Immunotherapy has emerged as a transformative approach for treating [neurodegenerative diseases[/[diseases[/[diseases[/[diseases[/[diseases[/[diseases[/diseases, leveraging the immune system to target and clear pathological protein aggregates that drive disease progression. The field achieved a landmark milestone with the FDA approval of [lecanemab[/treatments/[lecanemab[/treatments/[lecanemab[/treatments/[lecanemab--TEMP--/treatments)--FIX-- (Leqembi) in 2023 and [donanemab[/treatments/[donanemab[/treatments/[donanemab[/treatments/[donanemab--TEMP--/treatments)--FIX-- (Kisunla) in 2024 for early [Alzheimer's disease[/diseases/[alzheimers[/diseases/[alzheimers[/diseases/[alzheimers--TEMP--/diseases)--FIX--, demonstrating that targeting [Amyloid-Beta (Aβ)[/proteins/[amyloid-beta[/proteins/[amyloid-beta[/proteins/[amyloid-beta--TEMP--/proteins)--FIX-- can produce measurable clinical benefit [1].
Immunotherapeutic strategies for neurodegeneration encompass both passive immunization (administration of monoclonal antibodies) and active immunization (vaccination to stimulate endogenous antibody production). While anti-[Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- antibodies have achieved clinical success, immunotherapies targeting tau] protein] and [alpha-synuclein[/proteins/[alpha-synuclein[/proteins/[alpha-synuclein[/proteins/[alpha-synuclein--TEMP--/proteins)--FIX-- remain in active development, with significant challenges related to intracellular target accessibility [2].
[lecanemab[/treatments/[lecanemab[/treatments/[lecanemab[/treatments/[lecanemab--TEMP--/treatments)--FIX-- is a humanized IgG1 monoclonal antibody that preferentially binds [Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- protofibrils — soluble aggregated forms considered the most neurotoxic species:
- Mechanism: Targets [Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- protofibrils and large soluble oligomers, promoting their clearance through microglial phagocytosis
- CLARITY AD trial: 27% slowing of cognitive decline on CDR-SB over 18 months in early AD (MCI and mild dementia)
- [Amyloid] reduction: Achieved significant reduction in [amyloid PET[/entities/[amyloid-pet[/entities/[amyloid-pet[/entities/[amyloid-pet--TEMP--/entities)--FIX-- signal, with 68% of participants becoming amyloid-negative
- Dosing: 10 mg/kg IV biweekly
- FDA approval: Full approval January 2023; expanded labeling to include subcutaneous formulation in 2025 [3]
[donanemab[/treatments/[donanemab[/treatments/[donanemab[/treatments/[donanemab--TEMP--/treatments)--FIX-- targets pyroglutamate-modified [Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- (AβpE3), a form present predominantly in established amyloid plaques:
- Mechanism: Binds N-terminal pyroglutamate [Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- (AβpE3-42) in deposited plaques, promoting rapid amyloid clearance via Fc receptor-mediated microglial phagocytosis
- TRAILBLAZER-ALZ 2 trial: 35% slowing of cognitive decline on iADRS in the combined tau]-low/medium population over 18 months
- Amyloid reduction: 84% of patients achieved amyloid clearance at 18 months, enabling treatment discontinuation
- Dosing: 700 mg IV monthly for 3 doses, then 1,400 mg monthly; discontinuation protocol when amyloid clearance achieved
- FDA approval: July 2024 for early symptomatic AD [4]
Aducanumab was the first anti-amyloid antibody to receive FDA accelerated approval (June 2021), targeting aggregated forms of [Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- including fibrils and plaques:
- Mixed clinical results across Phase III trials (EMERGE positive, ENGAGE negative)
- Significant controversy over accelerated approval based on amyloid reduction as surrogate endpoint
- Discontinued from the market in November 2024 due to limited commercial uptake
- Provided critical lessons about trial design, patient selection, and the amyloid hypothesis [1]
Several next-generation antibodies are in development:
- Remternetug: Eli Lilly's subcutaneous anti-pyroglutamate [Aβ[/entities/[amyloid-beta[/entities/[amyloid-beta[/entities/[amyloid-beta--TEMP--/entities)--FIX-- antibody, designed for monthly dosing with potentially faster amyloid clearance
- Trontinemab: Roche's brain-shuttle anti-Aβ antibody using transferrin receptor-mediated transcytosis to enhance [BBB[/entities/[blood-brain-barrier[/entities/[blood-brain-barrier[/entities/[blood-brain-barrier--TEMP--/entities)--FIX-- penetration
- Bispecific antibodies: Novel constructs targeting multiple epitopes or combining Aβ targeting with enhanced [BBB[/entities/[blood-brain-barrier[/entities/[blood-brain-barrier[/entities/[blood-brain-barrier--TEMP--/entities)--FIX-- crossing [5]
The first Aβ vaccine trial (AN-1792) was halted in 2002 when 6% of participants developed meningoencephalitis, caused by a pro-inflammatory T-cell response to the full-length Aβ1-42 peptide. Post-mortem analysis revealed near-complete amyloid clearance in some participants, providing proof-of-concept despite the safety failure.
