Piromelatine 20 mg in Participants With Mild Dementia Due to Alzheimer's Disease
NCT ID: NCT05267535
Last Updated: 2024-06-21
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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ACTIVE_NOT_RECRUITING
PHASE2/PHASE3
225 participants
INTERVENTIONAL
2022-05-12
2025-06-30
Brief Summary
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Detailed Description
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To differentiate between symptomatic effects and potential disease modifying effects of piromelatine, there will be a delayed-start open-label extension period of 12 months treatment wherein placebo-treated participants will be treated with piromelatine (20 mg daily) and the piromelatine-treated patients will be continued. This exploratory phase is aimed to continue randomized assignment of piromelatine treatment, long-term (18 months overall) to evaluate its potential disease modifying effect compared to patients in the placebo-randomized group who started the treatment after a 6-month delay.
The primary efficacy analysis (blinded) is planned after completion of the 26 weeks double blind period. If efficacy is not confirmed, then the study will be ended without completing the extension period
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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Piromelatine 20 mg
Piromelatine 20 mg tablets once daily taken before going to bed, preferably between 2100h and 2300h, and after food consumption.
Piromelatine 20 mg
Tablets
Placebo
Matched placebo tablets, with identical features to the piromelatine tablets, will be used as control treatment
Placebo
Tablets
Interventions
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Piromelatine 20 mg
Tablets
Placebo
Tablets
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Participant is an outpatient living at home or in an assisted living facility and is willing to attend all planned visits during the study.
* The participant has a study partner (who is not expected to change during the study) who will accompany the patient to the clinic, and/or be available by telephone at designated times, monitor administration of prescribed medications, control the minimum 2 hour daily light exposure requirement. The study partner must, in the opinion of the investigator, have enough contact with the participant to be able to perform the duties described above.
* Signed informed consent from the patient who has the capacity to provide informed consent as judged by the study investigator
* Signed informed consent from the study partner.
* Meets NIA AA research criteria for probable AD (McKhann, Knopman et al. 2011).
* Patient has a clearly documented history of cognitive decline over at least 12 months.
* Patient has MRI/CT scan, performed within 12 months before Screening, with findings consistent with the diagnosis of AD without any other clinically significant comorbid pathologies as detailed in Appendix 3. If MRI/CT was not performed within 12 months before Screening, it can be done during the screening period
* MMSE score of 20 26 (inclusive) at Screening and stability of MMSE - no more than three-point change on successive screening and baseline visits before randomization.
* Patient has a CDR GS of 0.5 1 (mild dementia) at Screening.
* Patients taking acetylcholinesterase inhibitors and or memantine for the treatment of AD may be enrolled if the patient has been taking such medication for at least 6 months before Visit 2 (Baseline) and is stable on any dose for the last 4 months prior to Baseline, and if the dose is not expected to change during study participation.
* Patients not receiving acetylcholinesterase inhibitors may be enrolled but must be stable off acetylcholinesterase inhibitors for at least 3 months before Baseline, and agreeable to not starting throughout the first 26 weeks of the trial.
* Patient has a negative drug screen (benzodiazepines or opiates) at Screening. Positive drug screen of BZDs, is allowed only if the use is intermittent and drug intake was 4 days or more before the visit
* Female patients must have had last natural menstruation ≥ 24 months before Screening OR be surgically sterile.
* Male patients and their female spouse/partners who are of childbearing potential must agree to use highly effective methods of contraception, consisting of 2 forms of birth control (at least one of which must be a barrier method) starting at Screening, throughout the study and for 90 days post last dose, OR be surgically sterile.
* Patients who are taking medications for non excluded concurrent medical conditions should be on a stable dose for at least 4 weeks before Screening. Patients taking allowed antidepressants (see Section 12.9) should be on a stable dose for at least 3 months before Screening and throughout the study
* Patient has ability and commitment to spend at least 2 hours per day exposed to daylight (preferably outside but can be next to a window if weather or personal situation does not permit).
* Participant and study partner have the ability to read and write in English or Spanish and have hearing, vision, and physical abilities adequate to perform assessments (corrective aids allowed).
