AC Immune

Path: /organizations/ac-immune Type: Biotechnology Company Headquarters: Lausanne, Switzerland Founded: 2003 Stock: NASDAQ (ACIU)

Overview

Path: /organizations/ac-immune Type: Biotechnology Company Headquarters: Lausanne, Switzerland Founded: 2003 Stock: NASDAQ (ACIU)

Overview

AC Immune is a Swiss biotechnology company headquartered in Lausanne, Switzerland, focused on developing novel therapeutics for neurodegenerative diseases, particularly Alzheimer's disease and tauopathies. The company specializes in immunotherapy approaches targeting pathological proteins including tau, amyloid-beta, alpha-synuclein, and TDP-43[@acimmune_website].

Founded in 2003, AC Immune has established itself as a leader in the field of neurodegenerative disease immunotherapy, with a particular focus on tau-targeting approaches. The company's proprietary SupraAntigen™ technology platform enables the development of highly specific vaccines and antibodies against pathological protein aggregates["@supraantigen_platform"].

Company History

Founding and Early Development

AC Immune was founded in 2003 by Dr. Andrea Pfeifer and Prof. Andreas Muhs, based on research from the Ecole Polytechnique Federale de Lausanne (EPFL). The company's early focus was on developing vaccines against amyloid-beta and tau proteins, recognizing that these pathological proteins were central to neurodegenerative disease pathogenesis.

Key historical milestones:

• 2003: Company founded in Lausanne, Switzerland
• 2006: First partnership with Genentech/Roche
• 2012: SupraAntigen™ platform established
• 2016: ACI-35 tau vaccine enters clinical trials
• 2018: NASDAQ IPO (ACIU)
• 2020: ACI-35 Phase 1b results published[@tau_vaccine_aci35]

Pipeline Overview

Tau Programs (Lead Indication)

| Program | Mechanism | Indication | Stage | Partner |
|---------|-----------|-----------|-------|---------|
| ACI-35 | Tau vaccine (phospho-tau) | Alzheimer's disease | Phase 2/3 | Genentech/Roche |
| ACI-35.030 | Next-gen tau vaccine | Alzheimer's disease | Phase 1 | — |
| ACI-302.24 | Anti-tau antibody (C-terminal) | AD/PSP | Phase 1 | — |
| ACI-306.01 | Anti-tau antibody (phospho-specific) | AD/PSP | Preclinical | — |

Amyloid-beta Programs

| Program | Mechanism | Indication | Stage | Partner |
|---------|-----------|-----------|-------|---------|
| ACI-24 | Amyloid-beta vaccine | Alzheimer's disease | Phase 1/2 | — |
| ACI-24.060 | Next-gen Aβ vaccine | Alzheimer's disease | Phase 1 | — |
| Anti-Aβ antibodies | Various | AD | Preclinical | Genentech/Roche |

Alpha-Synuclein Programs

| Program | Mechanism | Indication | Stage |
|---------|-----------|-----------|-------|
| ACI-35.s1 | α-Syn vaccine | Parkinson's disease | Preclinical |
| Anti-α-Syn antibodies | Passive immunotherapy | PD/DLB | Discovery |

TDP-43 Programs

| Program | Mechanism | Indication | Stage |
|---------|-----------|-----------|-------|
| Anti-TDP-43 antibodies | Passive immunotherapy | ALS/FTD | Discovery |

ACI-35: Lead Tau Vaccine Program

Mechanism of Action

ACI-35 is a liposome-based vaccine that targets phosphorylated tau (p-tau) at specific epitopes believed to be critical for tau pathology propagation[@phospho_tau]. The vaccine induces antibodies that:

Clinical Development

Phase 1b Trial (NCT02880982):

• Randomized, placebo-controlled study in 48 patients with mild-to-moderate AD
• Primary endpoint: Safety and tolerability
• Secondary endpoints: Antibody response, cognitive measures
• Results: ACI-35 was well-tolerated with robust IgG antibody response to p-tau[@tau_vaccine_aci35]

• Currently evaluating in larger AD cohorts
• Primary outcomes: ADAS-Cog, CDR-SB
• Biomarker endpoints: CSF p-tau181, tau PET

Safety Profile

Key safety considerations for tau vaccines include[@vaccine_adverse_events]:

• ARIA-E: Amyloid-related imaging abnormalities (edema) — monitored via MRI
• Immune response: Robust antibody titers without excessive inflammation
• Off-target effects: Minimal cross-reactivity with normal tau protein

SupraAntigen™ Platform Technology

AC Immune's proprietary SupraAntigen™ platform enables the generation of highly specific immunogens:

Platform Features

Applications

The platform is applicable to multiple neurodegenerative disease targets:

• Tau: ACI-35, ACI-35.030
• Amyloid-beta: ACI-24 series
• α-Synuclein: α-Syn vaccines
• TDP-43: TDP-43 vaccines

Tau Immunotherapy Rationale

Tau Pathology in Alzheimer's Disease

Tau protein pathology follows a characteristic pattern in AD[@tau_pathology_spread]:

Why Target Tau?

