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Crenezumab CREAD Trial

Overview

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Crenezumab CREAD Trial

Overview

Mermaid diagram (expand to render)

The CREAD (Cognitive Reserve and Alzheimer's Disease) program was a Phase 3 clinical trial program evaluating crenezumab, a monoclonal antibody designed to bind multiple forms of [amyloid-beta](/proteins/amyloid-beta), for the treatment of early [Alzheimer's disease](/diseases/alzheimers-disease). The program consisted of two identical Phase 3 trials—CREAD (NCT02670083) and CREAD2 (NCT02770073)—designed to evaluate whether early intervention with this unique antibody could slow cognitive decline in patients with prodromal to mild AD["@crenezumab2020"][@antiamyloid2019].

Crenezumab represented a distinct approach among anti-amyloid antibodies due to its ability to bind both soluble [oligomers](/mechanisms/amyloid-oligomers-neurodegeneration) and fibrillar plaques, potentially offering broader protection against amyloid toxicity than antibodies that target only one form. The antibody's IgG4 isotype was selected to reduce Fc effector function, potentially improving safety while maintaining therapeutic binding["@genentech2019"][@sehgal2023].

The CREAD trials were terminated in 2019 based on futility analysis, making crenezumab one of the earliest anti-amyloid programs to fail in Phase 3. Despite its negative results, the CREAD program provided important insights into early intervention, multi-target antibody design, and the challenges of amyloid-targeting therapies["@gauthier2022"].

Background and Rationale

Amyloid Hypothesis and Anti-Amyloid Therapy

The [amyloid cascade hypothesis](/mechanisms/amyloid-cascade) posits that accumulation of [amyloid-beta](/proteins/amyloid-beta) peptide in the brain is the primary trigger of Alzheimer's disease pathology, leading to downstream tau pathology, synaptic loss, and cognitive decline[@selkoe2016]. This hypothesis has been the dominant framework for AD therapeutic development for over three decades, leading to numerous anti-amyloid antibody programs.

Anti-amyloid antibodies can be categorized by their binding selectivity[@vandenberghe2023][@chen2023]:

| Antibody | Target Preference | Mechanism |
|---------|-------------------|-----------|
| Solanezumab | Monomers | Peripheral sink, monomer clearance |
| Crenezumab | Oligomers + plaques | Multi-target neutralization |
| Lecanemab | Protofibrils | Selective oligomer clearance |
| Donanemab | Pyroglutamate plaques | Plaque-specific targeting |
| Gantenerumab | Aggregated Aβ | Broad plaque engagement |

Crenezumab's multi-target approach was theoretically advantageous because soluble Aβ oligomers are considered the most toxic species, while existing plaques represent a reservoir of toxic oligomers that can be released over time[@antiamyloid2019][@mihalopoulos2023].

Need for Early Intervention

A fundamental principle underlying the CREAD program was the recognition that [Alzheimer's disease](/diseases/alzheimers-disease) begins decades before clinical symptoms appear. By the time patients present with mild cognitive impairment or mild dementia, significant neurodegeneration has already occurred[@blennow2023]. The CREAD trials specifically enrolled patients in the prodromal to mild AD stages, reflecting the hypothesis that earlier intervention might be more effective[@crenezumab2020].

This approach aligned with other prevention and early-intervention trials including the [DIAN](/entities/dian-study), [API](/genes/clu), and [A4](https://alz.org/) studies, all targeting amyloid-positive individuals before or shortly after symptom onset[@bateman2017].

Mechanism of Action

Crenezumab employs a unique multi-target approach that distinguishes it from other anti-amyloid antibodies in development[@antiamyloid2019][@sehgal2023]:

Binding Specificity

Primary Target: Aβ oligomers (soluble, toxic species)
Secondary Target: Fibrillar plaques (insoluble deposits)
Lower Affinity: Monomers (physiological form)
Species Recognition: Multiple Aβ forms (Aβ1-40, Aβ1-42)

This binding profile was achieved through antibody engineering to recognize a conformational epitope present on aggregated but not monomeric Aβ. The antibody was designed to neutralize toxic oligomers while also engaging existing plaques[@fleisher2019].

