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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT05462106
Other study ID # ACI-24-AD-DS-2102
Secondary ID 2021-006195-1720
Status Recruiting
Phase Phase 1/Phase 2
First received
Last updated
Start date June 21, 2022
Est. completion date June 2026

Study information

Verified date May 2024
Source AC Immune SA
Contact Olivier Sol, MD
Phone +41 21 345 9121
Email clinicaltrials@acimmune.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to assess the safety, tolerability, immunogenicity and pharmacodynamic effects of ACI-24.060 in subjects with prodromal Alzheimer's disease and in non-demented adults with Down syndrome.


Description:

This phase 1b/2 study will be in 2 parts. Study Part 1 will involve subjects with prodromal Alzheimer's disease. Study Part 2 will involve subjects with Down syndrome.


Recruitment information / eligibility

Status Recruiting
Enrollment 140
Est. completion date June 2026
Est. primary completion date June 2026
Accepts healthy volunteers No
Gender All
Age group 35 Years to 85 Years
Eligibility Inclusion Criteria: Study Part 1 1. Age =50 and =85 years at screening. 2. Diagnosis of prodromal AD: MCI due to AD according to National Institute on Aging Alzheimer's Association (NIA-AA) criteria. 3. PET scan at screening consistent with the presence of amyloid pathology. 4. Clinical Dementia Rating (CDR)-Global Score of 0.5. 5. Subjects either not taking any marketed treatment for AD or receiving a stable dose of an acetylcholinesterase inhibitor (ACHEI) and/or memantine for at least 2 months prior to baseline. Study Part 2 1. Age =35 and =50 years at screening (subjects with DS with age =35 and =39 years may be considered on the condition that there is prior evidence of amyloid results compatible with AD pathology at PET-scan and/or in biofluids). 2. Male or female subjects with DS with a cytogenetic diagnosis being either trisomy 21 or complete unbalanced translocation of the chromosome 21. 3. PET scan at screening consistent with the presence of amyloid pathology. 4. Mild to moderate intellectual disability as per Diagnostic and Statistical Manual of Mental Disorders (DSM-5) classification. 5. Subjects must have a study partner who has direct and regular contact, at least 10 hours per week, with the subject and who is able to provide reliable answers to questions related to the subject, according to the study investigator. Exclusion Criteria: 1. Any unstable and/or clinically significant medical condition likely to hamper the evaluation of safety and/or efficacy of the study vaccine (eg, moderate and/or severe untreated obstructive sleep apnea, clinically significant reduction in serum B12 or folate levels, clinically significant abnormalities of thyroid function, stroke, or other cerebrovascular conditions), as per investigator's judgement. 2. DSM-5 criteria for drug or alcohol abuse or dependence currently met within the past 5 years. 3. History or presence of uncontrolled seizures. If history of seizures, they must be well controlled with no occurrence of seizures in the 2 years before study screening. The use of antiepileptic medications is permitted. 4. Concomitant or past history psychiatric or neurologic disorder other than those considered to be related to AD (eg, head injury with loss of consciousness, symptomatic stroke, Parkinson's disease, severe carotid occlusive disease, transient ischemic attacks [TIAs], hemorrhagic and/or non-hemorrhagic stroke). 5. History of meningitis or meningoencephalitis. 6. History of moderate or severe traumatic brain injury. 7. History of inflammatory neurological disorders. 8. History or presence of immunological or inflammatory conditions, including neurological disorders, judged to be clinically significant by the investigator. 9. History of severe allergic reaction (eg, anaphylaxis) including, but not limited to severe allergic reaction to previous vaccines, foods, and/or medications. 10. Significant risk of suicide, defined using the C-SSRS as the subject answering "yes" to suicidal ideation questions 4 or 5 or answering "yes" to suicidal behavior within the past 12 months. 11. MRI scan at screening showing a single area of cerebral vasogenic edema, superficial siderosis, or evidence of a previous macro-hemorrhage or showing more than 4 cerebral microhemorrhages (regardless of their anatomical location or diagnostic characterization as "possible" or "definite"). Evidence of space occupying lesions other than benign meningioma of less than 1 cm diameter, more than 2 lacunar infarcts, or 1 single infarct larger than 1 cm in diameter. Screening MRI scan showing structural evidence of alternative pathology not consistent with AD and is considered to be at the origin of subject's symptoms. 12. Deviations from normal values for hematologic parameters, liver function tests, and other biochemical measures, judged to be clinically significant by the investigator. 13. Subjects with a positive Human Immunodeficiency Virus (HIV-1 and 2) test at screening. 14. Subjects with clinical or laboratory evidence of active hepatitis B or C at screening (eg, HBV or HCV antigens). 15. Subjects with positive syphilis serology consistent with active syphilis at screening. 16. MRI examination cannot be done for any reason, including but not limited to metal implants contraindicated for MRI and/or severe claustrophobia. 17. Any contraindication for PET scan imaging. 18. Any contraindication to lumbar puncture in subjects undergoing this procedure (note: lumbar puncture is optional in subjects with DS). 19. Previous treatment with ACI-24 or any other active immunotherapy against AD at any time in the past unless there is firm evidence that the subject received placebo only and the placebo formulation is not expected to induce any specific immune response. 20. Previous treatment with any investigational and/or marketed passive immunotherapy against AD within 6 months before screening or 5 half-lives, whichever is longer, unless there is firm evidence that the subject received placebo only. 21. Ongoing treatment with any approved anti-amyloid passive immunotherapy for Alzheimer's disease. 22. Use of acetylcholinesterase inhibitor or glutamatergic drugs (eg, memantine, topiramate, lamotrigine) if not on stable dose for at least 2 months before screening. 23. Any vaccine received within the 2 weeks before screening, including an anti-influenza or anti-COVID 19 vaccine received within 4 weeks before randomization. 24. Subjects with treated hypothyroidism not on a stable dose of replacement medication for at least 2 months before screening and having clinically significant abnormal serum T4 and/or thyroid stimulating hormone at screening. 25. Subjects undergoing lumbar puncture and being treated with any anticoagulants or antiplatelet drugs, except aspirin at doses of 100 mg daily or lower. 26. Use of antidepressants (other than selective serotonin reuptake inhibitors/serotonin-norepinephrine reuptake inhibitors at stable dose); typical antipsychotics; ?-aminobutyric acid agonists (eg, gabapentin); or stimulants (eg, methylphenidate, modafinil). Stable doses of atypical antipsychotics or benzodiazepines are only allowed if this is not considered to influence the safety and the efficacy of the study vaccine according to the site investigator and the sponsor medical monitor. 27. Chronic use of opioid analgesics. A limited treatment duration for acute conditions until 24 hours before cognitive assessment is allowed. 28. Current use of immunosuppressant or immunomodulating drugs or their use within the 6 months before study screening. Current use of oral steroids or their use within the 3 months before study screening. Additional Exclusion Criteria in Study Part 2 The following are exclusion criteria at the time of randomization but will not be considered as exclusionary after treatment assignment: 29. Clinical diagnosis of AD dementia in DS as per International Classification of Diseases 10 (ICD-10). 30. DSQIID >20. 31. Intelligence quotient score <40 (KBIT-2).

