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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT06335173
Other study ID # ACU193-201
Secondary ID 2023-509807-34-0
Status Recruiting
Phase Phase 2/Phase 3
First received
Last updated
Start date February 29, 2024
Est. completion date January 2031

Study information

Verified date May 2024
Source Acumen Pharmaceuticals
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The primary purpose of this study is to evaluate the efficacy of ACU193 infusions administered once every four weeks (Q4W) in slowing cognitive and functional decline as compared to placebo in participants with early Alzheimer's disease.


Recruitment information / eligibility

Status Recruiting
Enrollment 2040
Est. completion date January 2031
Est. primary completion date January 2031
Accepts healthy volunteers No
Gender All
Age group 50 Years to 90 Years
Eligibility Inclusion Criteria: - Body weight of at least 30 kilograms (kg) (66 pounds [lbs]) and no more than 160 kg (352 lbs) at Screening - Must consent to apolipoprotein E4 (APOE4) genotype status assessment - Must meet all of the following criteria 1. National Institute on Aging-Alzheimer's Association (NIA-AA) criteria for mild cognitive impairment (MCI) due to Alzheimer's Disease (AD) or probable AD 2. Screening and baseline score between 22 and 30 (inclusive) on the Mini-Mental State Examination (MMSE) 3. Screening score of 0.5 or 1.0 on the Clinical Dementia Rating Global Score (CDR-GS) and Screening score =0.5 on the CDR Memory Box score 4. Evidence of cerebral amyloid accumulation by either PET scan or CSF - If using cholinesterase inhibitors or memantine to treat symptoms related to AD, doses must be stable for at least three months (12 weeks) prior to Baseline and every attempt should be made to keep them at stable doses throughout the study - Must have a reliable informant or study partner who is willing and able to perform all the roles as specified in the study partner Informed Consent Form (ICF) - Female participants must be surgically sterile or be at least one-year post-menopausal. Male participants with a female partner of child-bearing potential must use adequate contraception Exclusion Criteria: - Has any contraindications for MRI studies, including claustrophobia, the presence of metal (ferromagnetic) implants, or a cardiac pacemaker that is not compatible with MRI - MRI of the brain that is inconsistent with MCI or AD or results showing greater than four ARIA-H, presence of any ARIA-E, or superficial siderosis - History of significant or unstable neurological disease, other than AD, which may affect cognition or ability to complete the study, such as other dementias, serious infection of the brain, significant head trauma, uncontrolled seizures, stroke, or ParkinsonĀ“s disease - Current serious or unstable clinically important illness that, in the judgment of the site investigator, is likely to affect cognitive assessment including visual and hearing impairment or affect the participant's safety or ability to complete the study - Malignant disease in the last five years except for resected cutaneous squamous cell carcinoma in situ, basal cell carcinoma, cervical carcinoma in situ, or in situ prostate cancer with a normal posttreatment prostate-specific antibody (PSA) - Geriatric Depression Scale-Short Form (GDS-SF) score >10 or current symptoms meeting Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition (DSM-V), criteria for major depressive disorder or any current primary psychiatric diagnosis other than AD if, in the judgment of the site investigator, the psychiatric disorder or symptom is likely to confound interpretation of drug effect, affect cognitive assessments, or affect the participantĀ“s ability to complete the study - Suicide risk, as determined by meeting any of the following criteria: 1. Any suicide attempt or preparatory acts/behavior on the C-SSRS Baseline/Screening in the last six months 2. Suicidal ideation in the last six months as defined by a positive response to Question 5 (Suicidal Ideation) on the C-SSRS Baseline/Screening 3. Significant risk of suicide, as judged by the site investigator - Conditions that may affect cognitive assessments during the study - Alcohol use disorder and/or substance use disorder within the last five years

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
ACU193
Intravenous ACU193
Placebo
Intravenous Placebo

