Antioxidant‐Mediated Reversal of Oxidative Damage in Mouse Modeling of Complex I Inhibition

Parameshwaran, Kodeeswaran; Irwin, Michael H.; Steliou, Kosta; Suppiramaniam, Vishnu; Pinkert, Carl A.

doi:10.1002/ddr.21242

Cited by 9 publications

(16 citation statements)

References 79 publications

(79 reference statements)

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“…It is postulated that the antioxidant and antiinflammatory properties of AAM are the most important attributes of this compound [Hnia et al, 2007;Maczurek et al, 2008;Shenk et al, 2009;Mecocci and Polidori, 2012;Sozio et al, 2013;Salminen et al, 2014]. In addition, data from our labs Parameshwaran et al, 2015;Moos et al, 2016] and other studies [Karagiannis and Maulik, 2012;Karagiannis and Ververis, 2012] suggest epigenetic chromatin remodeling may also be involved [Aydin et al, 2012;Jakovcevski and Akbarian, 2012;Lunnon and Mill, 2013;Millan, 2013].…”

Section: Parkinson Diseasementioning

confidence: 73%

“…An optimal balance of BCL2 family proteins is essential in ensuring cell survival [Dixit et al, 2015;Denzer et al, 2016]. Parameshwaran et al [2015] showed that when mice were exposed to rotenone, the induced changes in increased BAX translocation to mitochondria and decreased phospho BCL-associated agonist of cell death were ameliorated by PMX-500FI.…”

Section: Synthetic Carnitine Esters (Carnitinoids)mentioning

confidence: 97%

“…Studies by Parameshwaran et al [2010] showed lipoyl-L-carnitine, PMX-500FI, protected against neuromotor decline in vivo, and reversed rotenone-induced reductions in LTP in the mouse Schaffer collateral-CA1 synapses [Irwin et al, 2013;Parameshwaran et al, 2012Parameshwaran et al, , 2015. Treatment with PMX-500FI also prevented rotenoneinduced decline in presynaptic release and basal synaptic transmission [Parameshwaran et al, 2015]. Mitochondrial apoptotic priming [Gibson and Davids, 2015] is a critical factor in determining whether or not a stressed-cell will undergo apoptosis [for review see Sarosiek et al, 2013].…”

Section: Synthetic Carnitine Esters (Carnitinoids)mentioning

confidence: 99%

“…The carnitinoids PMX-500FI, PMX500DBr, PMX-550B, and PMX-550DBr overcome these deficiencies. They cross the blood-brain-barrier, are actively transported into cells and accumulate inside the mitochondrial matrix, and, importantly, are able to accumulate in the nucleus of cells harboring impaired mitochondria, where they can act as HDACi [Donohoe et al, 2012] to upregulate the proapoptotic protein, BAX [Dmitriev and Papkovsky, 2015;Parameshwaran et al, 2015;Salama et al, 2015;Vahid et al, 2015], and the Nrf2 pathway [Fern andez-Galilea et al, 2015]. Thus, these compounds have therapeutic potential for treating a wide range of neurological disorders, as well as mitochondrial diseases and syndromes, including GWI, all of which share mitochondrial dysfunction in their etiology [Wallace, 2013;Nicolson et al, 2014;Pagano et al, 2014;Pickrell and Youle, 2015 …”

Section: Traumatic Brain Injurymentioning

confidence: 99%

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Epigenetic Treatment of Neurodegenerative Disorders: Alzheimer and Parkinson Diseases

