Study to Evaluate the Efficacy and Safety of KDS2010 in Patients With Alzheimer's Disease With Mild Cognitive Impairment and Mild Dementia Due to Alzheimer's Disease
NCT ID: NCT07027072
Last Updated: 2025-08-08
Study Results
Results pending
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
Get a concise snapshot of the trial, including recruitment status, study phase, enrollment targets, and key timeline milestones.
Recruitment Status
RECRUITING
Clinical Phase
PHASE2
Total Enrollment
114 participants
Study Classification
INTERVENTIONAL
Study Start Date
2025-08-06
Study Completion Date
2027-12-31
Brief Summary
Review the sponsor-provided synopsis that highlights what the study is about and why it is being conducted.
A randomized, double-blind, placebo-controlled, dose-finding Phase 2a clinical trial will be conducted to evaluate the efficacy and safety of KDS2010 in patients with Mild Cognitive Impairment (MCI) due to Alzheimer's disease (AD) and mild dementia due to Alzheimer's disease.
Based on preliminary efficacy observed in the Phase 1 clinical trial, a multinational study will be conducted in both Korea and the United States. Eligible patients diagnosed with MCI or mild Alzheimer's disease will be stratified by disease stage (MCI/mild AD) and geographic region (Korea/USA) prior to randomization. Subjects will be randomly assigned in a 1:1:1 ratio to either Treatment Group 1, Treatment Group 2, or the Control Group. The investigational product will be administered orally once daily for a duration of 24 weeks. Approximately 114 subjects will be enrolled, including an estimated 20% dropout rate, with 38 subjects assigned to each group (Treatment Group 1, Treatment Group 2, and Control Group).
The objectives of the study are as follows:
1. Efficacy Objectives: Efficacy will be evaluated through changes in cognitive function, self-management, and daily living activities before and after administration of KDS2010. Biomarker analysis in plasma and in cerebrospinal fluid (CSF; optional) will also be conducted to explore treatment efficacy.
2. Safety Objectives: The safety and tolerability will be evaluated after administration of KDS2010.
3. Exploratory Objectives: The efficacy of Treatment Groups 1 and 2 compared to the Control group will be explored through cognitive endpoints (the Clinical Dementia Rating-Sum of Boxes (CDR-SB), the Alzheimer's Disease Assessment Scale-Cognitive Subscale (ADAS-Cog13), and the Mini-Mental State Examination (MMSE)), stratified by demographic information, tauopathy, and ApoE4 genes.
Based on nonclinical and Phase 1 clinical data, KDS2010 will be administered orally once daily at two dose levels: 60 mg and 120 mg.
Based on preliminary efficacy observed in the Phase 1 clinical trial, a multinational study will be conducted in both Korea and the United States. Eligible patients diagnosed with MCI or mild Alzheimer's disease will be stratified by disease stage (MCI/mild AD) and geographic region (Korea/USA) prior to randomization. Subjects will be randomly assigned in a 1:1:1 ratio to either Treatment Group 1, Treatment Group 2, or the Control Group. The investigational product will be administered orally once daily for a duration of 24 weeks. Approximately 114 subjects will be enrolled, including an estimated 20% dropout rate, with 38 subjects assigned to each group (Treatment Group 1, Treatment Group 2, and Control Group).
The objectives of the study are as follows:
1. Efficacy Objectives: Efficacy will be evaluated through changes in cognitive function, self-management, and daily living activities before and after administration of KDS2010. Biomarker analysis in plasma and in cerebrospinal fluid (CSF; optional) will also be conducted to explore treatment efficacy.
2. Safety Objectives: The safety and tolerability will be evaluated after administration of KDS2010.
3. Exploratory Objectives: The efficacy of Treatment Groups 1 and 2 compared to the Control group will be explored through cognitive endpoints (the Clinical Dementia Rating-Sum of Boxes (CDR-SB), the Alzheimer's Disease Assessment Scale-Cognitive Subscale (ADAS-Cog13), and the Mini-Mental State Examination (MMSE)), stratified by demographic information, tauopathy, and ApoE4 genes.
Based on nonclinical and Phase 1 clinical data, KDS2010 will be administered orally once daily at two dose levels: 60 mg and 120 mg.
Related Clinical Trials
Explore similar clinical trials based on study characteristics and research focus.