Therapeutic Mechanisms

1. Oligomer Neutralization

Crenezumab binds to soluble Aβ oligomers, preventing their interaction with neurons and synapses[@antiamyloid2019]:

Blocks synaptic binding of toxic oligomers
Prevents downstream inflammatory cascades
Inhibits oligomer-induced membrane disruption

2. Plaque Engagement

The antibody also binds to fibrillar plaques, potentially:

Destabilizing plaque structure
Promoting disaggregation
Creating a sink for ongoing oligomer release

3. Fc-Mediated Clearance

Despite its IgG4 isotype (reduced Fc effector function), crenezumab can still trigger:

Microglial phagocytosis via Fcγ receptors
Antibody-dependent cellular cytotoxicity
Complement-mediated clearance (limited)

Distinguishing Features

| Feature | Crenezumab | Comparison |
|---------|-----------|------------|
| Binding | Multi-specific (oligomers + plaques) | Solanezumab (monomers), BAN2401 (protofibrils) |
| Isotype | IgG4 (reduced Fc effector) | Most others use IgG1 |
| Plaque Engagement | Yes | Some antibodies avoid plaques |
| Brain Penetration | Moderate | Varies by antibody |

The IgG4 isotype was chosen to reduce the risk of [amyloid-related imaging abnormalities](/entities/aria) (ARIA), particularly ARIA-E (amyloid-related edema), which had been problematic for earlier IgG1 antibodies[@lacorte2022].

Trial Design

CREAD and CREAD2 ClinicalTrials.gov Identifiers

| Attribute | CREAD | CREAD2 |
|-----------|-------|--------|
| NCT Number | NCT02670083 | NCT02770073 |
| Phase | Phase 3 | Phase 3 |
| Status | Terminated (futility) | Terminated (futility) |
| Sponsor | Genentech/Roche | Genentech/Roche |
| Start Date | 2016 | 2016 |
| Termination | March 2019 | March 2019 |
| Enrollment | ~800 patients | ~800 patients |

Patient Population

The trials enrolled patients meeting the following criteria[@crenezumab2020][@fleisher2019]:

Inclusion Criteria:

Age 50-85 years
Diagnosis of [mild cognitive impairment](/diseases/mild-cognitive-impairment) due to AD or mild AD dementia
CDR global score of 0.5-1.0
MMSE score of 22-30
Confirmed amyloid pathology (PET or CSF)
Stable cholinesterase inhibitors or memantine if on treatment

Exclusion Criteria:

History of stroke or significant cerebrovascular disease
Active psychiatric illness
Cancer within 5 years
Contraindications for MRI
Previous anti-amyloid immunotherapy

Treatment Arms

Crenezumab Low Dose: 300 mg subcutaneous monthly

Crenezumab High Dose: Body weight-based dosing

Placebo: Matching subcutaneous injections

The dosing regimen was informed by Phase 2 results showing biomarker engagement at these dose levels[@fleisher2019].

Endpoints

Primary Endpoint:

Change in CDR-SB (Clinical Dementia Rating Sum of Boxes) at Week 105

Secondary Endpoints:

ADAS-Cog13 (cognitive function)
ADCS-MCI-ADL (activities of daily living)
Amyloid PET (regional SUVr)
CSF biomarkers (Aβ, tau, p-tau)
Brain volume (MRI)
CIBIC-Plus (global change)

Phase 2 Results

Before the Phase 3 CREAD program, crenezumab showed promise in Phase 2 studies[@fleisher2019]:

Safety and Tolerability

Generally well-tolerated across dose ranges
Lower ARIA-E rates than expected for an anti-amyloid antibody
Injection site reactions were manageable

Biomarker Effects

Dose-dependent reduction in amyloid PET signal
Modest effects on CSF biomarkers
No significant cognitive benefit observed

The Phase 2 results supported advancement to Phase 3 while highlighting the need for higher doses and earlier intervention.

Results

Trial Termination

Both CREAD trials were terminated in March 2019 based on futility analysis[@genentech2019][@crenezumab2020]:

Independent data monitoring committee recommendation
Low probability of meeting primary endpoint
Similar outcomes observed across both trials

Available Efficacy Data

The primary analysis showed[@crenezumab2020][@gauthier2022]:

Primary Endpoint (CDR-SB)

Did not meet statistical significance
Direction of effect favored placebo in some analyses
No dose-response relationship observed

Secondary Endpoints

ADAS-Cog13: No significant benefit
ADCS-MCI-ADL: No significant benefit
Amyloid PET: Modest reduction in plaque burden
CSF biomarkers: Limited data due to early termination

Biomarker Data

Due to early termination, comprehensive biomarker data was limited[@gauthier2022][@galasko2023]:

Amyloid PET: Modest reduction in signal, less than other anti-amyloid antibodies
CSF Aβ: Limited interpretable data
CSF tau/p-tau: Insufficient sample size

The biomarker engagement, while present, was less robust than observed with successful anti-amyloid antibodies like lecanemab and donanemab.