Locations

Country Name City State
Canada MoCA Research and Innovations Greenfield Park Quebec
Canada Okanagan Clinical Trials Kelowna British Columbia
Canada Parkwood Institute London Ontario
Canada Hippocampe d/b/a Ottawa Memory Clinic Ottawa Ontario
Canada The Kawartha Regional Memory Clinic (KRMC) Peterborough Ontario
Canada Baycrest - The Rotman Research Institute (RRI) Toronto Ontario
Canada Toronto Memory Program (TMP) (Neurology Research Inc.) Toronto Ontario
Canada University Health Network (UHN) - Toronto Western Hospital (TWH) - Krembil Neuroscience Centre (KNC) - Memory Clinic Toronto Ontario
Canada Office of Alexandre Henri-Bhargava, MD Victoria British Columbia
France Amiens university hospital Amiens
France Chu Pellegrin Bordeaux
France Hopital Neurologique Pierre Wertheimer Bron
France Hôpital de la Timone Marseille Cedex 05
France Chu Montpellier Montpellier
France Hopital Lariboisiere Paris
France Institut de la Mémoire et de la Maladie d'Alzheimer -IM2A Paris
France CHU de Rennes, CMRR Rennes
France CHU de NANTES-Hôpital Nord Laennec Saint-Herblain
France Hôpitaux Universitaires de Strasbourg Strasbourg
France Centre de Recherche du Gérontopôle - CHU de Toulouse Hôpital la Grave Toulouse
Germany Charité - Universitaetsmedizin Berlin Berlin
Germany Pharmakologisches Studienzentrum Chemnitz GmbH Chemnitz
Germany University Hospital of Cologne Cologne
Germany Saarland University Hospital Homburg
Germany Zentralinstitut für seelische Gesundheit Mannheim
Germany Technical University of Munich, School of Medicine and Health, Klinikum rechts der Isar Munich
Germany Rostock University Medical Center Rostock
Germany Praxisgemeinschaft Dr. Springub/Schwarz Westerstede
Italy Fondazione Istituto G. Giglio di Cefalù Cefalù
Italy Policlinico San Martino Genova
Italy Fondazione IRCCS Cà Granda Ospedale Maggiore Policlinico Milano
Italy Fondazione IRCCS San Gerardo dei Tintori Monza
Italy Neurology Clinic Perugia
Italy IRCCS Neuromed Pozzilli
Italy Fondazione Policlinico Universitario Agostino Gemelli IRCCS Roma
Italy Sapienza Università di Roma - AOU Policlinico Umberto I Roma
Italy SSD Alzheimer's disease and related dementias Torino
Italy A.O. Piafondazione Card. G. Panico Tricase
Poland Centrum Medyczne Neuromed Bydgoszcz
Poland Krakowska Akademia Neurologii Sp. z o.o. Krakow
Poland RCMed Sochaczew
Poland Centrum Medyczne Senior Sopot
Poland Centrum Medyczne NeuroProtect Warsaw
Spain Fundacio ACE Barcelona
Spain Hospital Universitario Reina Sofia Cordoba
Spain Fundacion Neuropolis - Hospital Viamed Montecanal Cuarte de Huerva Zaragoza
Spain Cae Oroitu Getxo
Spain Hospital Ruber Madrid
Spain Policlínica Gipuzkoa San Sebastian
Spain Fundacion CITA alzheimer San Sebastián Gipuzkoa
Spain Hospital Universitari General de catalunya Sant Cugat Del Vallès Barcelona
Spain Hospital Victoria Eugenia Sevilla
Spain Hospital Universitari i Politècnic La Fe Valencia
United Kingdom Re:Cognition Health - Birmingham Birmingham West Midlands
United Kingdom Re:Cognition Health - Bristol Bristol
United Kingdom Panthera Biopartners - Enfield Enfield Town Greater London
United Kingdom Re:Cognition Health - Guildford Guildford Surrey
United Kingdom Re:Cognition Health - London London Greater London
United Kingdom St. Pancras Clinical Research Ltd. London Greater London
United Kingdom Neuroclin Glasgow Motherwell Lanarkshire
United Kingdom Re:Cognition Health - Plymouth Plymouth Devon
United Kingdom Panthera Bio-Partners - Preston Preston Lancashire
United Kingdom Panthera Bio-Partners - Rochdale Rochdale Greater Manchester
United Kingdom Panthera Biopartners - Sheffield Sheffield Yorkshire
United Kingdom Re:Cognition Health - Winchester Winchester Hampshire
United States Abington Neurological Associates Abington Pennsylvania
United States Neurological Associates of Albany Albany New York
United States IMA Clinical Research - Albuquerque Albuquerque New Mexico
United States JEM Research Institute Atlantis Florida
United States Senior Adult Specialty Research Austin Texas
United States Gadolin Research, LLC Beaumont Texas
United States Alpine Clinical Research Center Boulder Colorado
United States Bradenton Research Center Bradenton Florida
United States The Neurology Center of Southern California - Carlsbad Carlsbad California
United States Columbus Memory Center Columbus Georgia
United States Gil Fernandez-Yera, MD, PA Coral Gables Florida
United States Neurology Clinic. P.C Cordova Tennessee
United States Kerwin Medical Center Dallas Texas
United States Accel Research- Neurostudies Decatur Georgia
United States CenExel - iResearch Atlanta Decatur Georgia
United States Brain Matters Research Delray Beach Florida
United States The Mile High Research Center Denver Colorado
United States Rhode Island Mood and Memory East Providence Rhode Island
United States Neurology Center of North Orange County Fullerton California
United States Hattiesburg Clinic - Memory Center Hattiesburg Mississippi
United States Coral Clinical Research Homestead Florida
United States Irvine Medical Research Irvine California
United States The Alliance for Multispecialty Research LLC (AMR) Knoxville Tennessee
United States K2 Medical Research - Villages Lady Lake Florida
United States Cleveland Clinic - Lou Ruvo Center for Brain Health (CCLRCBH) Lakewood Ohio
United States Las Vegas Medical Research Center Las Vegas Nevada
United States Healthy Brain Research Long Beach California
United States AMC Research Matthews North Carolina
United States Finlay Medical Research Miami Florida
United States Verus Clinical Research Miami Florida
United States Collier Neurologic Specialists (CNS), L.L.C. Naples Florida
United States Yale School of Medicine - Alzheimer's Disease Research Unit (ADRU) New Haven Connecticut
United States Neurological Institute of New York New York New York
United States Boston Center for Memory Newton Massachusetts
United States Keystone Clinical Research Norristown Pennsylvania
United States Office of Jeffrey S. Ross, MD Northbrook Illinois
United States Research Center for Clinical Studies, LLC Norwalk Connecticut
United States Ocala Health - Family Care Specialists - Ocala I Ocala Florida
United States IMA Clinical Research - Phoenix Phoenix Arizona
United States Donald S. Marks, MD. P.C. Plymouth Massachusetts
United States Progressive Medical Research Port Orange Florida
United States Summit Research Network Portland Oregon
United States ActivMed Practices and Research Portsmouth New Hampshire
United States Princeton Psychiatric Center Princeton New Jersey
United States Sharp Mesa Vista Hospital San Diego California
United States Syrentis Clinical Research Santa Ana California
United States CenExel - iResearch Savannah Savannah Georgia
United States CenExel - California Neuroscience Research Medical Group, Inc (CNR) Sherman Oaks California
United States The Cognitive and Research Center of New Jersey Springfield New Jersey
United States Alzheimer's Research and Treatment Center - Stuart Stuart Florida
United States SUNY Upstate Medical University - Upstate University Hospital (SUNY Health Science Center) Syracuse New York
United States K2 Medical Research - Tampa Tampa Florida
United States Charter Research - Lady Lake The Villages Florida
United States CenExel - Advanced Memory Research Institute of NJ Toms River New Jersey
United States Re:Cognition Health - Fairfax Washington District of Columbia
United States Alzheimers Research and Treatment Center - Wellington Wellington Florida
United States KU Wichita Center for Clinical Research Wichita Kansas
United States Charter Research - Winter Park Winter Park Florida
United States Conquest Research Winter Park Florida

