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Visualization of melatonin’s multiple mitochondrial levels of protection against mitochondrial Ca 2+ ‐mediated permeability transition and beyond in rat brain astrocytes
Author(s) -
Jou MeiJie,
Peng TsungI,
Hsu LeeFen,
Jou ShuoBin,
Reiter Russel J.,
Yang ChuenMao,
Chiao ChuanChin,
Lin YiFan,
Chen ChunChia
Publication year - 2010
Publication title -
journal of pineal research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.881
H-Index - 131
eISSN - 1600-079X
pISSN - 0742-3098
DOI - 10.1111/j.1600-079x.2009.00721.x
Subject(s) - melatonin , mitochondrial permeability transition pore , oxidative stress , ionomycin , reactive oxygen species , mitochondrion , apoptosis , microbiology and biotechnology , biology , chemistry , endocrinology , medicine , biochemistry , programmed cell death , intracellular
Melatonin protects cells against various types of oxidative stress‐induced apoptosis due primarily to its ability to effectively scavenge pathological and disease condition‐augmented generation of mitochondrial reactive oxygen species (mROS). Once produced, mROS indiscriminately damage mitochondrial components and more importantly they crucially activate directly the mitochondrial permeability transition (MPT), one of the critical mechanisms for initiating post mitochondrial apoptotic signaling. Whether or not melatonin targets directly the MPT, however, remains inconclusive, particularly during oxidative stress. This study, thus, investigated this possibility of an ‘oxidation free Ca 2+ stress’ in the presence of vitamin E after ionomycin exposure as a sole Ca 2+ ‐mediated MPT in order to exclude melatonin’s primary antioxidative effects as well as Ca 2+ ‐mediated oxidative stress. The studies were carried out using cultured rat brain astrocytes RBA‐1. With the application of laser scanning multiple fluorescence imaging microscopy, we visualized for the first time multiple mitochondrial protective effects provided by melatonin during Ca 2+ stress. First, melatonin, due to its primary antioxidative actions, completely prevented mCa 2+ ‐induced mROS formation during ionomycin exposure. Secondly, when melatonin ’ s antioxidative effects were prevented due to the addition of vitamin E, melatonin significantly prevented mCa 2+ ‐mediated MPT and apoptosis suggesting its direct targeting of the MPT. Surprisingly, in the presence of cyclosporin A, a MPT inhibitor, melatonin reduced further mCa 2+ ‐mediated apoptosis during ionomycin exposure also suggesting its targeting beyond the MPT. As astrocytes are actively involve in regulating synaptic transmission and neurovascular coupling in the CNS, these multiple mitochondrial layers of protection provided by melatonin against mCa 2+ ‐and/or mROS‐mediated apoptosis in astrocytes may be crucial for future therapeutic prevention and treatment of astrocyte‐mediated neurodegenerative diseases in the CNS.