Journal
FRONTIERS IN MOLECULAR NEUROSCIENCE
Volume 14, Issue -, Pages -Publisher
FRONTIERS MEDIA SA
DOI: 10.3389/fnmol.2021.673144
Keywords
benztropine; haloperidol; clozapine; MO3; 13 cell line; phytocannabinoid; proteome; schizophrenia
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Funding
- Sao Paulo Research Foundation (Fundacao de Amparo a Pesquisa do Estado de Sao Paulo, FAPESP) [2017/25588-1, 2017/18242-1, 2018/03673-0, 2018/10362-0, 2018/03422-7, 2018/03450-0, 2019/22398-2, 2019/00098-7]
- Coordination for the Improvement of Higher Education Personnel (Coordenacao de Aperfeicoamento de Pessoal de Nivel Superior, CAPES) [88887.495565/2020-00]
- CNPq (Conselho Nacional de Desenvolvimento Cientifico e Tecnologico) [157265/2018-8, 166571/2018-0]
- Instituto Nacional de Ciencia e Tecnologia Translational em Medicina (INCT-TM
- CNPq/FAPESP) [2008/09009-2]
- University Global Partnership Network (UGPN)-Global Priorities in Cannabinoid Research Excellence Program
- CNPq research fellowships
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The study found that cannabidiol shares similarities in molecular pathways with clozapine and benztropine, exhibiting characteristics of atypical antipsychotic drugs. These drugs affect metabolic and gene expression pathways, and post-cuprizone-induced toxicity, cannabidiol, benztropine, and clozapine modulated cell proliferation and apoptosis.
Cannabidiol, a compound of Cannabis sativa, has been proposed as an alternative treatment of schizophrenia. Preclinical and clinical data have suggested that cannabidiol shares more similarity with atypical antipsychotics than typical, both of which are customarily used to manage schizophrenia symptoms. While oligodendrocytes are known to be relevant targets of antipsychotics, the biochemical knowledge in this regard is still limited. Here we evaluated the molecular pathways modulated by cannabidiol compared to the antipsychotics clozapine (atypical) and haloperidol (typical), additionally evaluating the effects of benztropine, a muscarinic receptor antagonist that displays a protective effect in oligodendrocytes and myelination. For this purpose, we employed nano-chromatography coupled with mass spectrometry to investigate the proteomic response to these drugs both in healthy oligodendrocytic cells and in a cuprizone-based toxicity model, using the human oligodendrocyte precursor cell line MO3.13. Cannabidiol shares similarities of biochemical pathways with clozapine and benztropine, in agreement with other studies that indicated an atypical antipsychotic profile. All drugs tested affected metabolic and gene expression pathways and cannabidiol, benztropine, and clozapine modulated cell proliferation and apoptosis when administered after cuprizone-induced toxicity. These general pathways are associated with cuprizone-induced cytotoxicity in MO3.13 cells, indicating a possible proteomic approach when acting against the toxic effects of cuprizone. In conclusion, although modeling oligodendrocytic cytotoxicity with cuprizone does not represent the entirety of the pathophysiology of oligodendrocyte impairments, these results provide insight into the mechanisms associated with the effects of cannabidiol and antipsychotics against cuprizone toxicity, offering new directions of study for myelin-related processes and deficits.
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