NM_024675.4:c.886dupA (p.Met296AsnfsTer7) is a frameshift duplication in exon 4 of PALB2 that introduces a premature termination codon predicted to trigger nonsense-mediated decay, meeting PVS1 at very strong strength under the ClinGen PALB2 VCEP v1.2.0.1 The variant is present in gnomAD v4.1 at an overall frequency of 0.00031% (5/1,613,880 alleles, no homozygotes), below the PALB2 VCEP PM2_Supporting threshold of 0.000333%, satisfying PM2 at supporting strength.2 The premature termination codon at residue 302 lies upstream of p.Tyr1183, the most C-terminal known pathogenic variant in PALB2, satisfying PM5_Supporting under the PALB2 VCEP.3 Under the ACMG/AMP 2015 combining rules adopted by the PALB2 VCEP, one Very Strong (PVS1) plus two Supporting (PM2, PM5) criteria satisfies Rule 4, yielding a classification of Pathogenic.4