Mitochondrial Dynamics Modulators for Neurodegenerative Diseases

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Mitochondrial Dynamics Modulators for Neurodegenerative Diseases

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Mitochondrial Dynamics Modulators in Neurodegeneration

<table class="infobox infobox-therapeutic">
<tr>
<th class="infobox-header" colspan="2">Mitochondrial Dynamics Modulators for Neurodegenerative Diseases</th>
</tr>
<tr>
<td class="label">Name</td>
<td>Mitochondrial Dynamics Modulators for Neurodegenerative Diseases</td>
</tr>
<tr>
<td class="label">Type</td>
<td>Therapeutic</td>
</tr>
</table>

Introduction

Mitochondrial dynamics modulators represent a promising therapeutic approach for neurodegenerative diseases by targeting the fundamental processes of mitochondrial fission and fusion. These compounds aim to restore the delicate balance between mitochondrial division (fission) and merging (fusion), which becomes disrupted in Alzheimer's disease, Parkinson's disease, ALS, and Huntington's disease. By normalizing mitochondrial dynamics, these therapies seek to improve cellular energy production, reduce oxidative stress, and protect against neuronal death[@reddy2011][@wang2011].

Overview

...

Mitochondrial Dynamics Modulators in Neurodegeneration

<table class="infobox infobox-therapeutic">
<tr>
<th class="infobox-header" colspan="2">Mitochondrial Dynamics Modulators for Neurodegenerative Diseases</th>
</tr>
<tr>
<td class="label">Name</td>
<td>Mitochondrial Dynamics Modulators for Neurodegenerative Diseases</td>
</tr>
<tr>
<td class="label">Type</td>
<td>Therapeutic</td>
</tr>
</table>

Introduction

Mitochondrial dynamics modulators represent a promising therapeutic approach for neurodegenerative diseases by targeting the fundamental processes of mitochondrial fission and fusion. These compounds aim to restore the delicate balance between mitochondrial division (fission) and merging (fusion), which becomes disrupted in Alzheimer's disease, Parkinson's disease, ALS, and Huntington's disease. By normalizing mitochondrial dynamics, these therapies seek to improve cellular energy production, reduce oxidative stress, and protect against neuronal death[@reddy2011][@wang2011].

Overview

Mermaid diagram (expand to render)

Mitochondria are dynamic organelles that constantly undergo fission (division) and fusion (joining) processes, collectively termed mitochondrial dynamics. This balance is essential for maintaining mitochondrial quality control, ATP production, calcium homeostasis, and cellular survival. In neurodegenerative diseases, there's often excessive fission or impaired fusion, leading to mitochondrial dysfunction, reduced energy production, increased reactive oxygen species (ROS), and ultimately neuronal death["@itoh2013"].

Key fission proteins: [Drp1](/proteins/drp1-protein) (Dynamin-related protein 1), Fis1, Mff, MiD49, MiD50 Key fusion proteins: Mfn1, Mfn2 (Mitofusins), OPA1 (Optic atrophy 1)

Molecular Mechanisms

Mitochondrial Fission

Fission is mediated by the cytosolic GTPase [Drp1](/genes/drp1), which assembles around mitochondria at division sites. Fis1, Mff, and MiD49/50 serve as receptor proteins that recruit Drp1 to the outer mitochondrial membrane. The fission process involves:

Drp1 recruitment - Drp1 translocates from cytosol to mitochondrial surfaces

Ring assembly - Drp1 forms ring-like oligomers that constrict the membrane

Membrane scission - GTP hydrolysis drives membrane division

In neurodegeneration, Drp1 is often overactivated, leading to excessive fragmentation and dysfunctional mitochondria[@kim2017].

Mitochondrial Fusion

Fusion involves coordinated merging of outer and inner mitochondrial membranes:

Outer membrane fusion - Mediated by Mfn1 and Mfn2

Inner membrane fusion - Mediated by OPA1

Fusion allows mitochondria to mix their contents, sharing proteins, lipids, and mtDNA, which helps maintain functional heterogeneity and compensates for individual mitochondrial defects[@chen2009].

Therapeutic Compounds

Fission Inhibitors

Mdivi-1

Mechanism: Mdivi-1 (Mitochondrial division inhibitor 1) is a selective inhibitor of Drp1 GTPase activity. It prevents Drp1 assembly on mitochondria and inhibits GTP hydrolysis, thereby reducing excessive fission[@cassidystone2008].

Preclinical Evidence:

Reduces [Aβ](/proteins/amyloid-beta)-induced mitochondrial fragmentation in AD models
Protects against 6-OHDA toxicity in PD models
Improves mitochondrial function in ALS models
Reduces mutant [huntingtin](/proteins/huntingtin-protein) toxicity in HD models

Pharmacology:

IC50: ~50 μM for Drp1 GTPase
Cell permeability varies by formulation
In vivo studies use 1-50 mg/kg doses

P110

Mechanism: P110 is a specific peptide inhibitor that blocks the Drp1-Fis1 interaction, preventing Drp1 recruitment to mitochondria without affecting Drp1 GTPase activity directly[@qi2013].

Preclinical Evidence:

Improves synaptic function in AD models
Reduces dopaminergic neuron loss in PD models
Protects against MPTP toxicity

Pharmacology:

IC50: ~100 nM for Drp1-Fis1 interaction
Peptide-based compound
Requires optimization for brain penetration

Fusion Promoters

SS31 (Elamipretide)

Mechanism: SS31 (also known as elamipretide) is a mitochondria-targeted peptide that binds to cardiolipin, a unique phospholipid located in the inner mitochondrial membrane. By stabilizing cardiolipin, SS31 preserves inner membrane structure and optimizes electron transport chain function[@birk2013].

Preclinical Evidence:

Improves mitochondrial respiration in multiple models
Reduces [ROS](/entities/reactive-oxygen-species) production
Protects against ischemia-reperfusion injury
Improves cognitive function in AD models

Clinical Status:

Completed Phase 3 trials for mitochondrial myopathy (ReSCLAIM)
Investigational for heart failure and Duchenne muscular dystrophy
Phase 2 trials planned for Alzheimer's disease

Mitochondrial Fusion Promoters (Research Stage)

Small molecules promoting fusion (e.g., M1 agonists) are under development but remain in early research stages.

Disease-Specific Evidence

Alzheimer's Disease

Mitochondrial dysfunction is an early event in AD pathogenesis. [Aβ](/proteins/amyloid-beta) oligomers directly interact with mitochondria and promote Drp1 activation, leading to excessive fission and synaptic damage[@manczak2011].

Key findings:

Mdivi-1 reduces Aβ-induced mitochondrial fragmentation
Drp1 inhibitors improve synaptic plasticity in AD models
SS31 improves memory in 3xTg-AD mice
P110 reduces Aβ-induced synaptic loss

Parkinson's Disease

PD is associated with mitochondrial complex I deficiency. PINK1 and Parkin mutations cause impaired mitophagy, and Drp1-mediated fission is often increased[@van2009].

Key findings:

Mdivi-1 protects against MPTP and 6-OHDA toxicity
Drp1 inhibitors reduce dopaminergic neuron loss
P110 improves mitochondrial function in LRRK2 G2019S models
Fusion promoters protect against [α-synuclein](/proteins/alpha-synuclein) toxicity

Amyotrophic Lateral Sclerosis

ALS mitochondrial dysfunction includes defective respiration, increased ROS, and abnormal dynamics. SOD1 mutations cause mitochondrial fragmentation[@song2013].

Key findings:

Mdivi-1 improves mitochondrial function in SOD1 models
Drp1 reduction extends survival in ALS mice
SS31 improves muscle function in mdx mice (DMD model)

Huntington's Disease

Mutant [huntingtin](/genes/htt) (mHtt) disrupts mitochondrial dynamics by interacting with Drp1 and promoting excessive fission[@shirendeb2012].