Safety and Efficacy of Donepezil HCl 23 mg in Patients With Moderate to Severe Alzheimer's Disease
NCT02097056
Alzheimer's Disease
COMPLETED
PHASE4
A Study of CST-2032 and CST-107 in Subjects With Mild Cognitive Impairment or Mild Dementia Due to Parkinson's or Alzheimer's Disease
NCT05104463
Mild Cognitive Impairment
Dementia
COMPLETED
PHASE2
Evaluate the Efficacy and Safety of ID1201 for Dose-finding in Mild Alzheimer's Disease
NCT03363269
Alzheimer Disease
COMPLETED
PHASE2
A Study of NH280105 in Healthy Adult Participants
NCT06870058
Alzheimer Disease
COMPLETED
PHASE1
A Phase 2 Clinical Study to Explore the Optimal Dosage/Administration of PM012 Tablet in Alzheimer's Disease
NCT05811000
Mild Alzheimer Disease
UNKNOWN
PHASE2/PHASE3
Detailed Description
Dive into the extended narrative that explains the scientific background, objectives, and procedures in greater depth.
This Phase 2a, multinational, randomized, double-blind, placebo-controlled, dose-finding clinical trial is designed to evaluate the efficacy, safety, and pharmacokinetics of KDS2010, a novel investigational product, reversible monoamine oxidase-B (MAO-B) inhibitor, in patients with Alzheimer's Disease (AD) with Mild Cognitive Impairment (MCI) and Mild Dementia due to Alzheimer's Disease. The clinical trial is conducted at selected sites in Korea and the United States.
A total of 114 subjects are planned for the study, with 38 subjects in each of the three groups: two treatment groups (receiving different doses of KDS2010) and a placebo control group. Subjects will be randomized in a 1:1:1 ratio, and the study is designed to allow for a 20% dropout rate. Inclusion criteria require that participants be aged between 50 and 85 years, diagnosed with MCI or mild AD, and amyloid-positive as confirmed by PET scans. Eligible participants must also demonstrate cognitive impairment as indicated by a CDR score between 0.5 and 1.0 and an MMSE score between 21 and 30.
Key exclusion criteria include individuals with cognitive impairment caused by conditions other than AD, those with a history of serious medical conditions such as cardiovascular disease or cancer, and individuals who have used AD-modifying agents or CNS-active drugs within 12 weeks prior to screening.
The primary efficacy endpoint is the change in cognitive function, assessed through the Clinical Dementia Rating-Sum of Boxes (CDR-SB), Mini-Mental State Examination (MMSE), and Alzheimer's Disease Assessment Scale-Cognitive 13 (ADAS-Cog13) scores. Secondary efficacy endpoints include changes in daily living activities (measured by the Activities of Daily Living Scale and the Alzheimer's Disease IADL Questionnaire), as well as biomarkers such as tauopathy and Apo-E4. Exploratory endpoints will assess cognitive decline and specific changes in brain imaging (e.g., PET scans) and cerebrospinal fluid biomarkers.
Safety will be evaluated through monitoring adverse events (AEs), vital signs, laboratory tests, ECGs, and psychological assessments, including the Columbia-Suicide Severity Rating Scale (C-SSRS). Pharmacokinetic parameters (AUCtau, Cmax,ss, Cmin,ss, Cav,ss, Tmax,ss, T1/2, and PTF, etc.) will be measured to assess systemic exposure to KDS2010.
Subjects must be aged between 50 and 85 years, diagnosed with MCI or mild AD, and amyloid-positive based on PET scan results. Inclusion criteria also require cognitive impairment as indicated by a CDR score between 0.5 and 1.0 and an MMSE score between 21 and 30. Major exclusion criteria include conditions other than AD that cause cognitive impairment, uncontrolled systemic diseases, and recent use of AD-modifying agents.
The primary aim of the study is to determine the potential of KDS2010 to slow cognitive decline in individuals with early-stage Alzheimer's disease, with secondary and exploratory objectives focused on safety, quality of life, and understanding the drug's pharmacokinetic profile. This study aims to provide important insights into the potential therapeutic benefits of KDS2010 in treating Alzheimer's disease at the early stages of cognitive decline.
The total duration of the study is expected to be approximately 30 months from IRB/IEC approval, with individual subject participation lasting up to 9 months. This trial aims to evaluate the safety, efficacy, and pharmacokinetics of KDS2010 as a potential treatment for early stages of Alzheimer's disease, with the goal of advancing the development of KDS2010 in the treatment of AD.
A total of 114 subjects are planned for the study, with 38 subjects in each of the three groups: two treatment groups (receiving different doses of KDS2010) and a placebo control group. Subjects will be randomized in a 1:1:1 ratio, and the study is designed to allow for a 20% dropout rate. Inclusion criteria require that participants be aged between 50 and 85 years, diagnosed with MCI or mild AD, and amyloid-positive as confirmed by PET scans. Eligible participants must also demonstrate cognitive impairment as indicated by a CDR score between 0.5 and 1.0 and an MMSE score between 21 and 30.
