Litcius/Paper detail

Regulation of Mitochondrial Dynamics in Parkinson’s Disease—Is 2-Methoxyestradiol a Missing Piece?

Paulina Bastian, Jarosław Dulski, Anna Roszmann, Dagmara Jacewicz, Alicja Kuban‐Jankowska, Jarosław Sławek, Michał Woźniak, Magdalena Górska‐Ponikowska

2021Antioxidants17 citationsDOIOpen Access PDF

Abstract

Mitochondria, as "power house of the cell", are crucial players in cell pathophysiology. Beyond adenosine triphosphate (ATP) production, they take part in a generation of reactive oxygen species (ROS), regulation of cell signaling and cell death. Dysregulation of mitochondrial dynamics may lead to cancers and neurodegeneration; however, the fusion/fission cycle allows mitochondria to adapt to metabolic needs of the cell. There are multiple data suggesting that disturbed mitochondrial homeostasis can lead to Parkinson's disease (PD) development. 2-methoxyestradiol (2-ME), metabolite of 17β-estradiol (E2) and potential anticancer agent, was demonstrated to inhibit cell growth of hippocampal HT22 cells by means of nitric oxide synthase (NOS) production and oxidative stress at both pharmacologically and also physiologically relevant concentrations. Moreover, 2-ME was suggested to inhibit mitochondrial biogenesis and to be a dynamic regulator. This review is a comprehensive discussion, from both scientific and clinical point of view, about the influence of 2-ME on mitochondria and its plausible role as a modulator of neuron survival.

Topics & Concepts

MitochondrionCell biologyNeurodegenerationmitochondrial fusionOxidative stressProgrammed cell deathMitochondrial fissionAdenosine triphosphateReactive oxygen speciesBiologyCellMitochondrial biogenesisCell growthMFN1ChemistryApoptosisBiochemistryMitochondrial DNADiseaseInternal medicineMedicineGeneMitochondrial Function and PathologyElectron Spin Resonance StudiesCoenzyme Q10 studies and effects