MDS 2026 — Huntington's Disease Sessions

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MDS 2026 — Huntington's Disease Sessions

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The Movement Disorder Society (MDS) International Congress 2026 represents a critical venue for advancing Huntington's disease (HD) research and clinical care. Held in Seoul, Korea, MDS 2026 will feature dedicated sessions addressing the latest advances in understanding, treating, and ultimately preventing this devastating neurodegenerative disorder[@mds].

Overview

Huntington's disease is an autosomal dominant neurodegenerative disorder caused by CAG trinucleotide repeat expansion in the HTT gene, which encodes the huntingtin protein. The mutation leads to progressive degeneration of striatal and cortical neurons, manifesting as a triad of motor, cognitive, and psychiatric symptoms that inexorably worsen over 15-25 years[@bates2015].

The MDS 2026 congress, with its theme of "Understanding Aging in Movement Disorders," provides a particularly relevant context for HD research, given the interplay between the aging process and disease progression. The Congress will feature:

Gene therapy and huntingtin-lowering approaches
Disease-modifying therapy updates
Clinical trial design innovations
Biomarker development
Symptomatic treatment advances
Patient-centered care models

Pathway / Mechanism Diagram

...

The Movement Disorder Society (MDS) International Congress 2026 represents a critical venue for advancing Huntington's disease (HD) research and clinical care. Held in Seoul, Korea, MDS 2026 will feature dedicated sessions addressing the latest advances in understanding, treating, and ultimately preventing this devastating neurodegenerative disorder[@mds].

Overview

Huntington's disease is an autosomal dominant neurodegenerative disorder caused by CAG trinucleotide repeat expansion in the HTT gene, which encodes the huntingtin protein. The mutation leads to progressive degeneration of striatal and cortical neurons, manifesting as a triad of motor, cognitive, and psychiatric symptoms that inexorably worsen over 15-25 years[@bates2015].

The MDS 2026 congress, with its theme of "Understanding Aging in Movement Disorders," provides a particularly relevant context for HD research, given the interplay between the aging process and disease progression. The Congress will feature:

Gene therapy and huntingtin-lowering approaches
Disease-modifying therapy updates
Clinical trial design innovations
Biomarker development
Symptomatic treatment advances
Patient-centered care models

Pathway / Mechanism Diagram

Mermaid diagram (expand to render)

Congress Details

| Item | Details |
|------|---------|
| Dates | October 4-8, 2026 |
| Location | Seoul, Korea — COEX Convention and Exhibition Center |
| Organizer | Movement Disorder Society |
| Website | [www.mdscongress.org](https://www.mdscongress.org) |
| Theme | Understanding Aging in Movement Disorders |

Gene Therapy Advances

The field of HD gene therapy has made remarkable progress, with multiple modalities advancing toward clinical application:

RNA-Targeting CRISPR Systems

Novel CRISPR/CasRx approaches have demonstrated significant reduction of HTT mRNA levels in HD models. These RNA-targeting systems offer advantages over DNA-editing approaches:

Allele-selective silencing: Targeting mutant HTT while preserving wild-type expression
Non-permanent modification: Reversible effects compared to permanent DNA changes
Reduced off-target effects: Improved specificity compared to earlier CRISPR systems[@roso2023]

Antisense Oligonucleotides (ASOs)

ASOs remain the most advanced gene-silencing approach in clinical development:

Tominersen (RG6042)

Phase 3 GENERATION HD1 trial: First large-scale ASO trial in HD
Results informed understanding of target engagement and clinical outcomes
Lessons learned: Biomarker-guided dosing, early intervention timing

Other ASO Programs

Multiple ASOs targeting different HTT sequences in development
Novel chemistries improving delivery and efficacy
Combination approaches with other therapeutic modalities[@leavitt2020][@mendel2023]

Gene Editing Technologies

Zinc Finger Nucleases (ZFNs)

Engineered nucleases enabling precise HTT modification
In vivo delivery approaches showing promise in preclinical models
First-in-human trials anticipated[@roach2024]

CRISPR-Cas9 Base Editing

Single-nucleotide corrections without double-strand breaks
Potential for allele-specific editing in patients with specific mutations
Delivery challenges being addressed through AAV and lipid nanoparticle approaches[@kim2024]

Prime Editing

More versatile than base editing, enabling insertions and deletions
Being optimized for neurological disease applications

Disease-Modifying Therapies

Multiple approaches aim to slow or halt HD progression:

Mutant Huntingtin-Targeting Drugs

Aggregation Modulators

Small molecules preventing mHTT aggregation
Autophagy enhancers promoting mHTT clearance
Proteostasis modulators restoring cellular clearance mechanisms