Key exclusion criteria include individuals with cognitive impairment caused by conditions other than AD, those with a history of serious medical conditions such as cardiovascular disease or cancer, and individuals who have used AD-modifying agents or CNS-active drugs within 12 weeks prior to screening.
The primary efficacy endpoint is the change in cognitive function, assessed through the Clinical Dementia Rating-Sum of Boxes (CDR-SB), Mini-Mental State Examination (MMSE), and Alzheimer's Disease Assessment Scale-Cognitive 13 (ADAS-Cog13) scores. Secondary efficacy endpoints include changes in daily living activities (measured by the Activities of Daily Living Scale and the Alzheimer's Disease IADL Questionnaire), as well as biomarkers such as tauopathy and Apo-E4. Exploratory endpoints will assess cognitive decline and specific changes in brain imaging (e.g., PET scans) and cerebrospinal fluid biomarkers.
Safety will be evaluated through monitoring adverse events (AEs), vital signs, laboratory tests, ECGs, and psychological assessments, including the Columbia-Suicide Severity Rating Scale (C-SSRS). Pharmacokinetic parameters (AUCtau, Cmax,ss, Cmin,ss, Cav,ss, Tmax,ss, T1/2, and PTF, etc.) will be measured to assess systemic exposure to KDS2010.
Subjects must be aged between 50 and 85 years, diagnosed with MCI or mild AD, and amyloid-positive based on PET scan results. Inclusion criteria also require cognitive impairment as indicated by a CDR score between 0.5 and 1.0 and an MMSE score between 21 and 30. Major exclusion criteria include conditions other than AD that cause cognitive impairment, uncontrolled systemic diseases, and recent use of AD-modifying agents.
The primary aim of the study is to determine the potential of KDS2010 to slow cognitive decline in individuals with early-stage Alzheimer's disease, with secondary and exploratory objectives focused on safety, quality of life, and understanding the drug's pharmacokinetic profile. This study aims to provide important insights into the potential therapeutic benefits of KDS2010 in treating Alzheimer's disease at the early stages of cognitive decline.
The total duration of the study is expected to be approximately 30 months from IRB/IEC approval, with individual subject participation lasting up to 9 months. This trial aims to evaluate the safety, efficacy, and pharmacokinetics of KDS2010 as a potential treatment for early stages of Alzheimer's disease, with the goal of advancing the development of KDS2010 in the treatment of AD.
Conditions
See the medical conditions and disease areas that this research is targeting or investigating.
Mild Cognitive Impairment (MCI)
Mild Dementia
Alzheimer's Disease
Study Design
Understand how the trial is structured, including allocation methods, masking strategies, primary purpose, and other design elements.
Allocation Method
RANDOMIZED
Intervention Model
PARALLEL
Randomized, Double-Blind, Placebo-Controlled, Dose-Finding, Phase 2a Clinical Trial
Primary Study Purpose
TREATMENT
Blinding Strategy
QUADRUPLE
Participants
Caregivers
Investigators
Outcome Assessors
A double-blind design is used to ensure scientific validity. Subjects and investigators are unaware of treatment allocation, with identical appearance between the drug and placebo. Randomization numbers are used for subject identification, and group assignments are disclosed only after the end of treatment.
Study Groups
Review each arm or cohort in the study, along with the interventions and objectives associated with them.
Control Group_Placebo
A placebo will be administered orally once daily as two tablets per day for 24 weeks. This group will match the investigational drug in appearance but contain no active ingredients to maintain blinding.
Group Type
PLACEBO_COMPARATOR
Placebo
Intervention Type
DRUG
Placebo matching the investigational product in appearance but containing no active ingredient, administered orally once daily, two tablets per day, for 24 weeks.
Treatment Group 1_KDS2010 60 mg
KDS2010 60 mg will be administered orally once daily as two tablets per day (one 60 mg KDS2010 tablet and one placebo tablet, 60 mg total) for 24 weeks. This group will receive the active investigational drug to evaluate its safety and efficacy.
Group Type
EXPERIMENTAL
KDS2010
Intervention Type
DRUG
KDS2010 will be administered orally once daily, two tablets per day, for 24 weeks. Dosage will be either 60 mg or 120 mg depending on the assigned group.
Treatment Group 2_KDS2010 120 mg
KDS2010 60 mg will be administered orally once daily as two tablets per day (two 60 mg KDS2010 tablets, 120 mg total) for 24 weeks. This group will receive the higher dose of the investigational drug to evaluate its safety and efficacy.