Tau immunotherapy represents a promising approach because[@tau_immunotherapy_2021]:

• Tau pathology correlates more directly with cognitive decline than amyloid
• Tau spreads transsynaptically, providing a mechanism for antibody-mediated prevention
• Tau is intracellular, but antibodies can target extracellular tau species that mediate spreading
• Passive and active immunization approaches are both feasible

Key Partnerships

Genentech/Roche Collaboration

AC Immune's primary partnership is with Genentech (a Roche company)[@genentech_partnership]:

Scope:

• ACI-35 global development and commercialization rights
• Amyloid-beta vaccine program
• Anti-tau antibody programs

• Upfront and milestone payments
• Royalties on commercial sales
• Co-development in key programs

Life Molecular Imaging

• Partnership for tau PET tracer development
• Access to novel imaging agents for clinical trials
• Diagnostic complement to therapeutic programs

Clinical Development Strategy

Biomarker-Driven Approach

AC Immune employs biomarker-based patient selection in clinical trials[@tau_biomarker]:

• Tau PET: Select patients with elevated tau pathology
• CSF biomarkers: p-tau181, p-tau217 for enrollment
• Amyloid status: Confirm amyloid positivity per AT(N) framework

Trial Design

Phase 2/3 ACI-35 Trial:

• Enrollment: Patients with early AD (MCI due to AD or mild AD dementia)
• Biomarker stratification: Tau PET positive required
• Primary endpoint: Clinical Dementia Rating Scale (CDR)
• Duration: 18-24 months

Competitive Landscape

| Company | Drug | Target | Mechanism | Status |
|---------|------|--------|-----------|--------|
| AC Immune | ACI-35 | Phospho-tau | Vaccine | Phase 2 |
| Eli Lilly | Donanemab | Amyloid-beta | Antibody | Approved |
| Biogen/Eisai | Leqembi | Amyloid-beta | Antibody | Approved |
| Biogen | BIIB080 | Tau | ASO | Phase 1/2 |
| Roche | Semorinemab | Tau | Antibody | Phase 2 |
| AbbVie | Etrasimod | Tau | Antibody | Phase 1 |

Financial Information

• Market Cap: ~$300M (as of 2025)
• Cash position: ~$150M
• Cash runway: Through 2026+
• Key investors: Life Sciences Partners, venBio, IDInvest, Bellevue Asset Management

Leadership

• CEO: Dr. Andrea Pfeifer (co-founder)
• CSO: Dr. Luc P. R. B. van der Haar
• CFO: Dr. Jochen B. W. L. Salm
• CMO: Dr. Cedric W. F. Van der Helling
• CTO: Prof. Andreas Muhs (co-founder)

Research Focus Areas

Relevance to PSP and Related Disorders

While AC Immune focuses primarily on Alzheimer's disease, their tau programs have significant relevance to PSP and other 4R-tauopathies[@psp_tau_therapy]:

PSP Applications

• ACI-306.01: Anti-tau antibody targeting p-tau in PSP
• Mechanism: 4R tau aggregation is central to PSP pathology
• Clinical potential: Antibody-based approaches may be applicable to PSP

Broader Tauopathy Applications

• Corticobasal Syndrome: Tau pathology responsive to immunotherapy
• FTD with MAPT mutations: Anti-tau approaches may benefit
• Alzheimer's disease with PSP features: Overlapping pathology

Clinical Trial Pipeline

Ongoing Trials

Planned Trials

• ACI-302.24 Phase 1: Anti-tau antibody for AD/PSP
• Combination studies: Vaccine + antibody approaches

Scientific Publications

AC Immune's science has been published in leading journals:

• ACI-35 Phase 1b results in Alzheimer's and dementia[@tau_vaccine_aci35]
• Tau immunotherapy mechanisms in Nature Reviews Neurology[@tau_immunotherapy_2021]
• Tau pathology spread in brain[@tau_pathology_spread]
• SupraAntigen platform in Vaccine[@supraantigen_platform]

Research and Development Facilities

• Primary site: Lausanne, Switzerland (headquarters)
• Research labs: State-of-the-art facilities in Lausanne
• Clinical operations: Global clinical trial management
• Manufacturing: GMP manufacturing capabilities for clinical supply

Future Directions

Upcoming Milestones

• 2026: ACI-35 Phase 2 topline data expected
• 2026-2027: Initiate Phase 3 if Phase 2 successful
• 2027: Potential BLA/MAA filing

Pipeline Expansion

• Additional tau programs in PSP
• α-Syn programs advancing to IND
• TDP-43 programs in preclinical development

See Also

• [Tau Consortium](/organizations/tau-consortium)
• [4R-Tauopathies](/mechanisms/4r-tauopathies)
• [Tau Immunotherapy](/therapeutics/tau-immunotherapy)
• [Progressive Supranuclear Palsy](/diseases/progressive-supranuclear-palsy)
• [Alzheimer's Disease](/diseases/alzheimers-disease)
• [Parkinson's Disease](/diseases/parkinsons-disease)
• [Biogen](/organizations/biogen) — partner on tau programs
• [Roche](/organizations/roche) — partner on immunotherapy

References