Cell & Bioscience (Mar 2022)

Transcriptomic characterization of tissues from patients and subsequent pathway analyses reveal biological pathways that are implicated in spastic ataxia

  • Andrea C. Kakouri,
  • Christina Votsi,
  • Anastasis Oulas,
  • Paschalis Nicolaou,
  • Massimo Aureli,
  • Giulia Lunghi,
  • Maura Samarani,
  • Giacomo M. Compagnoni,
  • Sabrina Salani,
  • Alessio Di Fonzo,
  • Thalis Christophides,
  • George A. Tanteles,
  • Eleni Zamba-Papanicolaou,
  • Marios Pantzaris,
  • George M. Spyrou,
  • Kyproula Christodoulou

DOI
https://doi.org/10.1186/s13578-022-00754-1
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 22

Abstract

Read online

Abstract Background Spastic ataxias (SAs) encompass a group of rare and severe neurodegenerative diseases, characterized by an overlap between ataxia and spastic paraplegia clinical features. They have been associated with pathogenic variants in a number of genes, including GBA2. This gene codes for the non-lysososomal β-glucosylceramidase, which is involved in sphingolipid metabolism through its catalytic role in the degradation of glucosylceramide. However, the mechanism by which GBA2 variants lead to the development of SA is still unclear. Methods In this work, we perform next-generation RNA-sequencing (RNA-seq), in an attempt to discover differentially expressed genes (DEGs) in lymphoblastoid, fibroblast cell lines and induced pluripotent stem cell-derived neurons derived from patients with SA, homozygous for the GBA2 c.1780G > C missense variant. We further exploit DEGs in pathway analyses in order to elucidate candidate molecular mechanisms that are implicated in the development of the GBA2 gene-associated SA. Results Our data reveal a total of 5217 genes with significantly altered expression between patient and control tested tissues. Furthermore, the most significant extracted pathways are presented and discussed for their possible role in the pathogenesis of the disease. Among them are the oxidative stress, neuroinflammation, sphingolipid signaling and metabolism, PI3K-Akt and MAPK signaling pathways. Conclusions Overall, our work examines for the first time the transcriptome profiles of GBA2-associated SA patients and suggests pathways and pathway synergies that could possibly have a role in SA pathogenesis. Lastly, it provides a list of DEGs and pathways that could be further validated towards the discovery of disease biomarkers.

Keywords