Sponsors (1)

Lead Sponsor Collaborator
Acumen Pharmaceuticals

Countries where clinical trial is conducted

United States,  Canada,  France,  Germany,  Italy,  Poland,  Spain,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Change from Baseline in Integrated Alzheimer's Disease Rating Scale (iADRS) Score iADRS is a validated composite of cognition and function made up of Alzheimer's Disease Assessment Scale - Cognitive Subscale 13-item (ADAS-Cog13) and the Alzheimer's Disease Cooperative Study - instrumental Activities of Daily Living scale (ADCS-iADL). ADAS-Cog13 is a rater-administered instrument consisting of 13 items assessing cognitive function areas most typically impaired in AD. ADAS-Cog13 scores range from 0 to 85, with higher scores indicating a greater deficit of global cognition. The ADCS-iADL is a subset of the 23-item ADCS-ADL (items 6a and 7 to 23). The iADLs are more complex skills required to successfully live independently. iADL-items score ranges from 0 to 59 (lower scores indicating greater impairment). The iADRS is calculated as a linear combination of total scores from the ADAS-Cog13 and ADCS-iADL. The iADRS score ranges from 0 to 144 with lower scores indicating worse performance. Baseline up to Week 80
Secondary Change from Baseline in ADCS-iADL Score The ADCS-ADL is a 23-item inventory developed as a rater-administered questionnaire to be answered by a participant's study partner, where a participant's performance level is rated over the last 4 weeks, based on a set of performance descriptions. The ADCS-iADL is a subset of the 23-item ADCS-ADL (items 6a and 7 to 23). The iADLs are more complex skills required to successfully live independently, and include shopping, keeping appointments, traveling outside of the home, making a meal or snack, and reading and writing. The iADL-items score ranges from 0 to 59 with lower scores indicating greater impairment. Baseline up to Week 80
Secondary Change from Baseline in ADAS-Cog13 Score ADAS-Cog is a rater-administered instrument, designed to assess the severity of dysfunction in cognition, characteristic of persons with AD. The ADAS-Cog13, the cognitive subscale of the ADAS, consists of 13 items assessing cognitive function areas most typically impaired in AD: orientation, verbal memory, language, praxis, delayed free recall, and digit cancellation. The scores range from 0 to 85, with higher scores indicating a greater deficit of global cognition. Baseline up to Week 80
Secondary Change from Baseline in Clinical Dementia Rating - Sum of Boxes (CDR-SB) The CDR is obtained through semi-structured interviews of individuals with AD and informants. The ratings are obtained in six domains: memory, orientation, judgment & problem-solving, community affairs, home & hobbies, and personal care. Each domain is rated on a five-point scale of functioning as follows: 0 = no impairment; 0.5 = questionable impairment; 1 = mild impairment; 2 = moderate impairment; and 3 = severe impairment. CDR-SB score is obtained by summing each of the domain scores, with scores ranging from 0 to 18. Higher scores reflect greater cognitive and functional impairment. Baseline up to Week 80
Secondary Change from Baseline in Mini-Mental State Examination (MMSE) MMSE is a standard staging and assessment tool in AD, designed for grading the cognitive state of individuals with AD. The scale comprises tasks concerning orientation, memory, attention, language, and praxis to evaluate an individual's cognitive state. MMSE total score ranges from 0 to 30, with lower scores indicative of greater cognitive impairment. Baseline up to Week 80
Secondary Change from Baseline in Quality of Life in Alzheimer's Disease (QoL-AD) The QOL-AD tool is a 13-item assessment with each question scored on a 4-point scale where 1 = poor quality of life and 4 = excellent quality of life. Scores range from 13 to 52 with higher scores indicating better quality of life. Baseline up to Week 80
Secondary Change from Baseline in Neuropsychiatric Inventory Questionnaire (NPI-Q) Score NPI-Q is a validated questionnaire completed by informants about participants for whom they care. Each of the 12 NPI-Q domains contains a survey question (answered in Yes/No) that reflects the cardinal symptoms of that domain. If the domain response is "Yes," the informant then rates the severity of the symptoms present within the last month on a 3-point scale and the distress of the symptom using a 5-point scale. The total NPI-Q severity score is the sum of the individual severity scores for each symptom and ranges from 0 to 36, with higher scores indicating more severe behavioral impairment. The total NPI-Q distress score is the sum of the individual distress scores for each symptom and ranges from 0 to 60, with higher scores indicating greater caregiver distress. Baseline up to Week 80
Secondary Change from Baseline in EuroQoL 5-Dimension 5-Level (EQ-5D-5L) EQ-5D-5L is a self-report survey that measures quality of life. The EQ-5D-5L consists of an EQ-5D descriptive system and EQ visual analog scale (EQ VAS). The descriptive system comprises five dimensions: mobility, self-care, usual activities, pain/discomfort, and anxiety/depression. Each dimension has five levels, each assigned a unique 1-digit number: no problems, slight problems, moderate problems, severe problems, and extreme problems. The digits are combined into a 5-digit number that describes the participant's health state. The EQ VAS records the participant's health on a vertical visual analog scale, where the endpoints are labeled 0= the best health you can imagine, and 100= the worst health you can imagine. Baseline up to Week 80