* Participant and study partner are fully vaccinated for COVID 19 including booster doses as indicated (6 months post second dose). Having been diagnosed with COVID 19 after completing the initial full Covid vaccine would meet the requirements for a booster shot
Exclusion Criteria
* Patient is 2:107,510,000-107,540,000 polymorphism carrier.
* Patient has an alternative cause for dementia other than AD.
* A past or recent CT or MRI scan or report indicating any cortical infarct defined as \> 1.5 cm3; more than 2 lacunar infracts defined as ≤ 1.5 cm3; or diffuse white matter disease), Fazekas score of more than 1 on MRI or CT scan (more details Appendix 3).
* Patient has evidence of any clinically significant neurodegenerative disease, or other serious neurological disorders other than AD as detailed in Appendix 3,
* Patient has a concurrent psychiatric disorder that prevents his/her participation in the trial including but not limited to Schizophrenia, Bipolar and related disorders, Substance use disorders within the past 2 years, major depression, etc.
* Patient has a history of uncontrolled or untreated cardiovascular, endocrine, gastrointestinal, respiratory, or rheumatologic disorders within the past 5 years.
* Patient has a history of severe agitation and medically treated agitation.
* Patient has a history of serious infectious disease including:
* Neurosyphilis
* Meningitis
* Encephalitis
* Patient has a history of a primary or recurrent malignant disease that has not been in remission for \> 5 years prior to the Screening visit, with the exceptions of excised cutaneous squamous cell carcinoma in situ, basal cell carcinoma without recurrences; and history of intraductal breast cancer, cervical carcinoma in situ, or in situ prostate cancer resected over 5 years previously. (For resected in situ prostate cancer, i.e., high grade intraepithelial neoplasia, the patient must have a normal prostate specific antigen \[PSA\] prior to Screening and no increase in PSA since his resection surgery).
* Patient has severe pain that is likely to interfere with sleep (in the opinion of the investigator).
* Patient has any concomitant documented progressive disease likely to interfere with the conduct of the study, particularly:
* Liver disease with aspartate aminotransferase (AST), alanine aminotransferase (ALT) or gamma glutamyltransferase (GGT) \> 3 times the upper limits of normal (ULN)
* Total bilirubin \> 3 times the ULN
* Mean corpuscular volume \> 95 µ3 if due to chronic alcoholism
* Renal failure with creatinine \< 30 ml / min
* Patients that are taking prohibited medications according to Appendix 2 See also section 12.9.
* Continuous use of benzodiazepines or other sedative hypnotics during the 2 weeks before Screening (see Section 12.9).
* Patient has a history of chronic use (more than 3 months of continuous use) and abuse of benzodiazepines or other sedative hypnotics.
* Use of any kind of melatonin/melatonin agonist during the 2 weeks before Screening (see Section 12.9).
* Patient has known or suspected hypersensitivity to exogenous melatonin or melatonin receptor agonists.
* Patient has clinically significant abnormal laboratory findings that have not been approved by the study safety officer.
* Patient has persistent bradycardia (heart beat \< 50 bpm) or tachycardia (heart beat \> 100 bpm).
* Patient has atrioventricular block (type II/Mobitz II and type III), congenital long QT syndrome, sinus node dysfunction or a marked prolongation of QTc interval (repeated demonstration in ECGs of QTc interval \> 450 msec for males and \> 470 msec for females using Fridericia's formula: QTc = QT/cube root of RR).
* Patient has other serious diseases that could interfere with patient assessment, in the opinion of the investigator.
* Patient has untreated B12 and/or folic acid deficiency.
* Patient has participated in a clinical trial with any investigational agent within 3 months before Screening. Participants in any former monoclonal antibody clinical trial for AD are not eligible until 6 months after the last visit of the previous study. Patients who have received active vaccine for AD in the past will be excluded.
* Patient with a body mass index (BMI) above 35 or below 18.