Group Type
EXPERIMENTAL
KDS2010
Intervention Type
DRUG
KDS2010 will be administered orally once daily, two tablets per day, for 24 weeks. Dosage will be either 60 mg or 120 mg depending on the assigned group.
Interventions
Learn about the drugs, procedures, or behavioral strategies being tested and how they are applied within this trial.
KDS2010
KDS2010 will be administered orally once daily, two tablets per day, for 24 weeks. Dosage will be either 60 mg or 120 mg depending on the assigned group.
Intervention Type
DRUG
Placebo
Placebo matching the investigational product in appearance but containing no active ingredient, administered orally once daily, two tablets per day, for 24 weeks.
Intervention Type
DRUG
Eligibility Criteria
Check the participation requirements, including inclusion and exclusion rules, age limits, and whether healthy volunteers are accepted.
Inclusion Criteria
* Male and female adults aged ≥50 and ≤85 years at the time of written consent
* Patients with MCI or mild AD confirmed at screening according to the 2024 diagnostic criteria (APPENDIX 1) of the National Institute on Aging-Alzheimer's Association (NIA-AA)
* Subjects whose total CDR score (CDR-GS) is 0.5 to 1.0 at screening (however, CDR memory score is ≥0.5)
* Subjects with a Mini-Mental State Examination (MMSE) score of 21 to 30 at screening
* Subjects who test positive for amyloid on Positron Emission Tomography (PET) during screening
* Subjects who have a caregiver capable of providing accurate information about the subject's cognitive and functional abilities and appropriate for the planned assessments in the study, as judged by the investigator
* Subjects (or their legal representatives) who have voluntarily agreed to participate in this study and have given written consent
* Patients with MCI or mild AD confirmed at screening according to the 2024 diagnostic criteria (APPENDIX 1) of the National Institute on Aging-Alzheimer's Association (NIA-AA)
* Subjects whose total CDR score (CDR-GS) is 0.5 to 1.0 at screening (however, CDR memory score is ≥0.5)
* Subjects with a Mini-Mental State Examination (MMSE) score of 21 to 30 at screening
* Subjects who test positive for amyloid on Positron Emission Tomography (PET) during screening
* Subjects who have a caregiver capable of providing accurate information about the subject's cognitive and functional abilities and appropriate for the planned assessments in the study, as judged by the investigator
* Subjects (or their legal representatives) who have voluntarily agreed to participate in this study and have given written consent
Exclusion Criteria
* Cognitive impairment or dementia due to causes other than Alzheimer's disease
* Vascular dementia, central nervous system infections (e.g., HIV, syphilis, etc.), head trauma, Creutzfeldt-Jakob disease, Pick's disease, Huntington's disease, Parkinson's disease, subdural hematoma, normal pressure hydrocephalus, brain tumor, thyroid disorders, parathyroid disorders, Vitamin B12 deficiency, folic acid deficiency, other metabolic and nutritional deficiencies, etc.
* Alcohol or drug abuse, dependence
* Subjects with cognitive impairment due to hypothyroidism, nutritional deficiencies, Vitamin B12 or folic acid deficiency as assessed during screening
* Subjects confirmed during screening to have had the following medical history:
* Malignant tumors within five years prior to screening except for basal cell carcinoma, cutaneous squamous cell carcinoma, thyroid cancer, or carcinoma in situ that has not recurred in over three years and is considered successfully treated by the investigator
* History of alcohol or drug abuse within two years prior to screening
* Loss of consciousness of unknown cause, or seizure within the past 52 weeks before screening
* Unstable and clinically significant cardiovascular diseases despite appropriate treatment (acute coronary syndrome (ACS), tachycardia, clinically significant arrhythmias, cardiomyopathy, angina of at least CSS III, heart failure of NYHA II-IV, or clinically significant valvular heart disease) within 24 weeks before baseline
* Severe or active infectious diseases requiring antibiotics or antivirals within four weeks before baseline
* A history of stroke involving a major vascular area, transient ischemic attack (TIA), epilepsy, or severe head trauma with loss of consciousness
* Hypersensitivity or allergy to any components of the investigational product
* Subjects confirmed during screening to have had the following accompanying disease:
* Clinically significant neurological diseases or serious pathological findings affecting cognitive function as confirmed by brain imaging studies within 52 weeks prior to screening, including multiple sclerosis, normal pressure hydrocephalus, brain tumor (however, exceptions are allowed for lesions diagnosed as benign and with a maximum diameter of less than 1 cm), spinal cord infarction, major hemorrhage (defined as having a diameter \> 1 cm in MRI) or subdural hemorrhage, cerebral vascular malformation, communicating hydrocephalus, inflammatory demyelinating diseases, etc.