Second-generation vaccines use shortened Aβ fragments to elicit antibody responses without T-cell activation:
- ABvac40: Targets the C-terminal end of Aβ40; Phase II results showed robust anti-Aβ40 antibody response with favorable safety
- UB-311: CpG-adjuvanted Aβ1-14 peptide vaccine; Phase II demonstrated anti-Aβ antibody generation and acceptable safety
- ACI-24.060: Liposomal vaccine displaying Aβ1-15 peptide; in Phase II for Down syndrome-associated AD and early-onset AD
Targeting tau pathology] represents the next frontier in neurodegeneration immunotherapy. Unlike amyloid, [tau[/entities/[tau-protein[/entities/[tau-protein[/entities/[tau-protein--TEMP--/entities)--FIX-- correlates more closely with cognitive decline and neuronal loss. However, tau is predominantly intracellular, presenting unique therapeutic challenges [2].
To date, 14 anti-tau antibodies have been evaluated in clinical trials for tauopathies:
- Semorinemab (RO7105705): Anti-tau antibody targeting the N-terminal domain. Phase II LAURIET trial in moderate AD showed significant slowing of functional decline (ADCS-ADL) but no benefit on cognition (ADAS-Cog) — an unexpected dissociation.
- Bepranemab (UCB0107): Targets the mid-domain of tau, inhibiting cell-to-cell tau propagation]. Phase II in early AD ongoing.
- Zagotenemab (LY3303560): Targets conformational changes in aggregated tau. Phase II trial discontinued after failing to demonstrate clinical benefit.
- Tilavonemab (ABBV-8E12): Anti-tau antibody tested in [PSP[/diseases/[psp[/diseases/[psp[/diseases/[psp--TEMP--/diseases)--FIX--; Phase II failed primary endpoint.
- E2814: Targets the microtubule-binding region of tau; being tested in the [DIAN]-TU prevention trial for dominantly inherited AD [6].
- ACI-35.030: Liposomal vaccine displaying phosphorylated tau peptide (pS396/pS404); Phase Ib/IIa showed robust anti-phospho-tau antibody responses
- AADvac1: Active vaccine targeting mis-disordered tau (amino acids 294–305); Phase II ADAMANT trial showed signals in specific biomarker subgroups
The clinical failure of most anti-tau antibodies reflects fundamental challenges:
- Tau pathology is predominantly intracellular, limiting antibody access
- Extracellular tau represents a small fraction of total pathological tau
- Optimal tau epitope for therapeutic targeting remains unclear (N-terminal, mid-domain, or phospho-epitopes)
- Tau propagation] may occur through multiple mechanisms beyond extracellular transfer
- Patient heterogeneity in tau isoform composition and [phosphorylation] patterns [2]
Targeting [alpha-synuclein (α-syn)[/mechanisms/[alpha-synuclein[/mechanisms/[alpha-synuclein[/mechanisms/[alpha-synuclein--TEMP--/mechanisms)--FIX-- is the primary immunotherapeutic strategy for [Parkinson's disease[/diseases/[parkinsons[/diseases/[parkinsons[/diseases/[parkinsons--TEMP--/diseases)--FIX--, [Lewy body dementia[/diseases/[lewy-body-dementia[/diseases/[lewy-body-dementia[/diseases/[lewy-body-dementia--TEMP--/diseases)--FIX--, and [MSA[/diseases/[msa[/diseases/[msa[/diseases/[msa--TEMP--/diseases)--FIX--.
Five anti-α-synuclein antibodies have entered clinical trials:
- Prasinezumab (PRX002/RO7046015): Targets aggregated α-synuclein. Phase II PASADENA trial showed trends toward motor benefit on MDS-UPDRS Part III but missed primary endpoint. Phase IIb PADOVA trial ongoing with enriched population [7].
- Cinpanemab (BIIB054): Targets aggregated α-synuclein N-terminus. Phase II SPARK trial discontinued after interim analysis showed no efficacy.
- MEDI1341 (Lu AF87908): Targets monomeric and aggregated α-synuclein; Phase I demonstrated dose-dependent CSF free α-synuclein reduction.
- Lu AF82422: Anti-α-synuclein antibody in Phase I/II for MSA.
- UB-312: Active peptide vaccine targeting the C-terminal region of α-synuclein; Phase I showed immunogenicity and acceptable safety
- AFFITOPE PD01A/PD03A: Short peptide mimotopes designed to elicit anti-α-synuclein antibodies; Phase I completed
- ACI-7104.056: Anti-α-synuclein vaccine in preclinical development
Like tau, α is primarily intracellular (Lewy bodies and Lewy neurites), limiting antibody access. Other challenges include:
- Disease heterogeneity within the synucleinopathy spectrum
- Difficulty demonstrating target engagement in vivo (no approved α-synuclein PET tracer)
- Potential protective roles of extracellular α-synuclein that antibody clearance might disrupt
- Optimal timing for intervention remains unknown [7]
[ARIA] is the most significant safety concern with anti-amyloid immunotherapy:
- Vasogenic edema and sulcal effusion on MRI
- Occurs in 12–35% of patients depending on the antibody
- Higher incidence in [APOE4[/diseases/[apoe4[/diseases/[apoe4[/diseases/[apoe4--TEMP--/diseases)--FIX-- burden increases risk
- Rarely symptomatic but may be irreversible
- Mandatory [APOE genotyping before treatment initiation
- Baseline and periodic MRI monitoring (approximately every 3 months during dose escalation)
- Enhanced monitoring for APOE4 homozygotes
- Shared decision-making regarding risk-benefit profile [8]
Beyond targeting pathological proteins, immunomodulatory strategies aim to reshape the neuroinflammatory environment:
- [TREM2[/genes/[trem2[/genes/[trem2[/genes/[trem2--TEMP--/genes)--FIX-- agonists: Antibodies activating [TREM2[/genes/[trem2[/genes/[trem2[/genes/[trem2--TEMP--/genes)--FIX-- to enhance microglial phagocytosis and reduce [neuroinflammation[/mechanisms/[neuroinflammation[/mechanisms/[neuroinflammation[/mechanisms/[neuroinflammation--TEMP--/mechanisms)--FIX--. AL002 (Alector) is in Phase II for AD.
- Anti-CD33 antibodies: CD33 is a negative regulator of microglial phagocytosis; blocking antibodies aim to enhance Aβ clearance.
- Colony-stimulating factor 1 receptor (CSF1R) modulators: Modulate microglial to prevent synapse elimination in AD.
- Combination immunotherapy: Simultaneous targeting of Aβ and tau, or protein targets combined with anti-inflammatory approaches
- Brain-penetrant antibody engineering: Transferrin receptor-mediated transcytosis and other strategies to increase CNS antibody levels
- Intrabodies and nanobodies: Single-domain antibodies that can access intracellular compartments to target tau and α-synuclein aggregates
- Prevention trials: Deploying anti-amyloid immunotherapy in presymptomatic individuals (AHEAD 3-45, A45-INJECT, [DIAN]-TU studies)
- Biomarker-guided treatment: Using plasma [p-tau217[/entities/[p-tau217[/entities/[p-tau217[/entities/[p-tau217--TEMP--/entities)--FIX--, amyloid PET, and tau PET to select patients and monitor treatment response
- Subcutaneous formulations: Improving patient convenience and potentially reducing infusion-related reactions
- [Clinical Trials Index[/[clinical-trials[/[clinical-trials[/[clinical-trials[/[clinical-trials[/[clinical-trials[/clinical-trials
- [Gene Therapy for Neurodegenerative Diseases[/treatments/[gene-therapy[/treatments/[gene-therapy[/treatments/[gene-therapy--TEMP--/treatments)--FIX--
The study of Immunotherapy For Neurodegenerative Diseases has evolved significantly over the past decades. Research in this area has revealed important insights into the underlying mechanisms of neurodegeneration and continues to drive therapeutic development.
Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions.
- [Cummings J, et al. (2025). A 2025 update on treatment strategies for the [Alzheimer's disease[/diseases/[alzheimers[/diseases/[alzheimers[/diseases/[alzheimers--TEMP--/diseases)--FIX-- spectrum. Alzheimers Dement. [PMC12637128)(https://pmc.ncbi.nlm.nih.gov/articles/PMC12637128/)
- [Wang Y, et al. (2025). Immunization targeting diseased proteins in synucleinopathy and tauopathy: insights from clinical trials. Transl Neurodegener. [DOI)(https://link.springer.com/article/10.1186/s40035-025-00490-9)
- [Bhatt DK, et al. (2024). [lecanemab[/treatments/[lecanemab[/treatments/[lecanemab[/treatments/[lecanemab--TEMP--/treatments)--FIX-- and [donanemab[/treatments/[donanemab[/treatments/[donanemab[/treatments/[donanemab--TEMP--/treatments)--FIX-- as Therapies for Alzheimer's Disease. eNeuro. DOI)
- [El-Bakry MG, et al. (2025). Amyloid solutions: lecanemab, gantenerumab, and donanemab in the treatment of [Alzheimer's disease[/diseases/[alzheimers[/diseases/[alzheimers[/diseases/[alzheimers--TEMP--/diseases)--FIX--. Egypt J Neurol Psychiatry Neurosurg. [DOI)(https://link.springer.com/article/10.1186/s41983-025-00968-3)
- [Hamamura K, et al. (2025). Recent Advances in Antibody Therapy for Alzheimer's Disease: Focus on Bispecific Antibodies. Int J Mol Sci. [DOI)(https://www.mdpi.com/1422-0067/26/13/6271)
- [Bhatt D, et al. (2023). Analysis of clinical failure of anti-tau and anti-synuclein antibodies in neurodegeneration using quantitative systems pharmacology. CPT Pharmacometrics Syst Pharmacol. [PMC10474108)(https://pmc.ncbi.nlm.nih.gov/articles/PMC10474108/)
- [Bhatt DK, et al. (2024). An update on immune-based [alpha-synuclein[/proteins/[alpha-synuclein[/proteins/[alpha-synuclein[/proteins/[alpha-synuclein--TEMP--/proteins)--FIX-- trials in [Parkinson's disease[/diseases/[parkinsons[/diseases/[parkinsons[/diseases/[parkinsons--TEMP--/diseases)--FIX--. J Parkinsons Dis. [PMC11638298)(https://pmc.ncbi.nlm.nih.gov/articles/PMC11638298/)
- [Gueorguieva I, et al. (2025). Anti-Amyloid Monoclonal Antibodies for Alzheimer's Disease: Evidence, ARIA Risk, and Precision Patient Selection. J Alzheimers Dis. [PMC12470750)(https://pmc.ncbi.nlm.nih.gov/articles/PMC12470750/)
- [Pasquier F, et al. (2024). Critical assessment of anti-amyloid-β monoclonal antibodies effects in Alzheimer's Disease. Sci Rep. [DOI)(https://www.nature.com/articles/s41598-024-75204-8)
- [Medical Associates of North Georgia. (2025). Immunotherapy for Alzheimer's Disease. Link)
- [Chen X, et al. (2025). Comparisons of efficacy and safety of immunotherapies for Alzheimer's Disease treatment: A network meta-analysis. J Neuroimmunol. DOI)
- [Ross EL, et al. (2025). Clinical Benefits and Risks of Antiamyloid Antibodies in Sporadic AD. J Med Internet Res. DOI)