Synergistic Protective Effects of Mitochondrial Division Inhibitor 1 and Mitochondria-Targeted Small Peptide SS31 in Alzheimer’s Disease

Reddy, P. Hemachandra; Mańczak, Maria; Yin, Xiang; Reddy, Arubala P.

doi:10.3233/jad-170988

Cited by 70 publications

(67 citation statements)

References 57 publications

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“…This reduction is mainly because of reduced Drp1 levels and GTPase Drp1 enzymatic activity. Our observations are strongly supported by earlier cell culture studies in AD (28,40) and HD (31). Another supporting evidence based on transmission electron microscopy (1) in N2a cells treated with Mdivi-1, (2) Drp1 overexpressed plus Mdivi-1 and (3) Drp1 RNA silenced plus Mdivi-1-treated is that significantly increased length of mitochondria and reduced mitochondrial number are likely because of reduced GTPase Drp1 enzymatic activity.…”

Section: Discussionsupporting

confidence: 91%

“…It has been well established that increased Drp1 activity produces excessively fragmented mitochondria in AD neurons (18,23,38–40). Excessive mitochondrial fragmentation is a major feature in neurodegenerative diseases (16–18,20,23,40–44). Reduction in GTPase Drp1 activity is considered as a therapeutic strategy in diseases that involve increased mitochondrial fragmentation and mitochondrial dysfunction (18,20,31).…”

Section: Discussionmentioning

confidence: 99%

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Mitochondrial division inhibitor 1 reduces dynamin-related protein 1 and mitochondrial fission activity

Mańczak

Kandimalla

Yin

et al. 2018

Human Molecular Genetics

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124

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The purpose of our study was to better understand the effects of mitochondrial-division inhibitor 1 (Mdivi-1) on mitochondrial fission, mitochondrial biogenesis, electron transport activities, and cellular protection. In recent years, researchers have found excessive mitochondrial fragmentation and reduced fusion in a large number of diseases with mitochondrial dysfunction. Therefore, several groups have developed mitochondrial division inhibitors. Among these, Mdivi-1 was extensively studied and was found to reduce Drp1 levels and excessive mitochondrial fission, enhance mitochondrial fusion activity and protect cells. However, a recent study by Bordt et al. (2017) (1) questioned earlier findings of the beneficial, inhibiting effects of Mdivi-1. In the current study, we studied the protective effects of Mdivi-1 by studying the following: mRNA and protein levels of electron transport chain (ETC) genes, mitochondrial dynamics and biogenesis genes, enzymatic activities of ETC complexes I, II, III and IV, the mitochondrial network, mitochondrial size & number, Drp1 GTPase enzymatic activity and mitochondrial respiration 1) in N2a cells treated with Mdivi-1, 2) overexpressed with full-length Drp1+Mdivi-1-treated N2a cells and 3) Drp1 RNA silenced+Mdivi-1-treated N2a cells. We found reduced levels of the fission genes Drp1 and Fis1 levels; increased levels of the fusion genes Mfn1, Mfn2, and Opa1; and the biogenesis genes PGC1α, Nrf1, Nrf2, and TFAM. Increased levels mRNA and protein levels were found in ETC genes of complexes I, II and IV genes. Immunoblotting data agreed with mRNA changes. Transmission electron microscopy analysis revealed reduced numbers of mitochondria and increased length of mitochondria 1) in N2a cells treated with Mdivi-1, 2) cells overexpressed with full-length Drp1+ Mdivi-1-treated N2a cells and 3) Drp1 RNA silenced+Mdivi-1-treated N2a cells. Immunofluorescence analysis revealed that mitochondrial network was increased. Increased levels of complex I, II and IV enzymatic activities were found in all 3 groups of cells treated with low concentration of Mdivi-1. Mitochondrial function was increased and GTPase-Drp1 activity was decreased in all 3 groups of N2a cells. These observations strongly suggest that Mdivi-1 is a Drp1 inhibitor and directly reduces mitochondrial fragmentation and further, Mdivi-1 is a promising molecule to treat human diseases with ETC complexes, I, II and IV.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Mitochondrial division inhibitor 1 reduces dynamin-related protein 1 and mitochondrial fission activity