Study Design


Intervention

Biological:
Placebo
Administration of Placebo
ACI-24.060 at Dose A
Administration of Dose A of ACI-24.060
ACI-24.060 at Dose B
Administration of Dose B of ACI-24.060
ACI-24.060 at Dose C
Administration of Dose C of ACI-24.060
ACI-24.060 at Dose D
Administration of Dose D of ACI-24.060
Placebo
Administration of Placebo
ACI-24.060 at Dose X
Administration of Dose X of ACI-24.060. Dose X will be a dose already tested in Study Part 1
ACI-24.060 at Dose Y
Administration of Dose Y of ACI-24.060

Locations

Country Name City State
Spain Fundació ACE, Institut Català de Neurociències Aplicades Barcelona
Spain Hospital de la Santa Creu i Sant Pau Barcelona
Spain Hospital Universitario Virgen De Las Nieves Granada
Spain Hospital Clínico San Carlos Madrid
Spain Hospital Universitario de la Princesa Madrid
Spain Hospital Universitario Marqués de Valdecilla Santander
Spain Hospital Universitario y Politécnico La Fe Valencia
United Kingdom Cambridge and Peterborough NHS Foundation Trust - Windsor Research Units Cambridge
United Kingdom Liverpool University Hospitals NHS Foundation Trust Liverpool
United Kingdom Re:Cognition Health Limited London
United Kingdom South London and Maudsley NHS Foundation Trust of The Maudsley Hospital London
United Kingdom Oxford Health NHS Foundation Trust Oxford
United States Massachusetts General Hospital Boston Massachusetts
United States University of Kansas Medical Center Research Institute Fairway Kansas
United States Indiana University / IU Health Indianapolis Indiana
United States Vanderbilt University Medical Center Nashville Tennessee
United States Barrow Neurological Institute Phoenix Arizona
United States The Washington University Saint Louis Missouri
United States UT Health San Antonio San Antonio Texas

Sponsors (2)

Lead Sponsor Collaborator
AC Immune SA Worldwide Clinical Trials

Countries where clinical trial is conducted

United States,  Spain,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Other Change from baseline on brain amyloid levels Brain amyloid load measured via PET imaging. An increase indicates a worsening. From Baseline to W48 (Study Part 1)
Other Change from baseline on tau levels Brain tau load measured via PET imaging. An increase indicates a worsening. From Baseline to W48 (Study Part 1) and to W100 (Study Part 2)
Other Change from baseline in cognitive tests - Repeatable Battery for the Assessment of Neuropsychological Status (RBANS) The total scale index score ranges from 40 to 160. A higher score indicates a better outcome. From Baseline to Week 74 (Study Part 1)
Other Change from baseline in cognitive tests - Alzheimer's Disease Assessment Scale-Cognitive Subscale 13 item (ADAS-Cog 13) The score ranges from 0 to 85. A higher score indicates a worse outcome. From Baseline to Week 74 (Study Part 1)
Other Change from baseline in clinical function tests - Clinical Dementia Rating Scale (CDR) The score ranges from 0 to 18. A higher score indicates a worse outcome. From Baseline to Week 74 (Study Part 1)
Other Change from baseline in cognitive tests - Modified Cued Recall Test (mCRT) The modified CRT assesses verbal learning and episodic memory. The score ranges from X to Y. A higher score indicates a better outcome. From Baseline to Week 100 (Study Part 2)
Other Change from baseline in cognitive tests - Cambridge Cognitive Examination for Individuals with Down Syndrome (CAMCOG-DS2) CAMCOG-DS measures cognitive decline. The total score ranges from 0 to 107. A higher score indicates a better outcome. From Baseline to Week 100 (Study Part 2)
Other Change from baseline in cognitive tests - Cambridge Neuropsychological Test Automated Battery-Paired Associates Learning (CANTAB-PAL) The CANTAB-PAL assesses visual memory and new learning. A higher score indicates a better outcome. From Baseline to Week 100 (Study Part 2)
Primary Number of participants with Adverse Events (AEs) assessed by intensity (mild, moderate or severe) and causal relationship (unrelated, unlikely, possibly or probably related) From Screening to Week 74 (Study Part 1)
Primary Number of participants with Adverse Events (AEs) assessed by intensity (mild, moderate or severe) and causal relationship (unrelated, unlikely, possibly or probably related) From Screening to Week 100 (Study Part 2)
Primary Number of participants with abnormal MRI results From Baseline to Week 74 (Study Part 1)
Primary Number of participants with abnormal MRI results From Baseline to Week 100 (Study Part 2)
Primary Number of participants with abnormal physical and neurological examination results From Baseline to Week 74 (Study Part 1)
Primary Number of participants with abnormal physical and neurological examination results From Baseline to Week 100 (Study Part 2)
Primary Number of participants reporting suicidal ideation or behavior using Columbia-Suicide Severity Rating Scale (C-SSRS) From Baseline to Week 74 (Study Part 1)
Primary Number of participants reporting suicidal ideation or behavior using Columbia-Suicide Severity Rating Scale (C-SSRS) From Baseline to Week 100 (Study Part 2)
Primary Change from baseline in Anti-Abeta antibody titers in blood From Baseline to Week 100 (Study Part 2)
Secondary Change from baseline in Anti-Abeta antibody titers From Baseline to Week 74 (Study Part 1)
Secondary Change from baseline on brain amyloid levels Brain amyloid load measured via PET imaging. An increase indicates a worsening. From Baseline to W100 (Study Part 2)
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