The variant NM_001412.4:c.25G>C (p.Gly9Arg) lies within the N-terminal tail (NTT) of EIF1AX, a critical functional domain for translation initiation complex stability, satisfying PM1 at moderate strength.1 Functional studies demonstrate that p.Gly9Arg directly increases affinity for EIF5 and elevates nascent protein synthesis, consistent with a gain-of-function effect on the translation pre-initiation complex, supporting PS3 at moderate strength.2 The variant is absent from all population databases (gnomAD v2.1, v4.1, gnomAD-Canada), supporting PM2 at supporting strength.3 Multiple in silico tools predict a benign effect: SpliceAI delta score is 0.02 (no splicing impact) and BayesDel score is -0.100602 (benign range), supporting BP4 at supporting strength.4 The variant has been reported in somatic cancers (COSMIC, n=4) and is classified as Likely Oncogenic by OncoKB, confirming its oncogenic potential. However, as a germline variant, its clinical significance remains uncertain in the absence of germline case data.5