Glucocerebrosidase Mutations Cause Mitochondrial and Lysosomal Dysfunction in Parkinson's Disease: Pathogenesis and Therapeutic Implications

Wei Zheng^{1

2

3}, Dongsheng Fan^{1

2

3}

Affiliations

¹ Department of Neurology, Peking University Third Hospital, Beijing, China.
² Beijing Key Laboratory of Biomarker and Translational Research in Neurodegenerative Diseases, Beijing, China.
³ Key Laboratory for Neuroscience, National Health Commission/Ministry of Education, Peking University, Beijing, China.

PMID: 35401150
PMCID: PMC8984109
DOI: 10.3389/fnagi.2022.851135

Review

Glucocerebrosidase Mutations Cause Mitochondrial and Lysosomal Dysfunction in Parkinson's Disease: Pathogenesis and Therapeutic Implications

Wei Zheng et al. Front Aging Neurosci. 2022.

. 2022 Mar 23:14:851135.

doi: 10.3389/fnagi.2022.851135. eCollection 2022.

Authors

Wei Zheng^{1

2

3}, Dongsheng Fan^{1

2

3}

Affiliations

¹ Department of Neurology, Peking University Third Hospital, Beijing, China.
² Beijing Key Laboratory of Biomarker and Translational Research in Neurodegenerative Diseases, Beijing, China.
³ Key Laboratory for Neuroscience, National Health Commission/Ministry of Education, Peking University, Beijing, China.

PMID: 35401150
PMCID: PMC8984109
DOI: 10.3389/fnagi.2022.851135

Abstract

Parkinson's disease (PD) is the second most common neurodegenerative disease and is characterized by multiple motor and non-motor symptoms. Mutations in the glucocerebrosidase (GBA) gene, which encodes the lysosomal enzyme glucocerebrosidase (GCase), which hydrolyzes glucosylceramide (GlcCer) to glucose and ceramide, are the most important and common genetic PD risk factors discovered to date. Homozygous GBA mutations result in the most common lysosomal storage disorder, Gaucher's disease (GD), which is classified according to the presence (neuronopathic types, type 2 and 3 GD) or absence (non-neuronopathic type, type 1 GD) of neurological symptoms. The clinical manifestations of PD in patients with GBA mutations are indistinguishable from those of sporadic PD at the individual level. However, accumulating data have indicated that GBA-associated PD patients exhibit a younger age of onset and a greater risk for cognitive impairment and psychiatric symptoms. The mechanisms underlying the increased risk of developing PD in GBA mutant carriers are currently unclear. Contributors to GBA-PD pathogenesis may include mitochondrial dysfunction, autophagy-lysosomal dysfunction, altered lipid homeostasis and enhanced α-synuclein aggregation. Therapeutic strategies for PD and GD targeting mutant GCase mainly include enzyme replacement, substrate reduction, gene and pharmacological small-molecule chaperones. Emerging clinical, genetic and pathogenic studies on GBA mutations and PD are making significant contributions to our understanding of PD-associated pathogenetic pathways, and further elucidating the interactions between GCase activity and neurodegeneration may improve therapeutic approaches for slowing PD progression.

Keywords: Gaucher’s disease (GD); Parkinson’s disease (PD); glucocerebrosidase (GBA); lysosomal; mitochondrial.

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Conflict of interest statement

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Figures

**FIGURE 1**
The schematic diagram of proposed mechanisms by which *GBA* mutations contribute to the development of PD. Contributions to *GBA*-PD pathogenesis may include enhanced α-synuclein aggregation, altered lipid homeostasis, autophagy-lysosomal dysfunction and mitochondrial dysfunction. *GBA*, glucocerebrosidase; GCase, glucocerebrosidase.

See this image and copyright information in PMC

References

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Glucocerebrosidase Mutations Cause Mitochondrial and Lysosomal Dysfunction in Parkinson's Disease: Pathogenesis and Therapeutic Implications

Affiliations

Glucocerebrosidase Mutations Cause Mitochondrial and Lysosomal Dysfunction in Parkinson's Disease: Pathogenesis and Therapeutic Implications

Authors

Affiliations

Abstract

Conflict of interest statement

Figures

References

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