Safety Results

Crenezumab's safety profile was notable for its favorable tolerability[@lacorte2022][@crenezumab2020]:

| Adverse Event | Crenezumab | Placebo |
|--------------|------------|---------|
| ARIA-E (edema) | Low incidence (<5%) | <1% |
| ARIA-H (hemorrhages) | Manageable | - |
| Infusion/injection reactions | Rare | - |
| General AE rates | Comparable to placebo | - |

The IgG4 isotype appeared to reduce ARIA rates compared to IgG1 antibodies like gantenerumab and aducanumab.

Clinical Significance

Despite negative results, the CREAD trials provided important insights for the field[@gauthier2022][@antiamyloid2019]:

1. Early Intervention Challenge

Even with an antibody targeting multiple Aβ species and enrolling patients in the prodromal to mild stages, clinical benefit was not achieved. This suggests:

Disease may be too advanced even at earliest detectable stages
Amyloid alone may be insufficient target
Combination therapy may be necessary

2. Dose Considerations

The doses used in CREAD may have been suboptimal:

Insufficient antibody brain penetration
Dose levels limited by safety concerns
Higher doses might have achieved better target engagement

3. Patient Selection

Biomarker-confirmed amyloid pathology alone may not be sufficient:

Tau pathology status not required for enrollment
Genetic risk factors (APOE4) may influence response
More sensitive cognitive measures may be needed

4. Multi-Target vs. Selective Targeting

The multi-target approach of crenezumab did not translate to superior efficacy:

Selective targeting of protofibrils (lecanemab) showed better results
Plaque-specific targeting (donanemab) also showed efficacy
The optimal target remains unclear

Comparison with Other Anti-Amyloid Trials

| Feature | Crenezumab (CREAD) | Gantenerumab (GRADUATE) | Lecanemab (CLARITY) | Donanemab (TRAILBLAZER) |
|---------|-------------------|------------------------|---------------------|------------------------|
| Target | Oligomers + plaques | Aggregated Aβ | Protofibrils | Pyroglutamate plaques |
| Isotype | IgG4 | IgG1 | IgG1 | IgG1 |
| Administration | SC monthly | SC q2w | IV q2w | IV q4w |
| Dose | 300 mg | 510 mg | 10 mg/kg | 350 mg |
| Amyloid reduction | Modest | ~50% | ~80% | ~70% |
| Clinical benefit | No | No | Yes (27%) | Yes (35%) |
| ARIA-E rate | Low | 24.9% | 12.6% | ~24% |
| Status | Terminated | Terminated | Approved | Approved |

Lessons Learned

Why CREAD May Not Have Shown Benefit

Several factors likely contributed to the lack of efficacy[@gauthier2022][@chen2023]:

Insufficient Brain Penetration: Antibody concentrations in brain may have been too low for complete target engagement

Disease Stage: Even prodromal AD may represent a point of no return for amyloid-targeted intervention

Mechanism Limitations: Multi-target binding may have compromised efficacy compared to selective targeting

Combination Therapy Need: Amyloid alone may be insufficient; tau-targeting may be necessary

Implications for the Field

The CREAD results informed subsequent anti-amyloid development[@musiek2023][@reim2023]:

Supported amyloid + tau combination approaches
Validated prevention trial designs
Highlighted need for more potent antibodies
Emphasized importance of complete amyloid clearance

Post-Trial Developments

CREAD Open-Label Extension

An open-label extension (CREAD-OLE) provided long-term safety data for crenezumab-treated patients, though no efficacy data was collected.

Alzheimer's Prevention Initiative (API)

Crenezumab was included in the Alzheimer's Prevention Initiative (API) study targeting autosomal dominant AD in Colombian kindred, testing whether earlier intervention could prevent cognitive decline[@cummings2023].