Irwin

Moos

Faller

et al. 2016

Drug Development Research

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Preclinical Research In this review, we discuss epigenetic-driven methods for treating neurodegenerative disorders associated with mitochondrial dysfunction, focusing on carnitinoid antioxidant-histone deacetylase inhibitors that show an ability to reinvigorate synaptic plasticity and protect against neuromotor decline in vivo. Aging remains a major risk factor in patients who progress to dementia, a clinical syndrome typified by decreased mental capacity, including impairments in memory, language skills, and executive function. Energy metabolism and mitochondrial dysfunction are viewed as determinants in the aging process that may afford therapeutic targets for a host of disease conditions, the brain being primary in such thinking. Mitochondrial dysfunction is a core feature in the pathophysiology of both Alzheimer and Parkinson diseases and rare mitochondrial diseases. The potential of new therapies in this area extends to glaucoma and other ophthalmic disorders, migraine, Creutzfeldt-Jakob disease, post-traumatic stress disorder, systemic exertion intolerance disease, and chemotherapy-induced cognitive impairment. An emerging and hopefully more promising approach to addressing these hard-to-treat diseases leverages their sensitivity to activation of master regulators of antioxidant and cytoprotective genes, antioxidant response elements, and mitophagy. Drug Dev Res 77 : 109-123, 2016. © 2016 Wiley Periodicals, Inc.

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Section: Parkinson Diseasementioning

confidence: 73%

Section: Synthetic Carnitine Esters (Carnitinoids)mentioning

confidence: 97%

Section: Synthetic Carnitine Esters (Carnitinoids)mentioning

confidence: 99%

Section: Traumatic Brain Injurymentioning

confidence: 99%

See 2 more Smart Citations

Epigenetic Treatment of Neurodegenerative Disorders: Alzheimer and Parkinson Diseases

Irwin

Moos

Faller

et al. 2016

Drug Development Research

Self Cite

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“…In support of this concept, preliminary results from ongoing studies [Parameshwaran et al, ] show that PMX‐500FI can protect against neuromotor decline in vivo and restore deficits in long‐term potentiation (LTP) induced by rotenone exposure in mice. Thus, as demonstrated in Parameshwaran et al [], PMX‐500FI: Neutralizes synaptic LTP deficits, as evidenced by effects on field excitatory postsynaptic potentials (fEPSP) recorded following theta burst stimulation (Fig. ). Prevents declines in presynaptic release and basal synaptic transmission, also measured by effects on fEPSP amplitudes. Ameliorates declines in basal synaptic transmission, as shown by increased BAX protein translocation to mitochondria and decreases phosphorylated BCL‐associated agonist of cell death (BAD), as determined by western blot analysis. Inhibits decreases in phosphorylation of extracellular signal‐related kinase 1/2 (ERK1/2), as determined by western blot analysis. …”

Section: Novel Carnitinoids: Lipoic Acid Butyric Acid and Mitochondmentioning

confidence: 88%

Bioprotective Carnitinoids: Lipoic Acid, Butyrate, and Mitochondria‐Targeting to Treat Radiation Injury: Mitochondrial Drugs Come of Age

Steliou

Faller

Pinkert

et al. 2015

Drug Development Research

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Preclinical Research Given nuclear-power-plant incidents such as the 2011 Japanese Fukushima-Daiichi disaster, an urgent need for effective medicines to protect against and treat the harmful biological effects of radiation is evident. To address such a challenge, we describe potential strategies herein including mitochondrial and epigenetic-driven methods using lipoic and butyric acid ester conjugates of carnitine. The antioxidant and other therapeutically beneficial properties of this class of agents may protect against ionizing radiation and resultant mitochondrial dysfunction. Recent studies of the compounds described herein reveal the potential-although further research and development is required to prove the effectiveness of this approach-to provide field-ready radiation-protective drugs.

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Toward Mitochondrial Medicine

Dunn

Irwin

Moos

et al. 2018

Mitochondrial Dysfunction Caused by Drugs and Environmental Toxicants

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Antioxidant‐Mediated Reversal of Oxidative Damage in Mouse Modeling of Complex I Inhibition

Cited by 9 publications

References 79 publications

Epigenetic Treatment of Neurodegenerative Disorders: Alzheimer and Parkinson Diseases

Epigenetic Treatment of Neurodegenerative Disorders: Alzheimer and Parkinson Diseases

Bioprotective Carnitinoids: Lipoic Acid, Butyrate, and Mitochondria‐Targeting to Treat Radiation Injury: Mitochondrial Drugs Come of Age

Toward Mitochondrial Medicine

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