Juvenile mucopolysaccharidosis plus disease caused by a missense mutation in VPS33A

Elena V Pavlova; Dorit Lev; Marina Michelson; Keren Yosovich; Hila Gur Michaeli; Nicholas A Bright; Paul T Manna; Veronica Kane Dickson; Karen L Tylee; Heather J Church; J Paul Luzio; Timothy M Cox

doi:10.1002/humu.24479

Juvenile mucopolysaccharidosis plus disease caused by a missense mutation in VPS33A

Hum Mutat. 2022 Dec;43(12):2265-2278. doi: 10.1002/humu.24479. Epub 2022 Oct 8.

Authors

Elena V Pavlova¹, Dorit Lev^{2

3

4}, Marina Michelson², Keren Yosovich², Hila Gur Michaeli², Nicholas A Bright⁵, Paul T Manna^{5

6}, Veronica Kane Dickson⁵, Karen L Tylee⁷, Heather J Church⁷, J Paul Luzio⁵, Timothy M Cox¹

Affiliations

¹ Department of Medicine, University of Cambridge, Cambridge, UK.
² Wolfson Medical Centre, Institute of Medical Genetics, Holon, Israel.
³ The Rina Mor Institute of Medical Genetics, Holon, Israel.
⁴ The Sackler School of Medicine, Tel Aviv University, Tel Aviv, Israel.
⁵ Department of Clinical Biochemistry, Cambridge Institute for Medical Research, The Keith Peters Building, University of Cambridge, Cambridge, UK.
⁶ Department of Neuroscience and Physiology, University of Gothenburg, Gothenburg, Sweden.
⁷ Willink Biochemical Genetics Unit, Genomic Diagnostics Laboratory, Manchester Centre for Genomic Medicine, Central Manchester University Hospitals NHS Foundation Trust St Mary's Hospital, Manchester, UK.

Abstract

A rare and fatal disease resembling mucopolysaccharidosis in infants, is caused by impaired intracellular endocytic trafficking due to deficiency of core components of the intracellular membrane-tethering protein complexes, HOPS, and CORVET. Whole exome sequencing identified a novel VPS33A mutation in a patient suffering from a variant form of mucopolysaccharidosis. Electron and confocal microscopy, immunoblotting, and glycosphingolipid trafficking experiments were undertaken to investigate the effects of the mutant VPS33A in patient-derived skin fibroblasts. We describe an attenuated juvenile form of VPS33A-related syndrome-mucopolysaccharidosis plus in a man who is homozygous for a hitherto unknown missense mutation (NM_022916.4: c.599 G>C; NP_075067.2:p. Arg200Pro) in a conserved region of the VPS33A gene. Urinary glycosaminoglycan (GAG) analysis revealed increased heparan, dermatan sulphates, and hyaluronic acid. We showed decreased abundance of VPS33A in patient derived fibroblasts and provided evidence that the p.Arg200Pro mutation leads to destablization of the protein and proteasomal degradation. As in the infantile form of mucopolysaccharidosis plus, the endocytic compartment in the fibroblasts also expanded-a phenomenon accompanied by increased endolysosomal acidification and impaired intracellular glycosphingolipid trafficking. Experimental treatment of the patient's cultured fibroblasts with the proteasome inhibitor, bortezomib, or exposure to an inhibitor of glucosylceramide synthesis, eliglustat, improved glycosphingolipid trafficking. To our knowledge this is the first report of an attenuated juvenile form of VPS33A insufficiency characterized by appreciable residual endosomal-lysosomal trafficking and a milder mucopolysaccharidosis plus than the disease in infants. Our findings expand the proof of concept of redeploying clinically approved drugs for therapeutic exploitation in patients with juvenile as well as infantile forms of mucopolysaccharidosis plus disease.

Keywords: VPS33A; drug repurposing; endolysosomal acidification; glycosaminoglycan; glycosphingolipid trafficking; intracellular endocytic trafficking; mucopolysaccharidosis; proteasome inhibitor; substrate reduction therapy.

Publication types

Case Reports
Research Support, Non-U.S. Gov't

MeSH terms

Endosomes / metabolism
Humans
Lysosomes / metabolism
Male
Mutation
Mutation, Missense*
Vesicular Transport Proteins* / genetics
Vesicular Transport Proteins* / metabolism

Substances

Vesicular Transport Proteins
VPS33A protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding