NM_000535.7:c.2380C>T (p.Pro794Ser) is a missense variant in exon 14 of PMS2. This variant is extremely rare in population databases: gnomAD v4.1 grpmax filtering allele frequency is 3.67e-06 (5/1,604,584 alleles), meeting the VCEP PM2_Supporting threshold of <0.00002.1 The HCI prior probability for pathogenicity is 0.8253, exceeding the VCEP PP3_Moderate threshold of >0.81, supporting a deleterious computational prediction.2 No functional studies, segregation data, tumor pathology data, or de novo observations are available for this variant. The variant is absent from COSMIC and OncoKB reports no variant-specific functional evidence.3 In ClinVar, this variant is classified as Uncertain Significance by 12 clinical laboratories and as Benign by 1 laboratory (ClinVar ID 220740), with no expert panel classification.4 Applying the ClinGen InSiGHT PMS2 VCEP v2.0.0 combining criteria: PM2_Supporting (1 point) and PP3_Moderate (2 points) are met. These do not reach any pathogenic classification tier (requires ≥1 Strong or ≥3 Moderate for Likely Pathogenic, or ≥2 Supporting for Likely Benign). The variant remains a Variant of Uncertain Significance.5