsy, progressive myoclonic, 1B (Bassuk_2008). 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 suggesting it impacts protein function (Bassuk_2008). The following publications have been ascertained in the context of this evaluation (PMID: 18976727, 32214227, 35040250). Four submitters have cited clinical-significance assessments for this variant to ClinVar after 2014. All submitters classified the variant as pathogenic/likely pathogenic. Based on the evidence outlined above, the variant was classified as pathogenic.
Comment:
For these reasons, this variant has been classified as Pathogenic. Experimental studies have shown that this missense change affects PRICKLE1 function (PMID: 18976727). 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 PRICKLE1 protein function. ClinVar contains an entry for this variant (Variation ID: 2283). This missense change has been observed in individuals with progressive myoclonic epilepsy (PMID: 18976727, 32214227). It has also been observed to segregate with disease in related individuals. This variant is present in population databases (rs113994140, gnomAD 0.005%). This sequence change replaces arginine, which is basic and polar, with glutamine, which is neutral and polar, at codon 104 of the PRICKLE1 protein (p.Arg104Gln).
Comment:
PS3, PM2, PM3, PP1
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. |
Comment:
A published R104Q variant that is likely pathogenic has been identified in the PRICKLE1 gene. The R104Q variant has been previously reported as a homozygous variant in multiple unrelated individuals with progressive myoclonus epilepsy (PME)-ataxia syndrome; individuals in these families who were heterozygous for the variant were not affected (Bassuk et al., 2008). Functional studies suggest that the R104Q variant impairs protein function (Bassuk et al., 2008). The R104Q variant is not observed at a significant frequency in large population cohorts (Lek et al., 2016; 1000 Genomes Consortium et al., 2015; Exome Variant Server). The R104Q variant is a semi-conservative amino acid substitution, which may impact secondary protein structure as these residues differ in some properties. In silico analysis predicts this variant is probably damaging to the protein structure/function. However, this substitution occurs at a position that is not conserved. Therefore, this variant is likely pathogenic; however, the possibility that it is benign cannot be excluded.
Comment:
A Heterozygous Missense variant c.311G>A in Exon 4 of the PRICKLE1 gene that results in the amino acid substitution p.Arg104Gln was identified. The observed variant has a maximum allele frequency of 0.00001/0.00006% in gnomAD exomes and genomes, respectively. The severity of the impact of this variant on the protein is medium, based on the effect of the protein and REVEL score . Rare Exome Variant Ensemble Learner (REVEL) is an ensembl method for predicting the pathogenicity of missense variants based on a combination of scores from 13 individual tools: MutPred, FATHMM v2.3, VEST 3.0, PolyPhen-2, SIFT, PROVEAN, MutationAssessor, MutationTaster, LRT, GERP++, SiPhy, phyloP, and phastCons. The REVEL score for an individual missense variant can range from 0 to 1, with higher scores reflecting greater likelihood that the variant is disease-causing. ClinVar has also classified this variant as LikelyPathogenic. The p. Arg104Gln missense variant in PRICKLE1 has been previously reported in the homozygous in at least 3 unrelated families with progressive myoclonus epilepsy-ataxia (PME) syndrome. Functional studies suggest that this variant disrupts protein function and subcellular localization (Bassuk AG et al., 2008). Based on the above evidence this variant has been classified as Pathogenic according to the ACMG guidelines.
Comment:
Variant summary: PRICKLE1 c.311G>A (p.Arg104Gln) results in a conservative amino acid change located in the PET domain (IPR010442) 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 1.2e-05 in 251416 control chromosomes. c.311G>A has been reported in the literature in multiple individuals affected with Epilepsy, progressive myoclonic, 1B (Bassuk_2008). 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 suggesting it impacts protein function (Bassuk_2008). The following publications have been ascertained in the context of this evaluation (PMID: 18976727, 32214227, 35040250). Four submitters have cited clinical-significance assessments for this variant to ClinVar after 2014. All submitters classified the variant as pathogenic/likely pathogenic. Based on the evidence outlined above, the variant was classified as pathogenic.
Comment:
For these reasons, this variant has been classified as Pathogenic. Experimental studies have shown that this missense change affects PRICKLE1 function (PMID: 18976727). 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 PRICKLE1 protein function. ClinVar contains an entry for this variant (Variation ID: 2283). This missense change has been observed in individuals with progressive myoclonic epilepsy (PMID: 18976727, 32214227). It has also been observed to segregate with disease in related individuals. This variant is present in population databases (rs113994140, gnomAD 0.005%). This sequence change replaces arginine, which is basic and polar, with glutamine, which is neutral and polar, at codon 104 of the PRICKLE1 protein (p.Arg104Gln).
Comment:
PS3, PM2, PM3, PP1
Citations for germline classification of this variant
Help| Title | Author | Journal | Year | Link |
|---|---|---|---|---|
| Whole exome sequencing identifies potential candidate genes for spina bifida derived from mouse models. | Wang C | American journal of medical genetics. Part A | 2022 | PMID: 35040250 |
| PRICKLE1-Related Disorders. | Adam MP | - | 2022 | PMID: 20301774 |
| First-line exome sequencing in Palestinian and Israeli Arabs with neurological disorders is efficient and facilitates disease gene discovery. | Hengel H | European journal of human genetics : EJHG | 2020 | PMID: 32214227 |
| A homozygous mutation in human PRICKLE1 causes an autosomal-recessive progressive myoclonus epilepsy-ataxia syndrome. | Bassuk AG | American journal of human genetics | 2008 | PMID: 18976727 |
Text-mined citations for rs113994140 ...
HelpThese citations are identified by LitVar using
the rs number, so they may include citations for more than one variant
at this location. Please review the LitVar results carefully for your
variant of interest.
Record last updated Sep 29, 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.