PM2_Supporting is met: the variant is absent from gnomAD v4.1, meeting the VCEP threshold of <0.00002 allele frequency.1 PP3_Moderate is met: the HCI MAPP/PP2 Prior probability for p.Asp699Val is 0.8907, exceeding the VCEP PP3_Moderate threshold of >0.81.2 Multiple criteria could not be assessed due to absence of variant-specific data: PS3 (functional assays), PP1 (co-segregation), PP4 (tumor phenotype), BS2 (co-occurrence in trans), BS3 (benign functional evidence), BS4 (lack of co-segregation), and BP5 (tumor MSS/IHC data). The variant has not been observed in population databases and is predicted damaging by multiple in silico tools (REVEL 0.969, BayesDel 0.419), but no clinical case reports, tumor data, or functional studies have been identified to further support or refute pathogenicity.3