* Uncontrolled hypertension despite appropriate treatment at screening or baseline (SBP ≥160 mmHg or DBP ≥100 mmHg)
* Dizziness or fainting when standing due to orthostatic hypotension that may affect the evaluation according to the judgment of the investigator
* Uncontrolled diabetes (HbA1c \> 9%) during screening, despite appropriate treatment
* Bleeding disorders (Platelet \<50,000/mm³) during screening, despite appropriate treatment
* Patients with severe hepatic impairment (Child-pugh class C) at screening
* Following laboratory test values at screening:
* AST or ALT \> 2.5 x ULN
* total bilirubin \> 1.5 x ULN (however, in case of Gilbert syndrome, \> 3.0 mg/dL)
* MDRD eGFR \< 30 mL/min/1.73 m²
* QTcF interval \>450 msecs (12-lead ECG) during screening
* Gastrointestinal diseases that may affect oral administration or absorption (celiac disease, Crohn's disease, intestinal resection, etc.)
* Gastrointestinal diseases, including gastric and duodenal ulcers, that may affect the safety evaluation according to the judgment of the investigator
* Psychiatric diagnosis or symptoms that may interfere with the study (uncontrolled major depression, uncontrolled schizophrenia, uncontrolled bipolar affective disorder, etc.), as assessed by the investigator
* Positive responses to items 4 or 5 on the Columbia University Suicide Severity Rating Scale (C-SSRS) during screening
* Other conditions deemed by the investigator to potentially affect the outcome of the study
* Subjects who have undergone or require treatment with the following:
* AD disease-modifying agents (aducanumab, lecanemab, donanemab, gantenerumab, solanezumab, blarcamesine, simufilam, tricaprilin, valiltramiprosate, etc.) within 12 weeks before screening
* Medications that may improve cognitive abilities or affect AD treatment (AChEIs, donepezil, galantamine, rivastigmine, tacrine, memantine, etc.) within 12 weeks before screening, except if the subject has been on a stable dose for at least 12 weeks before baseline and maintains the same composition/dosage/method of administration during the study period
* CNS-active drugs or those affecting cognitive function antidepressants other than serotonergic drugs \[e.g., bupropion\], sedatives \[e.g., carbamazepine\], dopamine antagonists \[e.g., antipsychotics, metoclopramide\], amfepramone, mazindol) within 12 weeks before screening
* Central anticholinergics and sedating H1-antihistamines within 12 weeks before screening.
However, exceptions are allowed for one-time use of the drugs, such as second-generation H1 antihistamines (e.g., cetirizine, levocetirizine, etc.) or peripheral anticholinergics with no central action (e.g., trospium for treating overactive bladder). But the use is prohibited for at least 3 days from the date of cognitive function evaluation.
* Other investigational products or clinical trial devices within four weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* Monoamine oxidase inhibitors (MAOIs) and linezolid within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* Opioids (pethidine, tramadol, tapentadol, etc.) within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* Cyclobenzaprine and St. John's wort within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* The following serotonergic drugs within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out),
* selective serotonin (5HT1) agonists
* lithium
* lamotrigine
* ritonavir
* dapoxetine
* Selective serotonin reuptake inhibitors (SSRIs)
* dapoxetine
* Serotonin-norepinephrine reuptake inhibitors (SNRIs)
* Tricyclic or tetracyclic antidepressants
* triazolopyridine antidepressant However, amitriptyline ≤ 50 mg/day, trazodone ≤ 100 mg/day, citalopram ≤ 20 mg/day, and sertraline ≤ 100 mg/day are allowed without washout.
* Use of sympathomimetics (ephedrine, methylphenidate, amphetamine, methamphetamine, lisdexamfetamine, etc.) during the screening period
* Use of Dextromethorphan during the screening period
* Use of CYP3A4 strong inducer, CYP3A4 strong inhibitor, CYP2D6 strong inducer, and CYP2D6 strong inhibitor during the screening period
* Inability to undergo MRI or PET scans
* Pregnant or breastfeeding women
* Fertile women or men who are unwilling to use effective contraception\* from the date of written consent until 12 weeks after the last administration of the investigational product
\*Effective contraception is defined as follows, and at least one method should be used:
* Hormonal contraception (oral, injectable, implantable, etc.)
* Intrauterine device (IUD) or system (IUS)
* Sterilization or surgical procedures (vasectomy, bilateral tubal ligation/surgery, hysterectomy)
* Dual contraception methods: Simultaneous use of barrier methods (male condoms) with the methods listed above
* Absolute abstinence: Total abstinence from sexual intercourse is recognized if the investigator deems the subject's age, occupation, lifestyle, or sexual orientation assures contraception. However, periodic abstinence (calendar method, mucus method, and symptothermal method), withdrawal, and coitus interruptus are not recognized as effective contraception methods.
