Evidence Repository - Clinical Genome Resources

The ClinGen Evidence Repository is an FDA-recognized human genetic variant database containing expert-curated assertions regarding variants' pathogenicity and supporting evidence summaries. [Disclaimer]

Variant: NM_000152.5(GAA):c.1551+1G>T

Curation Version - 1.0
Curation History
JSON LD for Version 1.0

CA8815365

555986 (ClinVar)

Gene: GAA

Condition: glycogen storage disease II

Inheritance Mode: Autosomal recessive inheritance

Link to MONDO

UUID: a5bdd3e3-b15a-429e-95bd-36cc1672655e

Approved on: 2025-05-20

Published on: 2025-05-20

HGVS expressions

NM_000152.5:c.1551+1G>T

NM_000152.5(GAA):c.1551+1G>T

NC_000017.11:g.80110841G>T

CM000679.2:g.80110841G>T

NC_000017.10:g.78084640G>T

CM000679.1:g.78084640G>T

NC_000017.9:g.75699235G>T

NG_009822.1:g.14286G>T

ENST00000570803.6:c.1551+1G>T

ENST00000572080.2:c.1551+1G>T

ENST00000577106.6:c.1551+1G>T

ENST00000302262.8:c.1551+1G>T

ENST00000302262.7:c.1551+1G>T

ENST00000390015.7:c.1551+1G>T

NM_000152.3:c.1551+1G>T

NM_001079803.1:c.1551+1G>T

NM_001079804.1:c.1551+1G>T

NM_000152.4:c.1551+1G>T

NM_001079803.2:c.1551+1G>T

NM_001079804.2:c.1551+1G>T

NM_001079803.3:c.1551+1G>T

NM_001079804.3:c.1551+1G>T

Pathogenic

PVS1 PP4 PM2_Supporting PM3 PS1_Supporting

Evidence Links 0

Expert Panel

Lysosomal Diseases VCEP

Criteria Specification Information

Criteria Specification: ClinGen Lysosomal Storage Disorders Variant Curation Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines Version 2

PDF

Criteria Specification Approval History

Criteria Specifications for this VCEP

Evidence submitted by expert panel

Lysosomal Diseases VCEP

The NM_000152.5:c.1551+1G>T variant alters the donor splice site of intron 10 in GAA. RT-PCR in fibroblasts revealed that this variant results in skipping of exon 10, with low levels of normal splicing (PMID 25243733). Skipping of exon 10 causes and in frame loss of 38 amino acids, encompassing part of the GAA catalytic barrel, and including two residues, Trp481 and Trp516, which are part of the active site (PMIDs 1856189, 22253258; DOI 10.1101/212837). Therefore, loss of this exon is expected to abolish GAA activity (PVS1). At least four probands and one sibling with this variant have been reported; for 3 individuals, documented GAA activity is available in fibroblasts or dried blood spot and is in the affected range (PMID 25243733, 25703594) (PP4_Moderate). Three of these probands, each with late-onset Pompe disease, are compound heterozygous for the variant and another variant in GAA that has been classified as pathogenic for Pompe disease by the ClinGen LD VCEP. The phase is unconfirmed in all cases. The second variant is either c.1942G>A (p.Gly648Ser) (ClinVar Variation ID: 188902) (PMID: 31606152, 0.5 points) or c.-32-13T>G (ClinVar Variation ID: 4027) (2 patients and one sibling, PMID: 25703594, 30155607; 2 x 0.5 points). Another patient is compound heterozygous for the variant and c.1256A>T (p.Asp419Val) (PMID: 25243733, 27623443). The allelic data from this patient will be used in the assessment of p.Asp419Val and is not included here in order to avoid circular logic. Total 1.5 points (PM3). The highest population minor allele frequency in gnomAD v4.1.0. is 0.00002228 in the East Asian population, which is lower than the ClinGen LD VCEP threshold (<0.001) for PM2_Supporting, meeting this criterion (PM2_Supporting). Additional variants in the same splice region have been classified as pathogenic by the ClinGen LD VCEP including c.1551+1G>A (ClinVar Variation ID: 1065143), c.1551+1G>C (ClinVar Variation ID: 554983), and c.1551+3_1551+6del (aka c.1551+1_1551+4del) (PS1_Supporting; PMID: 37352859). There is a ClinVar entry for this variant (Variation ID: 555986). In summary, this variant meets the criteria to be classified as pathogenic for Pompe disease. GAA-specific ACMG/AMP criteria met, as specified by the ClinGen LD VCEP (Specifications Version 2.0.0.): PVS1, PM3, PP4_Moderate, PS1_Supporting, PM2_Supporting. (Classification approved by the ClinGen Lysosomal Diseases Variant Curation Expert Panel on May 20, 2025)

PVS1

PP4

At least four probands and one sibling with this variant have been reported; for 3 individuals, documented GAA activity is available in fibroblasts or dried blood spot and is in the affected range (PMID 25243733, 25703594) (PP4_Moderate).

PM2_Supporting

The highest population minor allele frequency in gnomAD v4.1.0. is 0.00002228 in the East Asian population, which is lower than the ClinGen LD VCEP threshold (<0.001) for PM2_Supporting, meeting this criterion.

PM3

Three probands, with late-onset Pompe disease, are compound heterozygous for the variant and another variant in GAA that has been classified as pathogenic for Pompe disease by the ClinGen LD VCEP. The phase is unconfirmed in all cases. The second variant is either c.1942G>A (p.Gly648Ser) (ClinVar Variation ID: 188902) (PMID: 31606152, 0.5 points) or c.-32-13T>G (ClinVar Variation ID: 4027) (2 patients and one sibling, PMID: 25703594, 30155607; 2 x 0.5 points). Another patient is compound heterozygous for the variant and c.1256A>T (p.Asp419Val) (PMID: 25243733, 27623443). The allelic data from this patient will be used in the assessment of p.Asp419Val and is not included here in order to avoid circular logic. Total 1.5 points (PM3)

PS1_Supporting

Additional variants in the same splice region have been classified as pathogenic by the ClinGen LD VCEP including c.1551+1G>A (ClinVar Variation ID: 1065143), c.1551+1G>C (ClinVar Variation ID: 554983), and c.1551+3_1551+6del (aka c.1551+1_1551+4del) (PS1_Supporting; PMID: 37352859).

Curation History

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