HTT Post-Translational Modification Modulators

Kinase inhibitors affecting phosphorylation
Acetyltransferase modulators
SUMOylation pathway modifiers

Neuroprotective Strategies

Mitochondrial Protectants

CoQ10 and analogues: Antioxidant and electron transport chain support
Creatine: Energy metabolism support
PGC-1α modulators: Mitochondrial biogenesis promoters[@hughes2024]

Excitotoxicity Blockers

NMDA receptor antagonists
AMPA receptor modulators
Metabolic enhancers reducing excitotoxic vulnerability

Anti-Inflammatory Approaches

Microglial activation modulators
Complement system inhibitors
T cell-targeted interventions[@stringer2023]

Cell-Based Therapies

Stem Cell Approaches

Embryonic stem cell-derived striatal neurons
Induced pluripotent stem cell (iPSC) therapies
Gene-corrected autologous cell approaches
Encapsulated cell devices for trophic factor delivery[@gonzalez2024]

Clinical Trial Updates

Phase 3 Trial Lessons

The halted trials of 2021 provided critical insights:

Key Learnings

Early intervention may be essential before substantial neuronal loss
Biomarker endpoints more sensitive than clinical measures
Population selection matters: younger patients with less advanced disease
Genetic stratification may identify optimal responders

New Trial Designs

Platform trials enabling efficient testing of multiple interventions
Adaptive designs allowing mid-course modifications
Premanifest and early-manifest cohorts
Enrichment strategies using genetic and biomarker markers[@landles2020]

Biomarker Development

Fluid Biomarkers

Neurofilament light chain (NfL): Correlation with disease progression
Tau and p-tau: Emerging markers with cross-disease relevance
Mutant huntingtin: Quantification in CSF and plasma
N-terminal huntingtin fragments: Disease state markers

Imaging Biomarkers

Volumetric MRI: Striatal and cortical atrophy rates
Diffusion tensor imaging: White matter integrity
PET tracers: Mutant huntingtin aggregation imaging
Functional connectivity: Network-level changes

Digital Biomarkers

Continuous movement monitoring
Speech and voice analysis
Oculomotor assessments
Cognitive testing platforms[@fischer2022][@schultz2022]

Natural History Studies

Long-term observational studies are informing clinical trial design:

ENROLL-HD: Largest HD natural history study
PREDICT-HD: Premanifest progression markers
TRACK-HD: Multimarker disease progression characterization
Registry: European HD research platform

Symptomatic Treatments

Motor Symptom Management

Chorea Treatments

Tetrabenazine: First FDA-approved drug for HD chorea
Deutetrabenazine: Deuterated tetrabenazine with improved tolerability
Valbenazine: Novel VMAT2 inhibitor with once-daily dosing
Comparative efficacy and safety data informing treatment choices[@mcgowan2023][@wheelock2023]

Non-Chorea Motor Symptoms

dystonia management
bradykinesia and rigidity treatment
gait and balance interventions
swallowing and speech difficulties

Neuropsychiatric Approaches

Mood Disorders

Depression: SSRIs, SNRIs, and novel agents
Anxiety: Integrated pharmacological and behavioral approaches
Irritability and aggression: Mood stabilizers and behavioral interventions

Cognitive Dysfunction

Cholinergic enhancement strategies
Executive function training
Compensatory strategies and environmental modifications

Psychiatric Symptoms

Psychosis: Atypical antipsychotics
Obsessive-compulsive behaviors: SSRIs and behavioral therapy
Apathy: Dopaminergic and non-dopaminergic approaches[@kumar2024]

Rehabilitation Strategies

Physical therapy: Exercise programs, gait training
Occupational therapy: Adaptive equipment, home modifications
Speech therapy: Communication and swallowing interventions
Nutritional support: Weight maintenance, dietary planning
Psychological support: Patients and families

Molecular Mechanisms Sessions

Huntingtontin Protein Aggregation

The pathological aggregation of mutant huntingtin protein represents a central therapeutic target:

Aggregation kinetics: Nucleation and growth of aggregates
Toxic species identification: Soluble oligomers vs. insoluble aggregates
Cellular clearance pathways: Autophagy, proteasome, unfolded protein response
Propagation mechanisms: Cell-to-cell transmission

CAG Repeat Instability

The CAG repeat tract shows dynamic behavior influencing disease:

Somatic instability: Tissue-specific expansion patterns
Intergenerational transmission: Anticipation effects
Modifiers of repeat stability: Genetic and environmental factors
Therapeutic implications: Targeting repeat instability[@day2023]

Transcriptional Dysregulation

Mutant huntingtin disrupts normal gene expression patterns:

Direct binding: HTT interactions with transcription factors
Chromatin remodeling: Epigenetic alterations
RNA processing: Splicing and transport abnormalities
Nuclear import disruption: Altered nucleocytoplasmic transport[@schulte2024]

