Transcript, protein, metabolite and cellular studies in skin fibroblasts demonstrate variable pathogenic impacts of NPC1 mutations

Dita Musalkova; Filip Majer; Ladislav Kuchar; Ondrej Luksan; Befekadu Asfaw; Hana Vlaskova; Gabriela Storkanova; Martin Reboun; Helena Poupetova; Helena Jahnova; Helena Hulkova; Jana Ledvinova; Lenka Dvorakova; Jakub Sikora; Milan Jirsa; Marie T Vanier; Martin Hrebicek

doi:10.1186/s13023-020-01360-5

Transcript, protein, metabolite and cellular studies in skin fibroblasts demonstrate variable pathogenic impacts of NPC1 mutations

Orphanet J Rare Dis. 2020 Apr 5;15(1):85. doi: 10.1186/s13023-020-01360-5.

Authors

Dita Musalkova¹, Filip Majer², Ladislav Kuchar¹, Ondrej Luksan³, Befekadu Asfaw¹, Hana Vlaskova¹, Gabriela Storkanova¹, Martin Reboun¹, Helena Poupetova¹, Helena Jahnova¹, Helena Hulkova¹, Jana Ledvinova¹, Lenka Dvorakova¹, Jakub Sikora¹, Milan Jirsa³, Marie T Vanier^{4

5}, Martin Hrebicek⁶

Affiliations

¹ Research Unit for Rare Diseases, Department of Pediatrics and Adolescent Medicine, First Faculty of Medicine, Charles University and General University Hospital, Ke Karlovu 2, 120 00, Prague 2, Czech Republic.
² Research Unit for Rare Diseases, Department of Pediatrics and Adolescent Medicine, First Faculty of Medicine, Charles University and General University Hospital, Ke Karlovu 2, 120 00, Prague 2, Czech Republic. filip.majer@lf1.cuni.cz.
³ Laboratory of Experimental Hepatology, Institute of Clinical and Experimental Medicine, Prague, Czech Republic.
⁴ INSERM U820, Lyon, France.
⁵ Laboratoire Gillet-Mérieux, Lyon University Hospitals (HCL), Lyon, France.
⁶ Research Unit for Rare Diseases, Department of Pediatrics and Adolescent Medicine, First Faculty of Medicine, Charles University and General University Hospital, Ke Karlovu 2, 120 00, Prague 2, Czech Republic. martin.hrebicek@lf1.cuni.cz.

Abstract

Background: Niemann-Pick type C (NP-C) is a rare neurovisceral genetic disorder caused by mutations in the NPC1 or the NPC2 gene. NPC1 is a multipass-transmembrane protein essential for egress of cholesterol from late endosomes/lysosomes. To evaluate impacts of NPC1 mutations, we examined fibroblast cultures from 26 NP-C1 patients with clinical phenotypes ranging from infantile to adult neurologic onset forms. The cells were tested with multiple assays including NPC1 mRNA expression levels and allele expression ratios, assessment of NPC1 promoter haplotypes, NPC1 protein levels, cellular cholesterol staining, localization of the mutant NPC1 proteins to lysosomes, and cholesterol/cholesteryl ester ratios. These results were correlated with phenotypes of the individual patients.

Results: Overall we identified 5 variant promoter haplotypes. Three of them showed reporter activity decreased down to 70% of the control sequence. None of the haplotypes were consistently associated with more severe clinical presentation of NP-C. Levels of transcripts carrying null NPC1 alleles were profoundly lower than levels of the missense variants. Low levels of the mutant NPC1 protein were identified in most samples. The protein localised to lysosomes in cultures expressing medium to normal NPC1 levels. Fibroblasts from patients with severe infantile phenotypes had higher cholesterol levels and higher cholesterol/cholesteryl ester ratios. On the contrary, cell lines from patients with juvenile and adolescent/adult phenotypes showed values comparable to controls.

Conclusion: No single assay fully correlated with the disease severity. However, low residual levels of NPC1 protein and high cholesterol/cholesteryl ester ratios associated with severe disease. The results suggest not only low NPC1 expression due to non-sense mediated decay or low mutant protein stability, but also dysfunction of the stable mutant NPC1 as contributors to the intracellular lipid transport defect.

Keywords: Cholesterol transport; Lysosomal storage disease; Mutant protein; Niemann-pick type C; Proteostasis.

Publication types

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

MeSH terms

Adolescent
Carrier Proteins* / genetics
Fibroblasts / metabolism
Humans
Intracellular Signaling Peptides and Proteins
Membrane Glycoproteins* / genetics
Membrane Glycoproteins* / metabolism
Mutation / genetics
Niemann-Pick C1 Protein

Substances

Carrier Proteins
Intracellular Signaling Peptides and Proteins
Membrane Glycoproteins
NPC1 protein, human
Niemann-Pick C1 Protein