NM_001122740.1:c.1150C>G (p.Leu384Val) is a missense variant in ESR1 exon 6. It is absent from gnomAD v2.1, v4.1, and gnomAD-Canada v1.0 across all populations (PM2_Supporting).1 Multiple in silico predictors support a deleterious effect: REVEL score 0.863 and BayesDel score 0.279 both exceed their respective pathogenicity thresholds (PP3_Supporting).2 The variant is absent from ClinVar, COSMIC, and all population databases. No functional studies, case reports, cosegregation data, or de novo observations exist for this variant.3 PVS1 is not applicable as this is a missense variant that does not fall into the null-variant buckets per ClinGen SVI PVS1 recommendations (PMC6185798).4 This variant does not lie in a statistically significant mutational hotspot (cancerhotspots.org negative), and no pathogenic ClinVar variants cluster at residue Leu384. PM1 is not met.5 No publications were identified that mention NM_001122740.1:c.1150C>G. A targeted review of five ESR1 germline disease-context publications (PMID:15361840, PMID:25139996, PMID:41129222, PMID:22086303, PMID:26557847) confirmed none contain variant-specific evidence. Overall classification: Variant of Uncertain Significance (VUS). Two supporting-level pathogenic criteria (PM2_Supporting, PP3_Supporting) are met, which is insufficient to reach Likely Pathogenic under the generic ACMG/AMP 2015 classification rules (PMID:25741868). No benign criteria are met.6