Table 1.
Potential therapeutic use of the retromer chaperones in human disease. List of neurological and non-neurological diseases with established links to the retromer pathway
| Pathogenic link‡ | Established pathway§ | Animal models | |
|---|---|---|---|
| Alzheimer’s disease* | + + + | APP endosomal trafficking | + + + |
| Parkinson’s disease* | + + + | Vps35 mutations, impaired autophagy | + |
| Down’s syndrome* | + | SNX27 dysfunction | + + |
| HSP* | + | Retromer/WASH complex interaction | + |
| Cerebral lipofuscinosis* | + | Deficient retromer recruitment machinery | + |
| Nieman Pick type C1* | +/– | ESCRT-mediated endosomal cholesterol trafficking | + |
| Type II diabetes† | + + | SORCS1 (Vps10 family) dysfunction | + + |
| Osteoporosis† | + | Vps35 deficiency, deregulation of RANK signaling | + |
HSP = hereditary spastic paraplegia; APP = amyloid precursor protein; Vps = vacuolar protein sorting; WASH = Wiskott–Aldrich Syndrome Protein and SCAR Homolog; ESCRT = Endosomal Sorting Complex Required for Transport; SORCS1 = sortilin-related VPS10 domain containing receptor; RANK = Receptor activator of nuclear factor-kappa B
*Neurological disease
†Non-neurological disease
‡The number of plus symbols depicts the amount/strength of experimental evidence associated in each disease with the role of the retromer complex/pathway
§A short description of the molecular/cellular pathway affected in each disease is shown. For further details please refer to the cited bibliography in the main text