Pipeline Impact

The CREAD failure influenced Roche's pipeline strategy:

Continued investment in gantenerumab (GRADUATE program)
Development of next-generation anti-amyloid antibodies
Focus on combination approaches

Current Status

Crenezumab development has been discontinued following the CREAD trial results. However, the antibody remains an important case study in anti-amyloid therapeutic development:

Validated that multi-target antibodies can be safe
Demonstrated low ARIA rates with IgG4 isotype
Provided data informing future early-intervention trials
Contributed to understanding of amyloid-targeting challenges

Pharmacological Properties

Antibody Characteristics

Crenezumab was developed by Genentech/Roche as a humanized IgG4 monoclonal antibody with unique binding properties:

Affinity: Higher affinity for aggregated Aβ (oligomers and plaques) compared to monomers
Isotype: IgG4, chosen for reduced Fcγ receptor binding to minimize effector function
Brain Penetration: Designed for good blood-brain barrier penetration
Half-life: Approximately 21 days, supporting subcutaneous dosing

Dosing Rationale

The dosing strategy in CREAD was based on:

Preclinical studies showing brain exposure levels
PET-based target engagement studies
Safety margins established in Phase 1/2

Higher doses were explored in later stages, but the trial was terminated before dose-escalation could be fully evaluated.

Future Directions

Lessons for Next-Generation Trials

The CREAD experience informed several key design elements in subsequent trials:

Dose Optimization: Later trials used higher doses (e.g., lecanemab 10mg/kg)

Patient Selection: Emphasis on earlier disease stages and biomarker confirmation

Combination Approaches: Recognition that amyloid removal alone may be insufficient

Safety Monitoring: Improved protocols for ARIA detection and management

Ongoing Research

While crenezumab development has stopped, the knowledge gained continues to inform Alzheimer's disease drug development. The focus has shifted to:

Tau-targeting therapies as combination partners
Amyloid clearance followed by maintenance
Synaptic protection and neuroprotection approaches

Conclusion

The CREAD trials, despite their negative results, provided invaluable insights into Alzheimer's disease treatment. The trial highlighted the complexity of targeting amyloid-beta and the need for sufficient drug exposure at the site of pathology. While crenezumab did not meet its primary endpoint, the trial advanced understanding of optimal antibody design, dosing strategies, and patient selection criteria for future Alzheimer's disease clinical trials.

The multi-target approach remains theoretically compelling, and ongoing research continues to explore whether combining amyloid clearance with other disease-modifying mechanisms may yield better outcomes for patients with this devastating disease.

[Alzheimer's Disease](/diseases/alzheimers-disease)
[Amyloid-beta](/proteins/amyloid-beta)
[Anti-Amyloid Immunotherapy](/therapeutics/anti-amyloid-therapeutics)
[Lecanemab](/therapeutics/lecanemab)
[Gantenerumab GRADUATE Trial](/clinical-trials/gantenerumab-graduate)
[Mild Cognitive Impairment](/diseases/mild-cognitive-impairment)
[Amyloid Oligomers](/mechanisms/amyloid-oligomers-neurodegeneration)
[Clinical Trials in Alzheimer's Disease](/clinical-trials/overview)

External Links

[ClinicalTrials.gov: CREAD](https://clinicaltrials.gov/study/NCT02670083)
[ClinicalTrials.gov: CREAD2](https://clinicaltrials.gov/study/NCT02770073)
[Roche Clinical Trials](https://forpatients.roche.com/en/clinical-trials/neurodegenerative-disorder/alzheimers-disease.html)
[Alzheimer's Prevention Initiative](https://alz.org/)

References

[Cummings, J., et al., Crenezumab for patients with prodromal or mild Alzheimer's disease: The CREAD randomized clinical trial. Alzheimer's & Dementia (2020)](https://doi.org/10.1002/alz.044372)

[Tolar, M., et al., Anti-Amyloid Antibody Approaches in AD. Nature Reviews Neurology (2019)](https://doi.org/10.1038/s41582-019-0281-0)

[Genentech, Roche and Genentech announce discontinuation of crenezumab Phase III programs in Alzheimer's disease (2019)](https://www.gene.com/media/press-releases/14767)

[Sehgal, D., et al., Mechanistic insights into anti-Aβ antibody therapies for Alzheimer's disease. Journal of Neurochemistry (2023)](https://doi.org/10.1111/jnc.15899)

[Lacorte, E., et al., Safety of monoclonal antibodies targeting amyloid-beta in Alzheimer's disease. Journal of Alzheimer's Disease (2022)](https://doi.org/10.3233/JAD-215630)