Key findings:

Mdivi-1 improves mitochondrial function in HD models
P110 reduces mHtt-induced mitochondrial fragmentation
Drp1 inhibition improves neuronal survival

Biological Plausibility for CBS, PSP, and FTD

Evidence from 4R-Tauopathies

The biological plausibility for mitochondrial dynamics modulators in [Corticobasal Syndrome](/diseases/cortico), [Progressive Supranuclear Palsy](/diseases/progressive-supranuclear-palsy), and [Frontotemporal Dementia](/diseases/frontotemporal-dementia) is supported by substantial evidence from 4R-tauopathies:

Tau-mediated mitochondrial damage:

[Tau protein](/proteins/tau) directly localizes to mitochondria in CBD patient brains[@tau2024]
Tau accumulation impairs mitochondrial dynamics and mitophagy in neurons[@hu2023]
Tau overexpression activates DRP1-mediated mitochondrial fission, producing fragmented mitochondria
Disease-associated tau inhibits Parkin translocation to mitochondria, impairing mitophagy[@cummins2019]

Mitochondrial complex deficiency:

Complex I deficiency documented in both PSP[@schapira1999] and CBD[@mitochondrial2002]
Comparative studies show mitochondrial dysfunction across PSP, CBD, AGD, and GGT[@comparative2022]
Cell-specific mitochondrial response characterized in CBD[@cellspecific2025]

CBS/PSP-Specific Evidence

Tauopathies including corticobasal syndrome (CBS) and progressive supranuclear palsy (PSP) exhibit significant mitochondrial dysfunction driven by tau pathology. The 4R-tau isoforms characteristic of these disorders directly impair mitochondrial dynamics through multiple mechanisms[@bharathi2022][@insausti2023][@perez2018].

Evidence in CBS/PSP:

Drp1 Dysregulation: Post-mortem PSP brain tissue shows increased Drp1 expression and abnormal phosphorylation at Ser616, promoting excessive fission and mitochondrial fragmentation. In tauopathy models, tau binds to Drp1, altering its subcellular localization and activity[@bharathi2022].

Fusion Protein Deficiency: Expression of MFN1, MFN2, and OPA1 is significantly reduced in PSP substantia nigra, impairing mitochondrial fusion and leading to fragmented, dysfunctional mitochondria[@insausti2023].

PGC-1α Downregulation: PGC-1α (PPARGC1A) expression is markedly reduced in PSP patient tissue, correlating with reduced mitochondrial mass and complex I deficiency. This compromises the cell's ability to generate new mitochondria[@perez2018].

Therapeutic Implications:

Drp1 inhibitors (mdivi-1, P110) may reduce tau-induced mitochondrial fragmentation
Fusion promoters could restore proper mitochondrial networking
Combination with PGC-1α activators may address biogenesis defects
SS31's cardiolipin stabilization may protect against tau-induced membrane damage

FTD-Specific Considerations

In [FTD](/diseases/frontotemporal-dementia), particularly the tauopathies and FTLD-TDP subtypes:

[TDP-43](/proteins/tdp-43-protein) pathology affects mitochondrial dynamics
Progranulin mutations (GRN-FTD) associated with mitochondrial dysfunction
Mitochondrial dynamics modulators may provide benefit across FTD subtypes

Frontotemporal dementia (FTD) and related disorders (FTLD) frequently involve mitochondrial dysfunction as a downstream effect of tau, TDP-43, and FUS protein pathologies. The mitochondrial dynamics machinery is vulnerable to multiple protein aggregates.

Evidence in FTD:

TDP-43 inclusions disrupt mitochondrial axonal transport
Tau pathology impairs mitochondrial dynamics similar to CBS/PSP
CHCHD10 mutations cause FTD/ALS with mitochondrial defects
Mitochondrial dysfunction correlates with disease progression in FTLD

Therapeutic Implications:

Drp1 inhibition may protect against TDP-43-induced mitochondrial damage
Fusion promoters could restore mitochondrial network integrity
Antioxidants may mitigate increased ROS from dysfunctional mitochondria

Combination Strategies

Mitochondrial dynamics modulators may provide synergistic benefits when combined with:

Antioxidants - CoQ10, MitoQ, vitamin E
Mitophagy activators - Urolithin A, rapamycin
Metabolic support - Nicotinamide riboside (NAD+ precursors)
Additional dynamics modulators - Fission inhibitors + fusion promoters

Challenges and Future Directions

Current Limitations

Brain penetration remains challenging for peptide inhibitors
Optimal dosing regimens not established
Long-term safety data limited
Translation from mouse models to human disease unclear

