Drp1 inhibition attenuates neurotoxicity and dopamine release deficits in vivo

Rappold, Phillip M.; Cui, Mei; Grima, Jonathan C.; Fan, Rebecca Z.; Mesy-Bentley, Karen L. de; Chen, Linan; Zhuang, Xiaoxi; Bowers, William J.; Tieu, Kim

doi:10.1038/ncomms6244

Cited by 174 publications

(164 citation statements)

References 71 publications

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“…Recent studies with mdivi-1 (mitochondrial division inhibitor), a small molecule, selective inhibitor of DLP1 [17,86], revealed that inhibition of DLP1 exerts protective effects in heart and cerebral ischemiareperfusion models and provides neuroprotection in Parkinson models [30,129]. Mdivi-1 prevented mitochondrial fission, loss of mitochondrial membrane potential, and cell death in acute brain injury.…”

Section: Dlp1 Deficiencymentioning

confidence: 98%

Proliferation and fission of peroxisomes — An update

Schrader

Costello

Godinho

et al. 2016

Biochimica et Biophysica Acta (BBA) - Molecular Cell Research

119

140

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In mammals, peroxisomes perform crucial functions in cellular metabolism, signalling and viral defense which are essential to the health and viability of the organism. In order to achieve this functional versatility peroxisomes dynamically respond to molecular cues triggered by changes in the cellular environment. Such changes elicit a corresponding response in peroxisomes, which manifests itself as a change in peroxisome number, altered enzyme levels and adaptations to the peroxisomal structure. In mammals the generation of new peroxisomes is a complex process which has clear analogies to mitochondria, with both sharing the same division machinery and undergoing a similar division process. How the regulation of this division process is integrated into the cell's response to different stimuli, the signalling pathways and factors involved, remains somewhat unclear. Here, we discuss the mechanism of peroxisomal fission, the contributions of the various division factors and examine the potential impact of post-translational modifications, such as phosphorylation, on the proliferation process. We also summarize the signalling process and highlight the most recent data linking signalling pathways with peroxisome proliferation.

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Section: Dlp1 Deficiencymentioning

confidence: 98%

Proliferation and fission of peroxisomes — An update

Schrader

Costello

Godinho

et al. 2016

Biochimica et Biophysica Acta (BBA) - Molecular Cell Research

119

140

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“…In addition to AD and HD, increased Drp1 activity and mitochondrial fission have also been observed in Parkinson's disease (PD). Dominant-negative inhibition of Drp1 in a PINK1 −/− mouse-knockout model of PD, as well as in 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP)-induced Parkinsonism in mice, prevented neuronal death and rescued the impaired dopamine release that is associated with PD (Rappold et al, 2014). More recent work on the MPTP mouse model of PD supports these findings, as p110-TAT-peptidemediated inhibition of Drp1 localization to mitochondria attenuated the death of dopaminergic neurons (Filichia et al, 2016).…”

Section: Mitochondrial Dynamics In Neurodegenerative Diseasesmentioning

confidence: 99%

Mitochondrial dynamics in neuronal injury, development and plasticity

Flippo

Strack

2017

Journal of Cell Science

175

122

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“…More recently inhibition of Drp1 has been tested in two Parkinson's disease models, a PINK1-/-mouse and a 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) mouse model [ 94 ]. This study is important because it was demonstrated that mdivi-1 crosses the blood-brain barrier and in doing so was able to restore a striatal dopamine release defi cit and reduce neurotoxicity.…”

Section: Fission-fusion Compoundsmentioning

confidence: 95%

Development of Treatments and Therapies to Target Mitochondrial Dysfunction

Helliwell

2016

Mitochondrial Dysfunction in Neurodegenerative Disorders

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Mitochondrial diseases affect 1:10,000 people worldwide, with a further 1:6,000 at risk of developing symptoms, and can be caused by mutations in the nuclear genome or by mutations within/deletion of mitochondrial DNA (mtDNA). There is currently no therapy for patients with these diseases. In addition, mitochondrial dysfunction can be considered contributory or causal for other neurological diseases, such that therapies that improve mitochondrial function may have widereaching benefi ts. This chapter summarizes cell-and animal-based attempts to fi nd a therapy by modulating major mitochondrial pathways including mitochondrial biogenesis, fi ssion, fusion and altering metabolic intermediates, mitophagy and the mammalian target of rapamycin (mTOR) pathway. Clinical trials currently in progress include drugs that are direct or indirect antioxidants, a mitogenesis activator, an antiapoptotic compound and a compound that improves electron transport chain effi ciency.

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Drp1 inhibition attenuates neurotoxicity and dopamine release deficits in vivo

Cited by 174 publications

References 71 publications

Proliferation and fission of peroxisomes — An update

Proliferation and fission of peroxisomes — An update

Mitochondrial dynamics in neuronal injury, development and plasticity

Development of Treatments and Therapies to Target Mitochondrial Dysfunction

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