PS2
No de novo occurrence with confirmed maternity and paternity was identified for this variant in any reviewed source.
PS3
No well-established in vitro or in vivo functional studies demonstrating a damaging effect specific to NM_024642.5:c.5G>A were identified in the reviewed literature.
PS4
The variant has been observed in one homozygous case (26-year-old female with grade 1 endometrioid endometrial carcinoma, PMID:30886832) and reported in one gastric adenocarcinoma case (PMID:32963463, per ClinVar submission SCV002655098).
PM1
Variant does not lie within a statistically significant mutational hotspot (cancerhotspots.org negative), and no well-established critical or well-characterized functional domain has been defined at amino acid position 2 of GALNT12.
PM6
No de novo observation (without confirmation of maternity and paternity) was identified for this variant in any reviewed source.
PP1
No cosegregation data with disease in multiple affected family members are available for this variant.
PP3
SpliceAI predicts no splicing impact (max delta score = 0.00).
PP4
Although the variant has been observed in a 26-year-old homozygous patient with grade 1 endometrioid endometrial carcinoma (PMID:30886832) and in a gastric adenocarcinoma patient (PMID:32963463), these cancer phenotypes are not highly specific for GALNT12-related disease.
PP5
The variant is classified as Uncertain Significance in ClinVar (VariationID: 1061178) by two clinical laboratories (Ambry Genetics, Labcorp/Invitae).