* Lifestyle exclusions:
* Patients unwilling to limit alcohol intake to less than 30 g of pure alcohol per day (see Appendix 1) and to abstain after 2000h throughout the study
* Patients unwilling to be exposed to at least 2 hours of daylight each day
* Divergence from the accepted level of study medication compliance (70% 130% of expected consumption) as verified at Visit 2 (see Section 12.10)
* Patients consuming more than 7 cups of tea or coffee (or equivalent amount of caffeine \[650 mg\] in other caffeinated beverages) per day
* Patients with an irregular lifestyle or life pattern (e.g., shift workers, patients likely to be jet lagged)
* Patients with evidence of serious risk of suicide based on the Columbia-Suicide Severity Rating Scale, i.e., active suicidal ideation with some intent to act, with or without a specific plan (a positive response to Suicidal Ideation Items 4 or 5) in the 6 months prior to Screening, OR with evidence of suicidal behavior in the 2 years prior to Screening (a positive response to any of the 5 Suicidal Behavior Items {actual attempt, interrupted attempt, aborted attempt, preparatory acts, or behavior}), OR who, in the opinion of the investigator, present a serious risk of suicide.
60 Years
85 Years
ALL
No
Sponsors
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Syneos Health
OTHER
Neurim Pharmaceuticals Ltd.
INDUSTRY
Responsible Party
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Principal Investigators
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Lon Schneider, MD
Role: STUDY_CHAIR
Keck School of Medicine of USC, Los Angeles, CA
Locations
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ATP Clinical Research
Costa Mesa, California, United States
Collaborative Neuroscience Research, LLC
Long Beach, California, United States
Asclepes Research Centers, P.C. Dba Alliance Research
Long Beach, California, United States
Pacific Research Network, LLC
San Diego, California, United States
RAA Apex Acquisition LLC DBA Syrentis Clinical Research
Santa Ana, California, United States
The Mile High Research Center
Denver, Colorado, United States
Linfritz Research Institute Inc.
Coral Gables, Florida, United States
Finlay Medical Research Corp.
Greenacres City, Florida, United States
Velocity Clinical Research, Inc
Hallandale, Florida, United States
K2 Medical Research The Villages
Lady Lake, Florida, United States
Verus Clinical research Corp
Miami, Florida, United States
BioMed Research Institute, Inc.
Miami, Florida, United States
CCM Clinical Research Group, LLC
Miami, Florida, United States
Advance Medical Research Center
Miami, Florida, United States
Allied Biomedical Research Institute (Clinical Trials)
Miami, Florida, United States
Vitae Research Center LLC.
Miami, Florida, United States
Stein Gerontological Institute, Inc.
Miami, Florida, United States
Miami Dade Medical Research Institute
Miami, Florida, United States
K2 Medical Research Winter Garden
Ocoee, Florida, United States
Interspond, LLC,
Orlando, Florida, United States
The University of South Florida Board of Trustees,
Tampa, Florida, United States
Alzheimer's Research and Treatment Center
Wellington, Florida, United States
Velocity Clinical Research, Inc
Meridian, Idaho, United States
Ocean Medical Research
Jersey City, New Jersey, United States
Advanced Memory Research Institute of New Jersey
Toms River, New Jersey, United States
Integrative Clinical Trials LLC
Brooklyn, New York, United States
New York University School of Medicine
New York, New York, United States
AMC Research, LLC
Matthews, North Carolina, United States
Rhode Island mood and memory research institute
Island Park, Rhode Island, United States
Neurology Clinic, P.C.
Cordova, Tennessee, United States
Northwest Clinical Research Center
Bellevue, Washington, United States
Froedtert & Medical College of Wisconsin
Milwaukee, Wisconsin, United States
Centricity Research Halifax Multispecialty
Nova Scotia, Halifax, Canada
Bluewater Clinical Research Group Inc
Sarnia, Ontario, Canada
LMC Clinical Research Inc. d.b.a. Centricity Research
Toronto, Ontario, Canada
OCT Research ULC (dba Okanagan Clinical Trials)
Kelowna, , Canada
Medical Arts Health Research Group
Vancouver, , Canada
Countries
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Related Links
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A Polymorphism Cluster at the 2q12 locus May Predict Response to Piromelatine in Patients with Mild Alzheimer's Disease
Other Identifiers
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NEUP11-7
Identifier Type: -
Identifier Source: org_study_id
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