Disclosing the potential of eleganolone for Parkinson's disease therapeutics: Neuroprotective and anti-inflammatory activities
被引:24
作者:
Silva, Joana
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Univ Santiago de Compostela, Fac Vet, Dept Pharmacol, Lugo 27002, SpainPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Silva, Joana
[1
,2
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Alves, Celso
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Alves, Celso
[1
]
Pinteus, Susete
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Pinteus, Susete
[1
]
Susano, Patricia
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Susano, Patricia
[1
]
Simoes, Marco
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Simoes, Marco
[1
]
Guedes, Miguel
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Guedes, Miguel
[1
]
Martins, Alice
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Martins, Alice
[1
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Rehfeldt, Stephanie
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Univ Vale Taquari UNIVATES, Cell Culture Lab, Grad Program Biotechnol, BR-95901120 Lajeado, RS, BrazilPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Rehfeldt, Stephanie
[3
]
Gaspar, Helena
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Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Univ Lisbon, Fac Sci, BioISI Biosyst & Integrat Sci Inst, P-1749016 Lisbon, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Gaspar, Helena
[1
,4
]
Goettert, Marcia
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Univ Vale Taquari UNIVATES, Cell Culture Lab, Grad Program Biotechnol, BR-95901120 Lajeado, RS, BrazilPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Goettert, Marcia
[3
]
Alfonso, Amparo
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Univ Santiago de Compostela, Fac Vet, Dept Pharmacol, Lugo 27002, SpainPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Alfonso, Amparo
[2
]
Pedrosa, Rui
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Polytech Leiria, MARE Marine & Environm Sci Ctr, ESTM, P-2520614 Peniche, PortugalPolytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
Pedrosa, Rui
[5
]
机构:
[1] Polytech Leiria, MARE Marine & Environm Sci Ctr, P-2520630 Peniche, Portugal
[2] Univ Santiago de Compostela, Fac Vet, Dept Pharmacol, Lugo 27002, Spain
[3] Univ Vale Taquari UNIVATES, Cell Culture Lab, Grad Program Biotechnol, BR-95901120 Lajeado, RS, Brazil
[4] Univ Lisbon, Fac Sci, BioISI Biosyst & Integrat Sci Inst, P-1749016 Lisbon, Portugal
[5] Polytech Leiria, MARE Marine & Environm Sci Ctr, ESTM, P-2520614 Peniche, Portugal
The treatment of Parkinson's disease (PD) has benefited from significant advances resulting from the increasing research efforts focused on new therapeutics. However, the current treatments for PD are mostly symptomatic, alleviating disease symptoms without reversing or retarding disease progression. Thus, it is critical to find new molecules that can result in more effective treatments. Within this framework, this study aims to evaluate the neuroprotective and anti-inflammatory effects of three compounds (eleganolone, eleganonal and fucosterol) isolated from the brown seaweed Bifurcaria bifurcata. In vitro neuroprotective effects were evaluated on a PD cellular model induced by the neurotoxin 6-hydroxydopamine (6-OHDA) on SH-SY5Y human cells, while lipopolysaccharide (LPS) stimulated RAW 264.7 macrophages were used to evaluate the anti-inflammatory potential. Additionally, the underlying mechanisms of action were also investigated. Compounds were isolated by preparative chromatographic methods and their structural elucidation attained by NMR spectroscopy. Among the tested compounds, eleganolone (0.1-1 mu M; 24 h) reverted the neurotoxicity induced by 6-OHDA in about 20%. The neuroprotective effects were mediated by mitochondrial protection, reduction of oxidative stress, inflammation and apoptosis, and inhibition of NF-kB pathway. The results suggest that eleganolone may provide advantages in the treatment of neurodegenerative conditions and, therefore, should be considered for future preclinical studies.