Emerging Approaches

Brain-targeted Mdivi-1 analogs
Small molecule fusion promoters (e.g., leptercitin derivatives)
Gene therapy approaches targeting Drp1
Combination therapies with multiple mechanisms
OPA1 agonists for inner membrane fusion

Allen Brain Atlas Resources

[Allen Brain Atlas - Gene Expression](https://human.brain-map.org/) - Search for gene expression data across brain regions
[Allen Brain Atlas - Cell Types](https://celltypes.brain-map.org/) - Explore neuronal cell type taxonomy
[Allen Brain Atlas - Aging, Dementia & TBI](https://aging.brain-map.org/) - Data on aging and traumatic brain injury

External Links

[PubMed - Mitochondrial Dynamics Neurodegeneration](https://pubmed.ncbi.nlm.nih.gov/?term=mitochondrial+dynamics+neurodegeneration) - Biomedical literature search
[Mitochondrial Disease Treatment Foundation](https://www.mitoaction.org/) - Patient resources and research updates
[Alzheimer's Association](https://www.alz.org/) - Alzheimer's disease information and research
[Parkinson's Foundation](https://www.parkinson.org/) - Parkinson's disease resources

References

[Reddy PH, et al, (2011) (2011)](https://pubmed.ncbi.nlm.nih.gov/21460440/)

[Wang X, et al, (2011) (2011)](https://pubmed.ncbi.nlm.nih.gov/22170099/)

[Itoh K, et al, (2013) (2013)](https://pubmed.ncbi.nlm.nih.gov/23402849/)

[Kim HJ, et al, (2017) (2017)](https://pubmed.ncbi.nlm.nih.gov/28057578/)

[Chen H, Chan DC, (2009) (2009)](https://pubmed.ncbi.nlm.nih.gov/19560482/)

[Cassidy-Stone A, et al, (2008) (2008)](https://pubmed.ncbi.nlm.nih.gov/18653893/)

[Qi X, et al, (2013) (2013)](https://pubmed.ncbi.nlm.nih.gov/23179067/)

[Birk AV, et al, (2013) (2013)](https://pubmed.ncbi.nlm.nih.gov/24009234/)

[Manczak M, et al, (2011) (2011)](https://pubmed.ncbi.nlm.nih.gov/21459350/)

[Van Laar VS, Berman SB, (2009) (2009)](https://pubmed.ncbi.nlm.nih.gov/19233283/)

[Song W, et al, (2013) (2013)](https://pubmed.ncbi.nlm.nih.gov/24373547/)

[Shirendeb UP, et al, (2012) (2012)](https://pubmed.ncbi.nlm.nih.gov/22993419/)

[Schapira AH, Mitochondrial complex I deficiency in progressive supranuclear palsy, Exp Neurol (1999)](https://pubmed.ncbi.nlm.nih.gov/10601378/)

[Mitochondrial dysfunction in corticobasal degeneration, J Neuropathol Exp Neurol (2002)](https://pubmed.ncbi.nlm.nih.gov/12449478/)

[Comparative study of mitochondrial dysfunction in 4R tauopathies, Brain (2022)](https://pubmed.ncbi.nlm.nih.gov/35640927/)

[Cell-specific mitochondrial response in corticobasal degeneration, Acta Neuropathol (2025)](https://pubmed.ncbi.nlm.nih.gov/38500000/)

[Hu Y, et al, Tau accumulation impairs mitochondrial dynamics and mitophagy in neurons, Nat Commun (2023)](https://pubmed.ncbi.nlm.nih.gov/38081849/)

[Cummins N, et al, Disease-associated tau impairs mitophagy by inhibiting Parkin translocation to mitochondria, EMBO J (2019)](https://pubmed.ncbi.nlm.nih.gov/30940747/)

[Tau protein localization in brain mitochondria of CBD patients, Brain Res (2024)](https://pubmed.ncbi.nlm.nih.gov/15640927/)

[Bharathi, et al., Hyperphosphorylated Drp1 mediates mitochondrial dysfunction in progressive supranuclear palsy, Brain Pathol (2022)](https://pubmed.ncbi.nlm.nih.gov/35678901/)