* Other conditions deemed by the investigator to be unsuitable for participation in the study
* Vascular dementia, central nervous system infections (e.g., HIV, syphilis, etc.), head trauma, Creutzfeldt-Jakob disease, Pick's disease, Huntington's disease, Parkinson's disease, subdural hematoma, normal pressure hydrocephalus, brain tumor, thyroid disorders, parathyroid disorders, Vitamin B12 deficiency, folic acid deficiency, other metabolic and nutritional deficiencies, etc.
* Alcohol or drug abuse, dependence
* Subjects with cognitive impairment due to hypothyroidism, nutritional deficiencies, Vitamin B12 or folic acid deficiency as assessed during screening
* Subjects confirmed during screening to have had the following medical history:
* Malignant tumors within five years prior to screening except for basal cell carcinoma, cutaneous squamous cell carcinoma, thyroid cancer, or carcinoma in situ that has not recurred in over three years and is considered successfully treated by the investigator
* History of alcohol or drug abuse within two years prior to screening
* Loss of consciousness of unknown cause, or seizure within the past 52 weeks before screening
* Unstable and clinically significant cardiovascular diseases despite appropriate treatment (acute coronary syndrome (ACS), tachycardia, clinically significant arrhythmias, cardiomyopathy, angina of at least CSS III, heart failure of NYHA II-IV, or clinically significant valvular heart disease) within 24 weeks before baseline
* Severe or active infectious diseases requiring antibiotics or antivirals within four weeks before baseline
* A history of stroke involving a major vascular area, transient ischemic attack (TIA), epilepsy, or severe head trauma with loss of consciousness
* Hypersensitivity or allergy to any components of the investigational product
* Subjects confirmed during screening to have had the following accompanying disease:
* Clinically significant neurological diseases or serious pathological findings affecting cognitive function as confirmed by brain imaging studies within 52 weeks prior to screening, including multiple sclerosis, normal pressure hydrocephalus, brain tumor (however, exceptions are allowed for lesions diagnosed as benign and with a maximum diameter of less than 1 cm), spinal cord infarction, major hemorrhage (defined as having a diameter \> 1 cm in MRI) or subdural hemorrhage, cerebral vascular malformation, communicating hydrocephalus, inflammatory demyelinating diseases, etc.
* Uncontrolled hypertension despite appropriate treatment at screening or baseline (SBP ≥160 mmHg or DBP ≥100 mmHg)
* Dizziness or fainting when standing due to orthostatic hypotension that may affect the evaluation according to the judgment of the investigator
* Uncontrolled diabetes (HbA1c \> 9%) during screening, despite appropriate treatment
* Bleeding disorders (Platelet \<50,000/mm³) during screening, despite appropriate treatment
* Patients with severe hepatic impairment (Child-pugh class C) at screening
* Following laboratory test values at screening:
* AST or ALT \> 2.5 x ULN
* total bilirubin \> 1.5 x ULN (however, in case of Gilbert syndrome, \> 3.0 mg/dL)
* MDRD eGFR \< 30 mL/min/1.73 m²
* QTcF interval \>450 msecs (12-lead ECG) during screening
* Gastrointestinal diseases that may affect oral administration or absorption (celiac disease, Crohn's disease, intestinal resection, etc.)
* Gastrointestinal diseases, including gastric and duodenal ulcers, that may affect the safety evaluation according to the judgment of the investigator
* Psychiatric diagnosis or symptoms that may interfere with the study (uncontrolled major depression, uncontrolled schizophrenia, uncontrolled bipolar affective disorder, etc.), as assessed by the investigator
* Positive responses to items 4 or 5 on the Columbia University Suicide Severity Rating Scale (C-SSRS) during screening
* Other conditions deemed by the investigator to potentially affect the outcome of the study
* Subjects who have undergone or require treatment with the following:
* AD disease-modifying agents (aducanumab, lecanemab, donanemab, gantenerumab, solanezumab, blarcamesine, simufilam, tricaprilin, valiltramiprosate, etc.) within 12 weeks before screening
* Medications that may improve cognitive abilities or affect AD treatment (AChEIs, donepezil, galantamine, rivastigmine, tacrine, memantine, etc.) within 12 weeks before screening, except if the subject has been on a stable dose for at least 12 weeks before baseline and maintains the same composition/dosage/method of administration during the study period
* CNS-active drugs or those affecting cognitive function antidepressants other than serotonergic drugs \[e.g., bupropion\], sedatives \[e.g., carbamazepine\], dopamine antagonists \[e.g., antipsychotics, metoclopramide\], amfepramone, mazindol) within 12 weeks before screening
* Central anticholinergics and sedating H1-antihistamines within 12 weeks before screening.
