The c.182A>G (p.Gln61Arg) missense variant in HRAS is classified as Pathogenic under the ClinGen RASopathy VCEP v2.3.0 framework.1 PS1 (Strong): p.Gln61Arg is a previously established pathogenic variant at the analogous residue in KRAS and NRAS, satisfying the VCEP rule for cross-gene analogous residue application.2 PM1 (Moderate): The variant falls within the Switch II domain (SW2, AA 57-64), a VCEP-defined critical functional domain essential for GTP hydrolysis and GAP interaction. Residue Q61 is a statistically significant cancer hotspot (cancerhotspots.org) with 417 somatic occurrences in COSMIC.3 PM5 (Moderate): At least one other pathogenic missense change at codon 61 (e.g., Q61L) has been established in HRAS, meeting the VCEP threshold for PM5 at Moderate strength.4 PM2 (Supporting): The variant is absent from gnomAD v2.1, v4.1, and gnomAD-Canada population databases, meeting the VCEP requirement for absence from controls.5 PP3 (Supporting): The REVEL score of 0.811 exceeds the VCEP threshold of >=0.7 for pathogenic computational prediction. SpliceAI predicts no splice impact (max delta = 0.00).6 Combination: PS1 (1 Strong) + PM1 (1 Moderate) + PM5 (1 Moderate) + PM2 (1 Supporting) + PP3 (1 Supporting) satisfies VCEP Rule 7 (1 Strong + 2 Moderate + >=2 Supporting = Pathogenic).7