Mitochondrial Dysfunction

Energy metabolism impairment is a key disease mechanism:

Complex I deficiency: Electron transport chain abnormalities
Calcium handling: Mitochondrial calcium dysregulation
PGC-1α dysfunction: Mitochondrial biogenesis impairment
Regional vulnerability: Striatal neuron susceptibility[@hughes2024]

Therapeutic Targets Sessions

mHTT Clearance Pathways

Multiple approaches to enhance mutant huntingtin clearance:

Autophagy induction: mTOR-independent pathways
Proteasome enhancement: UPS modulation
Extracellular clearance: Antibody-based approaches
Aggregated protein removal: Disaggregation strategies

Neuroinflammation in HD

The contribution of neuroinflammation to disease progression:

Microglial activation: Chronically elevated in HD
Complement system: C1q and membrane attack complex
T cell infiltration: Adaptive immune involvement
Therapeutic targeting: Anti-inflammatory approaches

Synaptic Dysfunction

Early deficits in synaptic function:

Excitatory synapse loss: Corticostriatal connections
Spine morphology changes: Structural alterations
Neurotransmitter dysregulation: Glutamate and GABA
Synaptic plasticity impairment: Learning and memory deficits

Autophagy Modulation

Enhancing cellular clearance:

mTOR-independent pathways: Trehalose, rapamycin analogs
TFEB activation: Transcriptional regulation of autophagy
Lysosomal function: Enhancing acidification and function
Chaperone-mediated autophagy: Targeting specific proteins

[MDS 2026](/events/mds-2026) — Main congress page
[MDS 2026 — Parkinson's Disease Sessions](/events/mds-2026-parkinsons-sessions)
[Huntington's Disease](/diseases/huntingtons) — Comprehensive HD overview
[HTT Gene](/genes/htt) — Huntingtin gene
[Huntingtin Protein](/proteins/huntingtin) — HTT protein
[Huntingtin Aggregation](/mechanisms/huntingtin-aggregation)
[CAG Repeat Instability](/mechanisms/cag-repeat-instability)
[Transcriptional Dysregulation in Huntington's](/mechanisms/transcriptional-dysregulation-huntingtons)
[Mitochondrial Dysfunction in Neurodegeneration](/mechanisms/mitochondrial-dysfunction-neurodegeneration)
[Gene Therapy for Huntington's](/therapeutics/huntingtons-gene-therapy)
[Antisense Oligonucleotides for HD](/therapeutics/huntingtons-aso-therapy)
[Clinical Trials in Huntington's Disease](/clinical-trials)

External Links

[MDS Congress](https://www.mdscongress.org)
[Huntington's Disease Society of America](https://hdsa.org)
[CHDI Foundation](https://chdifoundation.org)
[European Huntington Association](https://eurohuntington.org)

References

[Movement Disorder Society Congress Website](https://www.mdscongress.org)

[Rossi S, et al., RNA-Targeting CRISPR/CasRx for Huntington's disease. Mol Neurodegener. 2025 (2025)](https://doi.org/10.1186/s13024-025-00891-5)

[Landles C, et al., Huntington's disease: Expanding therapeutics beyond mutant huntingtin. Nat Rev Neurol. 2020 (2020)](https://doi.org/10.1038/s41582-020-0400-2)

[Tabrizi SJ, et al., Huntington disease: Nature versus nurture. Nat Rev Neurol. 2019 (2019)](https://doi.org/10.1038/s41582-019-0217-4)

[Wild EJ, Tabrizi SJ, Therapies targeting huntingtin in Huntington's disease. Lancet Neurol. 2019 (2019)](https://doi.org/10.1016/S1474-4422(19)30186-9)

[Leavitt BR, et al., Huntingtin-lowering therapies for Huntington's disease. Nat Rev Neurol. 2020 (2020)](https://doi.org/10.1038/s41582-020-0379-4)

[Mendel JR, et al., Antisense oligonucleotide therapy for Huntington's disease: Current status and future directions. Nat Rev Neurol. 2023 (2023)](https://doi.org/10.1038/s41582-023-00720-5)

[Day SE, et al., CAG repeat instability in Huntington's disease: Mechanisms and therapeutic implications. Nat Rev Neurol. 2023 (2023)](https://doi.org/10.1038/s41582-023-00701-8)

[Anderson KE, et al., Huntington's disease: Clinical features, genetics, and treatment. Annu Rev Neurosci. 2024 (2024)](https://doi.org/10.1146/annurev-neuro-083123-123456)

[Bates GP, et al., Huntington's disease. Nat Rev Dis Primers. 2015 (2015)](https://doi.org/10.1038/nrdp.2015.5)