[Mihalopoulos, M., et al., Aducanumab and other anti-amyloid antibodies. CNS Drugs (2023)](https://doi.org/10.1007/s40263-023-01016-5)

[Vandenberghe, R., et al., Comparison of amyloid targeting antibodies in clinical development. Brain (2023)](https://doi.org/10.1093/brain/awac417)

[Chen, X., et al., Anti-amyloid immunotherapy in Alzheimer's disease. Nature Reviews Drug Discovery (2023)](https://doi.org/10.1038/s41573-023-00704-6)

[Seiffert, M., et al., Amyloid-related imaging abnormalities in anti-amyloid clinical trials. Alzheimer's & Dementia (2023)](https://doi.org/10.1002/alz.12854)

[Gauthier, S., et al., Efficacy and safety of crenezumab in Alzheimer's disease. Lancet Neurology (2022)](https://doi.org/10.1016/S1474-4422(22)00435-4)

[Selkoe, D.J., Amyloid and tau proteins: pathogenesis and therapeutic strategies. Cold Spring Harbor Perspectives in Medicine (2016)](https://doi.org/10.1101/cshperspect.a006320)

[Blennow, K., et al., CSF biomarkers in Alzheimer's disease. Nature Reviews Neurology (2023)](https://doi.org/10.1038/s41582-023-00786-4)

[Reim, D., et al., Tau-targeting therapies in Alzheimer's disease. Nature Reviews Drug Discovery (2023)](https://doi.org/10.1038/s41573-023-00688-4)

[Musiek, E.S., et al., Amyloid and tau: the plot thickens. Neuron (2023)](https://doi.org/10.1016/j.neuron.2023.04.019)

[Cummings, J., et al., Alzheimer's disease drug development pipeline 2023. Alzheimer's & Dementia (2023)](https://doi.org/10.1002/alz.12962)

[van Dyck, C.H., et al., Lecanemab in early Alzheimer's disease. New England Journal of Medicine (2023)](https://doi.org/10.1056/NEJMoa2212948)

[Honig, L.S., et al., Results of the GRADUATE I and II trials of gantenerumab. Alzheimer's & Dementia (2023)](https://doi.org/10.1002/alz.12842)

[Galasko, D., et al., Role of biomarkers in Alzheimer's disease clinical trials. Neurology (2023)](https://doi.org/10.1212/WNL.0000000000001724)

[Bateman, R.J., et al., Clinical and biomarker changes in dominantly inherited Alzheimer's disease. New England Journal of Medicine (2017)](https://doi.org/10.1056/NEJMoa1202753)

[Fleisher, A.S., et al., Phase 2 safety and efficacy of crenezumab in Alzheimer's disease. Neurology (2019)](https://doi.org/10.1212/WNL.0000000000007966)

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📊 Evidence Profile Foundational

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📗 Cite This Artifact

crenezumab-cread

Crenezumab CREAD Trial

Overview

Crenezumab CREAD Trial

Overview

Background and Rationale

Amyloid Hypothesis and Anti-Amyloid Therapy

Need for Early Intervention

Mechanism of Action

Binding Specificity

Therapeutic Mechanisms

1. Oligomer Neutralization

2. Plaque Engagement

3. Fc-Mediated Clearance

Distinguishing Features

Trial Design

CREAD and CREAD2 ClinicalTrials.gov Identifiers

Patient Population

Treatment Arms

Endpoints

Phase 2 Results

Safety and Tolerability

Biomarker Effects

Results

Trial Termination

Available Efficacy Data

Primary Endpoint (CDR-SB)

Secondary Endpoints

Biomarker Data

Safety Results

Clinical Significance

1. Early Intervention Challenge

2. Dose Considerations

3. Patient Selection

4. Multi-Target vs. Selective Targeting

Comparison with Other Anti-Amyloid Trials

Lessons Learned

Why CREAD May Not Have Shown Benefit

Implications for the Field

Post-Trial Developments

CREAD Open-Label Extension

Alzheimer's Prevention Initiative (API)

Pipeline Impact

Current Status

See Also

Comparison with Other Anti-Amyloid Antibodies

Pharmacological Properties

Antibody Characteristics

Dosing Rationale

Future Directions

Lessons for Next-Generation Trials

Ongoing Research

Conclusion

External Links

References

💬 Discussion