Deciphering metabolic shifts in Gaucher disease type 1: a multi-omics study

Franklin Ducatez; Marc G Berger; Carine Pilon; Thomas Plichet; Céline Lesueur; Juliette Berger; Nadia Belmatoug; Stéphane Marret; Soumeya Bekri; Abdellah Tebani

doi:10.1007/s00109-024-02512-x

Deciphering metabolic shifts in Gaucher disease type 1: a multi-omics study

J Mol Med (Berl). 2024 Dec 30. doi: 10.1007/s00109-024-02512-x. Online ahead of print.

Authors

Franklin Ducatez^{1

2}, Marc G Berger^{3

4}, Carine Pilon¹, Thomas Plichet¹, Céline Lesueur¹, Juliette Berger^{3

4}, Nadia Belmatoug⁵, Stéphane Marret², Soumeya Bekri¹, Abdellah Tebani⁶

Affiliations

¹ Department of Metabolic Biochemistry, Referral Center for Lysosomal Diseases, Normandie Univ, UNIROUEN, CHU Rouen, INSERM U1245, Filière G2M, 76000, Rouen, France.
² Department of Neonatal Pediatrics, Intensive Care and Neuropediatrics, Referral Center for Lysosomal Diseases, Normandie Univ, UNIROUEN, CHU Rouen, INSERM U1245, Filière G2M, 76000, Rouen, France.
³ CHU Clermont-Ferrand, Hopital Estaing, CRB-Auvergne, 63003, Clermont-Ferrand, France.
⁴ Université Clermont Auvergne, EA, 7453 CHELTER, 63000, Clermont-Ferrand, France.
⁵ Referral Center for Lysosomal Diseases, Filière G2M, Paris Cité University, APHP-Nord, Paris, France.
⁶ Department of Metabolic Biochemistry, Referral Center for Lysosomal Diseases, Normandie Univ, UNIROUEN, CHU Rouen, INSERM U1245, Filière G2M, 76000, Rouen, France. [email protected].

PMID: 39738845
DOI: 10.1007/s00109-024-02512-x

Abstract

Gaucher disease (GD), an autosomal recessive lysosomal disorder, primarily affects the lysosomal enzyme β-glucocerebrosidase (GCase), leading to glucosylceramide accumulation in lysosomes. GD presents a wide spectrum of clinical manifestations. This study deploys immune-based proteomics and mass spectrometry-based metabolomics technologies to comprehensively investigate the biochemical landscape in 43 deeply phenotyped type 1 GD patients compared to 59 controls. Conventional and systems biology approaches have been used to analyze the data. The results show promising biological imprints. Elevated phosphatidylcholines in GD patients suggest altered lipid metabolism, potentially due to their increased synthesis. This points to endoplasmic reticulum stress and impaired lipid trafficking, commonly seen in lysosomal diseases. GD patients exhibit an inflammatory profile with elevated cytokines and autoimmune-like inflammation, even in treated patients, highlighting the complexity of GD-related immune imbalances. Mitochondrial dysfunction clues are found through increased oxidative stress markers and altered acylcarnitine profiles in GD patients, suggesting mitochondrial membrane dysfunction affecting carnitine-carrying capacity. Furthermore, platelet count, splenectomy, treatment, and clinical traits were associated with specific omics features, providing insights into GD's clinical heterogeneity and potential diagnostic markers. Autophagy inhibition appears pivotal in GD, driving lipid synthesis, impaired mitochondrial function, and inflammation through chronic activation of mTORC1. Despite limitations like focusing on type 1 GD and using targeted omics approaches, this study provides valuable insights into GD metabolic and immune dysregulation. It lays the basis for future comprehensive investigations into GD manifestations with broader scope and molecular coverage. KEY MESSAGES: The study sheds light on metabolic and immune dysregulation in Gaucher disease. Gaucher disease patients showed elevated phosphatidylcholines, disrupted lipid metabolism, and inflammation profiles. Signs of mitochondrial dysfunction are evident in Gaucher disease patients, with autophagy inhibition significantly affecting lipid synthesis, mitochondrial function, and inflammation via chronic activation of mTORC1.

Keywords: Gaucher disease; Inherited metabolic diseases; Lysosomal diseases; Omics; Systems biology.