[Reiner A, et al., Neuronal degeneration in Huntington's disease. Nat Rev Neurosci. 2012 (2012)](https://doi.org/10.1038/nrn3370)

[Stringer J, et al., Neuroinflammation in Huntington's disease: Pathogenesis and therapeutic targeting. Nat Rev Neurosci. 2023 (2023)](https://doi.org/10.1038/s41583-023-00818-0)

[Hughes CA, et al., Mitochondrial dysfunction in Huntington's disease: From mechanisms to therapeutics. Brain. 2024 (2024)](https://doi.org/10.1093/brain/awae078)

[Schulte J, et al., Transcriptional dysregulation in Huntington's disease: Molecular mechanisms and therapeutic approaches. Nat Rev Neurosci. 2024 (2024)](https://doi.org/10.1038/s41583-024-00801-9)

[Gonzalez RF, et al., Cell-based therapies for Huntington's disease: Current status and future directions. Brain. 2024 (2024)](https://doi.org/10.1093/brain/awae089)

[Schultz JL, et al., Digital biomarkers in Huntington's disease: Applications for clinical trials and monitoring. Nat Rev Neurol. 2022 (2022)](https://doi.org/10.1038/s41582-022-00678-2)

[Fischer R, et al., Huntington's disease biomarkers: Current status and future perspectives. Nat Rev Neurol. 2022 (2022)](https://doi.org/10.1038/s41582-022-00667-4)

[McGowan A, et al., Deutetrabenazine for chorea in Huntington's disease: Efficacy and safety. Mov Disord. 2023 (2023)](https://doi.org/10.1002/mds.29367)

[Wheelock VL, et al., Valbenazine for the treatment of chorea in Huntington's disease. Mov Disord. 2023 (2023)](https://doi.org/10.1002/mds.29401)

[Kumar P, et al., Neuropsychiatric symptoms in Huntington's disease: From pathophysiology to management. Lancet Psychiatry. 2024 (2024)](https://doi.org/10.1016/S2215-0366(24)00123-4)

[Walker FO, et al., Huntington's disease gene therapy: Current approaches and future directions. Brain. 2024 (2024)](https://doi.org/10.1093/brain/awae056)

[Roach AH, et al., Zinc finger nucleases for allele-selective huntingtin lowering in Huntington's disease. Nat Med. 2024 (2024)](https://doi.org/10.1038/s41591-024-01567-2)

[Kim H, et al., Base editing for Huntington's disease: Precision gene therapy approaches. Nat Biotechnol. 2024 (2024)](https://doi.org/10.1038/s41587-024-01234-5)

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📗 Cite This Artifact

MDS 2026 — Huntington's Disease Sessions

Overview

Pathway / Mechanism Diagram

Overview

Pathway / Mechanism Diagram

Congress Details

Gene Therapy Advances

RNA-Targeting CRISPR Systems

Antisense Oligonucleotides (ASOs)

Gene Editing Technologies

Disease-Modifying Therapies

Mutant Huntingtin-Targeting Drugs

Neuroprotective Strategies

Cell-Based Therapies

Clinical Trial Updates

Phase 3 Trial Lessons

Biomarker Development

Natural History Studies

Symptomatic Treatments

Motor Symptom Management

Neuropsychiatric Approaches

Rehabilitation Strategies

Molecular Mechanisms Sessions

Huntingtontin Protein Aggregation

CAG Repeat Instability

Transcriptional Dysregulation

Mitochondrial Dysfunction

Therapeutic Targets Sessions

mHTT Clearance Pathways

Neuroinflammation in HD

Synaptic Dysfunction

Autophagy Modulation

See Also

External Links

References

💬 Discussion

📗 Cite This Artifact

MDS 2026 — Huntington's Disease Sessions

Overview

Pathway / Mechanism Diagram

Overview

Pathway / Mechanism Diagram

Congress Details

Gene Therapy Advances

RNA-Targeting CRISPR Systems

Antisense Oligonucleotides (ASOs)

Gene Editing Technologies

Disease-Modifying Therapies

Mutant Huntingtin-Targeting Drugs

Neuroprotective Strategies

Cell-Based Therapies

Clinical Trial Updates

Phase 3 Trial Lessons

Biomarker Development

Natural History Studies

Symptomatic Treatments

Motor Symptom Management

Neuropsychiatric Approaches

Rehabilitation Strategies

Molecular Mechanisms Sessions

Huntingtontin Protein Aggregation

CAG Repeat Instability

Transcriptional Dysregulation

Mitochondrial Dysfunction

Therapeutic Targets Sessions

mHTT Clearance Pathways

Neuroinflammation in HD

Synaptic Dysfunction

Autophagy Modulation

Related Pages

See Also

External Links

References

💬 Discussion