Molecular Genetics & Genomic Medicine (Nov 2020)

NPC1 silent variant induces skipping of exon 11 (p.V562V) and unfolded protein response was found in a specific Niemann‐Pick type C patient

  • Marisa Encarnação,
  • Maria Francisca Coutinho,
  • Soo Min Cho,
  • Maria Teresa Cardoso,
  • Isaura Ribeiro,
  • Paulo Chaves,
  • Juliana Inês Santos,
  • Dulce Quelhas,
  • Lúcia Lacerda,
  • Elisa Leão Teles,
  • Anthony H. Futerman,
  • Laura Vilarinho,
  • Sandra Alves

DOI
https://doi.org/10.1002/mgg3.1451
Journal volume & issue
Vol. 8, no. 11
pp. n/a – n/a

Abstract

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Abstract Background Niemann‐Pick type C (NPC, MIM #257220) is a neuro‐visceral disease, caused predominantly by pathogenic variants in the NPC1 gene. Here we studied patients with clinical diagnosis of NPC but inconclusive results regarding the molecular analysis. Methods We used a Next‐Generation Sequencing (NGS)‐panel followed by cDNA analysis. Latter, we used massively parallel single‐cell RNA‐seq (MARS‐Seq) to address gene profiling changes and finally the effect of different variants on the protein and cellular levels. Results We identified novel variants and cDNA analysis allowed us to establish the functional effect of a silent variant, previously reported as a polymorphism. We demonstrated that this variant induces the skipping of exon 11 leading to a premature stop codon and identified it in NPC patients from two unrelated families. MARS‐Seq analysis showed that a number of upregulated genes were related to the unfolded protein response (UPR) and endoplasmic reticulum (ER) stress in one specific patient. Also, for all analyzed variants, the NPC1 protein was partially retained in the ER. Conclusion We showed that the NPC1 silent polymorphism (p.V562V) is a disease‐causing variant in NPC and that the UPR is upregulated in an NPC patient.

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