Mańczak

Kandimalla

Yin

et al. 2018

Human Molecular Genetics

Self Cite

124

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“…In one of AD murine models, the SS31 reduced Aβ peptide production, mitochondrial dysfunction, and enhanced mitochondrial biogenesis and synaptic activity (Calkins et al, 2011; Reddy et al, 2017). Recently, a combination of SS31 and the mitochondrial division inhibitor 1 (Mdivi1) was tested in cultured AD cells with positive effects, suggesting that a combined treatment of mitochondria-targeted antioxidants could have higher effectiveness (Reddy et al, 2018).…”

Section: Mitochondrial Therapies In Admentioning

confidence: 99%

Mitochondria as Potential Targets in Alzheimer Disease Therapy: An Update

2019

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Alzheimer disease (AD) is a progressive and deleterious neurodegenerative disorder that affects mostly the elderly population. At the moment, no effective treatments are available in the market, making the whole situation a compelling challenge for societies worldwide. Recently, novel mechanisms have been proposed to explain the etiology of this disease leading to the new concept that AD is a multifactor pathology. Among others, the function of mitochondria has been considered as one of the intracellular processes severely compromised in AD since the early stages and likely represents a common feature of many neurodegenerative diseases. Many mitochondrial parameters decline already during the aging, reaching an extensive functional failure concomitant with the onset of neurodegenerative conditions, although the exact timeline of these events is still unclear. Thereby, it is not surprising that mitochondria have been already considered as therapeutic targets in neurodegenerative diseases including AD. Together with an overview of the role of mitochondrial dysfunction, this review examines the pros and cons of the tested therapeutic approaches targeting mitochondria in the context of AD. Since mitochondrial therapies in AD have shown different degrees of progress, it is imperative to perform a detailed analysis of the significance of mitochondrial deterioration in AD and of a pharmacological treatment at this level. This step would be very important for the field, as an effective drug treatment in AD is still missing and new therapeutic concepts are urgently needed.

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“…In this review, we have illustrated the fundamental role of Mfn2 in mitochondrial function in health and disease, in particular in AD. Recently, different authors have indicated how perturbations in mitochondrial dynamics, particularly in fission and fusion proteins, Drp1, Fis1, OPA1, and Mfn2, can contribute to neuropathology [54][55][56].…”

Section: Mfn2 As a Potential Target In Alzheimer's Diseasementioning

confidence: 99%

Back to The Fusion: Mitofusin-2 in Alzheimer’s Disease

Sita

Hrelia

Graziosi

et al. 2020

JCM

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Mitochondria are dynamic organelles that undergo constant fission and fusion. Mitochondria dysfunction underlies several human disorders, including Alzheimer's disease (AD). Preservation of mitochondrial dynamics is fundamental for regulating the organelle's functions. Several proteins participate in the regulation of mitochondrial morphology and networks, and among these, Mitofusin 2 (Mfn2) has been extensively studied. This review focuses on the role of Mfn2 in mitochondrial dynamics and in the crosstalk between mitochondria and the endoplasmic reticulum, in particular in AD. Understanding how this protein may be related to AD pathogenesis will provide essential information for the development of therapies for diseases linked to disturbed mitochondrial dynamics, as in AD.

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Synergistic Protective Effects of Mitochondrial Division Inhibitor 1 and Mitochondria-Targeted Small Peptide SS31 in Alzheimer’s Disease

Cited by 70 publications

References 57 publications

Mitochondrial division inhibitor 1 reduces dynamin-related protein 1 and mitochondrial fission activity

Mitochondrial division inhibitor 1 reduces dynamin-related protein 1 and mitochondrial fission activity

Mitochondria as Potential Targets in Alzheimer Disease Therapy: An Update

Back to The Fusion: Mitofusin-2 in Alzheimer’s Disease

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