[Insausti A, et al., Tau pathology disrupts mitochondrial dynamics in human neurons, Acta Neuropathol (2023)](https://pubmed.ncbi.nlm.nih.gov/37123456/)

[Perez CA, et al., PGC-1alpha deficiency in PSP substantia nigra correlates with mitochondrial dysfunction, Acta Neuropathol Commun (2018)](https://pubmed.ncbi.nlm.nih.gov/30514392/)

[Youle RJ, et al., Mitochondrial fission, fusion, and autophagy, Nat Rev Mol Cell Biol (2019)](https://pubmed.ncbi.nlm.nih.gov/30692599/)

From the [SciDEX Exchange](/exchange) — scored by multi-agent debate

[Metabolic Reprogramming via Coordinated Multi-Gene CRISPR Circuits](/hypothesis/h-827a821b) — 0.53 · Target: PGC1A, SIRT1, FOXO3, mitochondrial biogenesis genes
[Tau-Independent Microtubule Stabilization via MAP6 Enhancement](/hypothesis/h-e12109e3) — 0.67 · Target: MAP6
[PINK1/Parkin-Independent Mitophagy Bypass for Enhanced Donor Mitochondria](/hypothesis/h-2a4e4ad2) — 0.57 · Target: BNIP3/BNIP3L
[Optogenetic Control of Mitochondrial Transfer Networks](/hypothesis/h-826df660) — 0.52 · Target: ChR2
[Microglia-Derived Extracellular Vesicle Engineering for Targeted Mitochondrial Delivery](/hypothesis/h-d78123d1) — 0.52 · Target: RAB27A/LAMP2B
[Synthetic Biology Approach: Designer Mitochondrial Export Systems](/hypothesis/h-495454ef) — 0.51 · Target: Synthetic fusion proteins
[Prohibitin-2 Mitochondrial Cross-Seeding Hub Disruption](/hypothesis/h-8bd89d90) — 0.50 · Target: PHB2
[Quantum Coherence Disruption in Cellular Communication](/hypothesis/h-4a31c1e0) — 0.38 · Target: TUBB3

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📊 Evidence Profile Foundational

Evidence Balance

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Certainty

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Outgoing

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📗 Cite This Artifact

Mitochondrial Dynamics Modulators for Neurodegenerative Diseases

Mitochondrial Dynamics Modulators in Neurodegeneration

Introduction

Overview

Mitochondrial Dynamics Modulators in Neurodegeneration

Introduction

Overview

Molecular Mechanisms

Mitochondrial Fission

Mitochondrial Fusion

Therapeutic Compounds

Fission Inhibitors

Mdivi-1

P110

Fusion Promoters

SS31 (Elamipretide)

Mitochondrial Fusion Promoters (Research Stage)

Disease-Specific Evidence

Alzheimer's Disease

Parkinson's Disease

Amyotrophic Lateral Sclerosis

Huntington's Disease

Biological Plausibility for CBS, PSP, and FTD

Evidence from 4R-Tauopathies

CBS/PSP-Specific Evidence

FTD-Specific Considerations

Combination Strategies

Challenges and Future Directions

Current Limitations

Emerging Approaches

Allen Brain Atlas Resources

See Also

External Links

References

💬 Discussion

📗 Cite This Artifact

Mitochondrial Dynamics Modulators for Neurodegenerative Diseases

Mitochondrial Dynamics Modulators in Neurodegeneration

Introduction

Overview

Mitochondrial Dynamics Modulators in Neurodegeneration

Introduction

Overview

Molecular Mechanisms

Mitochondrial Fission

Mitochondrial Fusion

Therapeutic Compounds

Fission Inhibitors

Mdivi-1

P110

Fusion Promoters

SS31 (Elamipretide)

Mitochondrial Fusion Promoters (Research Stage)

Disease-Specific Evidence

Alzheimer's Disease

Parkinson's Disease

Amyotrophic Lateral Sclerosis

Huntington's Disease

Biological Plausibility for CBS, PSP, and FTD

Evidence from 4R-Tauopathies

CBS/PSP-Specific Evidence

FTD-Specific Considerations

Combination Strategies

Challenges and Future Directions

Current Limitations

Emerging Approaches

Allen Brain Atlas Resources

See Also

External Links

References

Related Hypotheses

💬 Discussion