Secondary Change from Baseline in Resource Utilization in Dementia (RUD) The RUD questionnaire is a standardized tool and the most widely used instrument for resource use data collection in dementia, enabling comparison of costs of care across countries with differing health care provisions. It is designed to collect data on formal and informal care resource use and to be useful in different care settings, across different countries and care systems, and in both clinical studies and observational cost-of-illness studies. Baseline up to Week 80
Secondary Change from Baseline in Zarit Burden Interview (ZBI) ZBI consists of 22 items. Twenty-one of the items are designed to measure several aspects of burden, whereas Item 22 is a global measure of burden. Response options for each item range from 0-4, and total scores range from 0-88, with higher scores indicating greater self-reported burden. Baseline up to Week 80
Secondary Effect of ACU193 on Clinical Progression as Compared to Placebo Assessed Using Time Saved Analysis as Measured by iADRS Baseline up to Week 80
Secondary Effect of ACU193 on Clinical Progression as Compared to Placebo Assessed Using Time Saved Analysis as Measured by ADCS-iADL Baseline up to Week 80
Secondary Effect of ACU193 on Clinical Progression as Compared to Placebo Assessed Using Time Saved Analysis as Measured by ADAS-Cog13 Baseline up to Week 80
Secondary Effect of ACU193 on Clinical Progression as Compared to Placebo Assessed Using Time Saved Analysis as Measured by CDR-SB Baseline up to Week 80
Secondary Effect of ACU193 on Clinical Progression as Compared to Placebo Assessed Using Time Saved Analysis as Measured by MMSE Baseline up to Week 80
Secondary Percentage of Participants with No Clinical Progression at One Year No clinical progression in participants will be defined as no decline in CDR-SB score. The CDR is obtained through semi-structured interviews of individuals with AD and informants. The ratings are obtained in six domains: memory, orientation, judgment & problem-solving, community affairs, home & hobbies, and personal care. Each domain is rated on a five-point scale of functioning as follows: 0 = no impairment; 0.5 = questionable impairment; 1 = mild impairment; 2 = moderate impairment; and 3 = severe impairment. CDR-SB score is obtained by summing each of the domain scores, with scores ranging from 0 to 18. Higher scores reflect greater cognitive and functional impairment. Baseline up to Week 80
Secondary Number of Participants with Treatment-Related Adverse Events (TEAEs) Baseline up to Week 80
Secondary Number of Participants with Serious Adverse Events (SAEs) and Adverse Events of Special Interest (AESI) Baseline up to Week 80
Secondary Number of Participants who Discontinue or Withdraw due to TEAE Baseline up to Week 80
Secondary Number of Participants with Anti-Drug Antibodies (ADA) and Neutralizing Antibodies Baseline up to Week 80
Secondary Number of Participants with Amyloid-Related Imaging Abnormality with Edema/Effusions (ARIA-E) and ARIA with Hemorrhage/Hemosiderin Deposition (ARIA-H) as Measured by Magnetic Resonance Imaging (MRI) Baseline up to Week 80
Secondary Number of Participants with Suicidal Ideation and Behavior as Measured by Columbia-Suicide Severity Rating Scale (C-SSRS) The C-SSRS includes 'yes' or 'no' responses for assessment of suicidal ideation and behavior as well as numeric ratings for severity of ideation, if present (from 1 to 5, with 5 being the most severe). Greater lethality or potential lethality of suicidal behaviors (endorsed on the behavior subscale) indicates increased risk. Baseline up to Week 80
Secondary Serum Concentration of ACU193 Pre-dose and multiple timepoints post dose up to 80 weeks
Secondary Concentration of ACU193 in Cerebrospinal Fluid (CSF) Up to Week 76
Secondary CSF Concentrations of ACU193 in a Subset of Participants Up to Week 76
Secondary Correlation Between ACU193 Exposure with Clinical Efficacy Measures Correlation between ACU193 exposure and clinical outcomes (including iADRS, CDR-SB, ADCS-iADL, ADAS-Cog13, and MMSE) will be assessed in this study. Baseline up to 80 weeks
Secondary Change From Baseline in Amyloid Plaque Load or Deposition Measured by Positron Emission Tomography (PET) in Centiloids Baseline up to Week 76
Secondary Change from Baseline in Volumetric Magnetic Resonance Imaging (vMRI) of Whole Brain Volume, Ventricular Volume, and Volume of Selected Regions of Interest Baseline up to Week 76
Secondary Target Engagement Assessed by Measurement of ACU193- Amyloid-ß oligomer (AßO) Complex in CSF Up to Week 76
Secondary Change from Baseline in CSF Concentrations of Amyloid, Tau and Other Neurodegenerative Biomarkers Baseline up to Week 76
Secondary Change from Baseline in CSF Concentrations of Amyloid, Tau, and Other Neurodegenerative Biomarkers in a Subset of Participants Baseline up to Week 76
Secondary Change from Baseline in Blood Concentrations of Amyloid, Tau, and Other Neurodegenerative Biomarkers Baseline up to Week 76
Secondary Correlation Between Change in Biomarker that Reflect Disease Progression and Clinical Changes Assessment of the correlation between change in clinical outcomes (iADRS, CDR-SB, ADCS-iADL, ADAS-Cog13, and MMSE) and change in biomarker (amyloid PET) will be determined by computing Pearson's correlation coefficient for each treatment group. Up to 80 weeks
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