However, exceptions are allowed for one-time use of the drugs, such as second-generation H1 antihistamines (e.g., cetirizine, levocetirizine, etc.) or peripheral anticholinergics with no central action (e.g., trospium for treating overactive bladder). But the use is prohibited for at least 3 days from the date of cognitive function evaluation.
* Other investigational products or clinical trial devices within four weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* Monoamine oxidase inhibitors (MAOIs) and linezolid within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* Opioids (pethidine, tramadol, tapentadol, etc.) within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* Cyclobenzaprine and St. John's wort within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out)
* The following serotonergic drugs within two weeks before baseline or five times the half-life of the drug (whichever is longer, and patients can be enrolled after wash-out),
* selective serotonin (5HT1) agonists
* lithium
* lamotrigine
* ritonavir
* dapoxetine
* Selective serotonin reuptake inhibitors (SSRIs)
* dapoxetine
* Serotonin-norepinephrine reuptake inhibitors (SNRIs)
* Tricyclic or tetracyclic antidepressants
* triazolopyridine antidepressant However, amitriptyline ≤ 50 mg/day, trazodone ≤ 100 mg/day, citalopram ≤ 20 mg/day, and sertraline ≤ 100 mg/day are allowed without washout.
* Use of sympathomimetics (ephedrine, methylphenidate, amphetamine, methamphetamine, lisdexamfetamine, etc.) during the screening period
* Use of Dextromethorphan during the screening period
* Use of CYP3A4 strong inducer, CYP3A4 strong inhibitor, CYP2D6 strong inducer, and CYP2D6 strong inhibitor during the screening period
* Inability to undergo MRI or PET scans
* Pregnant or breastfeeding women
* Fertile women or men who are unwilling to use effective contraception\* from the date of written consent until 12 weeks after the last administration of the investigational product
\*Effective contraception is defined as follows, and at least one method should be used:
* Hormonal contraception (oral, injectable, implantable, etc.)
* Intrauterine device (IUD) or system (IUS)
* Sterilization or surgical procedures (vasectomy, bilateral tubal ligation/surgery, hysterectomy)
* Dual contraception methods: Simultaneous use of barrier methods (male condoms) with the methods listed above
* Absolute abstinence: Total abstinence from sexual intercourse is recognized if the investigator deems the subject's age, occupation, lifestyle, or sexual orientation assures contraception. However, periodic abstinence (calendar method, mucus method, and symptothermal method), withdrawal, and coitus interruptus are not recognized as effective contraception methods.
* Other conditions deemed by the investigator to be unsuitable for participation in the study
Minimum Eligible Age
50 Years
Maximum Eligible Age
85 Years
Eligible Sex
ALL
Accepts Healthy Volunteers
No
Sponsors
Meet the organizations funding or collaborating on the study and learn about their roles.
NeuroBiogen Co., Ltd
INDUSTRY
Sponsor Role
lead
Responsible Party
Identify the individual or organization who holds primary responsibility for the study information submitted to regulators.
Responsibility Role
SPONSOR
Principal Investigators
Learn about the lead researchers overseeing the trial and their institutional affiliations.
Sangwook Kim, Chief Executive Officer
Role: STUDY_DIRECTOR
NeuroBiogen Co., Ltd
Locations
Explore where the study is taking place and check the recruitment status at each participating site.
Chonnam National Unversity Hospital
Gwangju, Gwangju, South Korea
Site Status
RECRUITING
Hanyang University Guri Hospital
Guri-si, Gyeonggi-do, South Korea
Site Status
RECRUITING
The Catholic University of Korea St. Vincent's Hospital
Suwon, Gyeonggi-do, South Korea
Site Status
RECRUITING
Ajou University Hospital
Suwon, Gyeonggi-do, South Korea
Site Status
RECRUITING
Gachon University Gil Medical Center
Incheon, Incheon, South Korea
Site Status
RECRUITING
Hanyang University Seoul Hospital
Seoul, Seoul, South Korea
Site Status
RECRUITING
Konkuk University Medical Center
Seoul, Seoul, South Korea
Site Status
RECRUITING
Asan Medical Center
Seoul, Seoul, South Korea
Site Status
RECRUITING
Countries
Review the countries where the study has at least one active or historical site.
South Korea
Central Contacts
Reach out to these primary contacts for questions about participation or study logistics.
Dayoung Kim, Professor
Role: CONTACT
Facility Contacts
Find local site contact details for specific facilities participating in the trial.
