Wilson disease
Wilson disease is a hepatic/metabolic genetic disease caused by autosomal recessive variants in ATP7B. It is not placed in the rankable burden order: only 2 of five axes are scored (cut: three of five), so the remaining 3 stay open [O], not guessed. Mechanism, scored axes, and treatment follow below.
Wilson disease is inherited as autosomal recessive and acts by loss-of-function (biallelic; recessive) ([H]). Of the five burden axes, 2 are scored (O, P) and 3 are open [O] (S, M, D); because fewer than three are scored the disease is reported as “not placed — insufficient axis coverage” (rank null), not ranked on partial data.
Gene, inheritance, and molecular mechanism
Wilson disease is inherited as Autosomal recessive inheritance [L] and is classified mechanistically as loss-of-function (biallelic; recessive) [H]. ATP7B encodes a copper-transporting ATPase that exports hepatic copper into bile. Its loss causes copper to accumulate first in the liver and then in the brain and other organs.
Inheritance source: medgen:esummary:ModeOfInheritance:2026-06-17. Mechanism source: inference:recessive=>loss_of_function; basis=medgen_inheritance(recessive); corrob=clingen_AR(HI30):ATP7B. These are observed, cited inputs; the classification is the reproducible analysis layer (C-D1).
In-scope clinical involvement
Wilson disease presents with hepatic disease (hepatitis, cirrhosis), and the in-scope features extend to Kayser-Fleischer corneal rings and a Coombs-negative haemolytic anaemia.
| Organ system (HPO rollup) | terms |
|---|---|
| nervous system | 21 |
| metabolism/homeostasis | 17 |
| digestive system | 15 |
| genitourinary system | 8 |
| musculoskeletal system | 7 |
| blood and blood-forming tissues | 3 |
Organ systems [L] from HPO phenotype.hpoa v2026-06-06 (OMIM 277900,606882); P-aspect terms rolled up to HP:0000118 organ-system categories via hp.obo.
Burden axes and why this disease is not placed
| Burden axis | value | grade |
|---|---|---|
| Onset earliness (O) | 0.7000 | [L] |
| Progression (P) | 0.8000 | [H] |
| Symptom severity (S) | — | [O] |
| Mortality (M) | — | [O] |
| Disability (D) | — | [O] |
For transparency the partial composite over the 2 scored axis/axes is raw_burden = 0.7500, but it is not used to rank the disease (below the ≥ 3-axis cut). The open axes (severity, mortality, disability) are graded [O] with a named obstacle, never imputed.
The natural-history registry passes lift onset (Orphanet, R6) and disability (GBD 2013 disability weights, R7) to registry [L] where an entity-anchored mapping exists, lift severity (HPO Severity-modifier subtree, R8) where the dominant sequela is annotated, and lift progression (curated PMC open-access literature with a frozen-R3-derived tier, R9) where a cited disease-level magnitude for the dominant untreated sequela exists. For some diseases the added disability axis was enough to cross the ≥ 3-axis cut and enter the placed residual order; for this one it was not — and its dominant sequela carries no open HPO severity annotation, so no registry severity tier is available (the open HPO severity annotations elsewhere are feature-level; the OMIM clinical synopsis, the disease-level alternative, is API-key-gated and the key is unobtainable for an individual researcher). Scoring three or more axes at registry grade (via published functional & survival literature) would let this disease enter the rankable residual order; until then it is reported here, never imputed.
Established treatment
The established disease-directed approach is copper chelation (penicillamine or trientine) with zinc. Mechanistically: chelators promote urinary copper excretion; zinc blocks intestinal copper absorption [L]. Its effect on natural history is classified disease-modifying (substantial) (efficacy offset e = 0.5500, residual factor R_treat = 0.4500); this offset would apply to the burden score once the disease is placed.
Evidence tier: accession-dated to the GeneReviews NBK1512 Management section [L] (initial posting October 22, 1999; last revision January 12, 2023; retrieved 2026-06-18; corroborating term(s): “copper, chelation, penicillamine, trientine, zinc”).