NM_001277115.2:c.4879C>T (p.Arg1627Cys) is a missense variant in DNAH11, a gene associated with autosomal recessive primary ciliary dyskinesia (PCD) and heterotaxy syndromes. This variant is extremely rare in population databases: gnomAD v2.1 AF = 0.00107% (3/280,426 alleles), gnomAD v4.1 AF = 0.00155% (25/1,613,592 alleles), and it is absent from gnomAD-Canada, with no homozygotes observed in any population database (PM2_supporting).1 In silico prediction tools support a deleterious effect, with a REVEL score of 0.887 exceeding the damaging threshold (PP3_supporting).2 SpliceAI predicts no splicing impact (max delta score = 0.00), and the variant does not lie in a statistically significant mutational hotspot.3 This variant has been reported in ClinVar with conflicting classifications: four clinical laboratories classify it as Uncertain Significance, one as Pathogenic, and one as Likely Pathogenic. No expert panel review has been performed (ClinVar Variation ID: 163104).4 The variant has been observed somatically in COSMIC (COSV60977423, n = 2). No variant-specific functional data, case-control studies, segregation data, or de novo reports were identified in the reviewed literature. The five publications cited by ClinVar submitters are either methodology/guideline papers (PMID:24033266, PMID:25741868, PMID:28492532), a general GeneReviews overview (PMID:20301301), or a PCD cohort study that does not specifically mention c.4879C>T (PMID:31772028).5