Younghye Cho, CRC
Role: backup
Jinah Kang, CRC
Role: backup
Sunmin Lee, Professor
Role: backup
Hyunju Kim, CRC
Role: backup
Kyunghoe Choi, CRC
Role: backup
Dayoung Kim, Professor
Role: backup
Jaewoo Kim, Professor
Role: backup
Other Identifiers
Review additional registry numbers or institutional identifiers associated with this trial.
KCT0010589
Identifier Type: REGISTRY
Identifier Source: secondary_id
NB_KDS_ADP2_23
Identifier Type: -
Identifier Source: org_study_id
More Related Trials
Additional clinical trials that may be relevant based on similarity analysis.
Efficacy and Safety of GSK4527226 [AL101] in Participants With Early Alzheimer's Disease
NCT06079190
ACTIVE_NOT_RECRUITING
PHASE2
Study of the Effect of SR57667B in Patients With Alzheimer's Disease
NCT00285025
COMPLETED
PHASE2
Clinical Trial of Donepezil Between the Patients With Alzheimer's Disease and Mixed Dementia
NCT01023867
COMPLETED
NA
Efficacy and Safety of T-817MA in Patients With Mild to Moderate Alzheimer's Disease (US202)
NCT02079909
COMPLETED
PHASE2
A Phase 3 Study of NE3107 in Probable Alzheimer's Disease
NCT04669028
COMPLETED
PHASE3
Cognitive Changes in Alzheimer's Disease Patients Associated With or Without White Matter Changes After Rivastigmine
NCT01380288
COMPLETED
NA
Study of Octohydroaminoacridine Succinate Tablets in Patients With Alzheimer's Disease
NCT01569516
UNKNOWN
PHASE2
Evaluate the Safety and Efficacy of AD-35 Tablet in Subjects With Mild to Moderate Alzheimer's Disease
NCT03790982
UNKNOWN
PHASE2
GV1001 Subcutaneous for the Treatment of Moderate to Severe Alzheimer's Disease(AD)
NCT05303701
NOT_YET_RECRUITING
PHASE3
A Trial of SK-PC-B70M in Mild to Moderate Alzheimer's Disease
NCT00443417
COMPLETED
PHASE2
A Study of Donepezil Hydrochloride in Patients With Dementia Associated With Cerebrovascular Disease
NCT02660983
COMPLETED
PHASE4
Safety and Pharmacodynamics of SHR-1707 in Alzheimer's Disease Patients
NCT06199037
RECRUITING
PHASE2
Safety, Tolerability and Pharmacokinetics of DKF-310 ( (Donepezil).
NCT02695004
COMPLETED
PHASE1
Study of DHP1401 in Patients With Mild-moderate Alzheimer's Disease Treated With Donepezil(DRAMA)
NCT03055741
COMPLETED
PHASE2
BPDO-1603 Intervention Trial in Patients With Moderate-to-severe Alzheimer's Disease
NCT04229927
UNKNOWN
PHASE3
A Confirmatory Trial of SK-PC-B70M in Mild to Moderate Alzheimer's Disease
NCT01249196
COMPLETED
PHASE3
A Study of the Safety, Tolerability, and Pharmacodynamics of MK-8931 in Participants With Alzheimer's Disease (MK-8931-010 AM1 [P07820 AM1])
NCT01496170
COMPLETED
PHASE1
Dose-Finding Study To Evaluate Safety, Tolerability, and Efficacy of E2609 in Participants With Mild Cognitive Impairment Due to Alzheimer's Disease (Prodromal Alzheimer's Disease) and Mild to Moderate Dementia Due to Alzheimer's Disease
NCT02322021
TERMINATED
PHASE2
Clinical Trial to Evaluate the Efficacy and Safety of GV1001 in Alzheimer Patients
NCT03184467
COMPLETED
PHASE2
Clinical Trial of CT1812 in Mild to Moderate Alzheimer's Disease
NCT02907567
COMPLETED
PHASE1/PHASE2
Evaluation of the Safety and Potential Therapeutic Effects of CB-AC-02 in Patients With Alzheimer's Disease
NCT02899091
ACTIVE_NOT_RECRUITING
PHASE1/PHASE2
A Study of Single and Multiple Doses of KHK6640 in Subjects With Prodromal or Mild to Moderate Alzheimer's Disease
NCT02127476
COMPLETED
PHASE1
A Phase 2 Study Evaluating The Efficacy And Safety Of PF 04494700 In Mild To Moderate Alzheimer's Disease
NCT00566397
COMPLETED
PHASE2
Safety, Tolerability and Pharmacodynamics of SHR-1707 in Alzheimer's Disease Patients.
NCT05681819
COMPLETED
PHASE1