This variant is absent from all population databases (gnomAD v2.1, v4.1, gnomAD-Canada), meeting PM2_Supporting under the ATM VCEP v1.5 threshold of ≤0.001%.1 SpliceAI predicts no splice impact (max delta 0.01), meeting BP4_Supporting under the ATM VCEP v1.5 splicing threshold of ≤0.1. REVEL is unavailable for this indel variant.2 The same amino acid change p.(Asp1371Asn) exists via c.4111G>A, classified as Uncertain Significance in ClinVar. The VCEP functional supplement (Suppl_TableS1, PMID 40580951) computationally predicts the D1371N change as 'Functional' via DeepATM, but this does not constitute experimental functional evidence for PS3 or BS3.3 One pathogenic supporting criterion (PM2_Supporting) and one benign supporting criterion (BP4_Supporting) are met. Per ACMG/AMP 2015 combination rules (Rule31), >=1 benign supporting and >=1 pathogenic supporting results in Uncertain Significance with conflicting evidence.4