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Search / Trial NCT06957418

Alzheimer's Tau Platform: Master Protocol

Launched by UNIVERSITY OF SOUTHERN CALIFORNIA · Apr 25, 2025

Trial Information

Current as of June 02, 2025

Not yet recruiting

Keywords

Alzheimer's Disease Preclinical Alzheimer's Prodromal Alzheimer's Mild Cognitive Impairment (Mci) Neurodegeneration Dementia Tau Directed Therapy Donanemab Monoclonal Antibody Anti Tau Therapy Combination Therapy Immunotherapy

ClinConnect Summary

The Alzheimer's Tau Platform (ATP) trial is a research study aimed at finding out if new treatments targeting tau proteins can help slow the progression of Alzheimer's disease. It specifically looks at adults aged 50 to 80 who are in the early stages of Alzheimer's or are at risk for it. The trial will test different tau therapies alone or in combination with a medication called donanemab to see if they can reduce tau buildup in the brain and slow down cognitive decline.

If you or someone you know is interested in participating, you must be between 50 and 80 years old and have certain cognitive test scores that indicate early Alzheimer's or no cognitive impairment at all. Participants will be randomly assigned to one of several treatment groups, which may include taking donanemab or a placebo (a non-active treatment) for six months, followed by up to two years of tau therapy. Throughout the study, participants will undergo regular brain scans and cognitive tests to monitor their progress. It’s important to note that this trial is not yet recruiting participants, but it will be an ongoing study that adds new treatment options as they become available.

Gender

ALL

Eligibility criteria

  • Inclusion Criteria:
  • 1. Documentation of the participant's informed consent to study procedures (including APOE genotyping).
  • 2. Ages 50-80 years (inclusive). Participants between the ages of 50 and 60 (inclusive) must be cognitively impaired at screening (global CDR=0.5 and maximum CDR-SB \<1.5).
  • 3. Cognitively unimpaired (preclinical AD with a global CDR=0) or mildly impaired (prodromal AD with a global CDR=0.5 and maximum CDR-SB \<1.5).
  • 4. MMSE score at screening of 24-30 (inclusive) with educational adjustments:
  • 1. If \<12 years of education, MMSE required to be \>20.
  • 2. If 13 to 15 years (inclusive) of education, MMSE required to be \>22.
  • 3. If \>16 years of education, MMSE required to be \>24.
  • 5. Plasma biomarker result at screening that demonstrate the presence of amyloid pathology, consistent with preclinical-prodromal AD.
  • 6. Elevated brain tau at screening.
  • 7. Stable doses of permitted medications as described per protocol for a minimum of 30 days prior to screening.
  • 8. Resides at home or in the community (assisted living acceptable).
  • 9. In the opinion of the site Principal Investigator (PI) has a study partner able and willing to provide accurate information (including clinical symptoms and medical history) about the participant and participate in study visits and informant-based assessments (usually requires at least 5 hours of contact per week) for the duration of the study.
  • 10. As assessed by the site PI, participant is likely to be able to comply with the protocol for the duration of the study, and has adequate vision, hearing (hearing aid permitted), and literacy (English or Spanish) sufficient for compliance with the required testing procedures.
  • 11. Must complete all screening evaluations as outlined per protocol
  • Exclusion Criteria:
  • 1. Females who are lactating or pregnant (as documented by a urine pregnancy test) during screening, or plan to become pregnant during the study.
  • 2. Females of childbearing potential who did not use a highly effective method of contraception within 28 days of screening and/or are not willing to use highly effective method of contraception for the duration of their participation in the study. Males who are sexually active with a female of childbearing potential and do not agree to use barrier methods of contraception (condoms with spermicide) during the trial and for 6 months after the last dose of study drug unless the female is using a highly effective method of contraception.
  • 3. Inability to receive study intervention from any of the available regimen.
  • 4. Lacks good venous access such that multiple blood draws would be precluded.
  • 5. Weighs less than 40 kilograms (kg), or more than 136 kg at screening.
  • 6. Suspected or known allergic reactions, adverse reactions, or hypersensitivity to any components of the study intervention for any of the available regimen.
  • 7. Previous treatment with the study intervention from any available regimen unless it can be confirmed the participant received placebo in the previous study.
  • 8. Prior or current treatment with a prohibited medication as described per protocol.
  • 9. Enrollment in another investigational study as described per protocol. NOTE: Participants enrolled in an observational study may be permitted with Medical Monitor review and approval.
  • 10. Contraindications to MRI studies, including metal (ferromagnetic) implants, a cardiac pacemaker that is not compatible with MRI, and/or severe claustrophobia.
  • 11. Magnetic resonance imaging (MRI) scan at screening showing a single area of cerebral vasogenic edema, superficial siderosis, or evidence of a prior macrohemorrhage, or showing more than four (4) cerebral microhemorrhages (defined as 10 millimeter (mm) or less at the greatest diameter); a single macrohemorrhage greater than 10 mm at greatest diameter (also referred to within this protocol as intracerebral hemorrhage \>1 centimeter (cm)); cerebral contusion; encephalomalacia; aneurysms greater than 6 mm, or any aneurysms that have not been stable in size for the past 2 years; vascular malformations that are at high risk for hemorrhage; infective lesions; evidence of multiple lacunar infarcts (that in the opinion of the investigator, may impact cognition); stroke involving a major vascular territory; severe small vessel; severe diffuse white matter disease; space occupying lesions; or brain tumors (however, lesions diagnosed as meningiomas or arachnoid cysts and less than 1 cm at their greatest diameter need not be exclusionary).
  • NOTE: Other minor or clinically insignificant MRI abnormalities, as agreed by the medical monitor and after discussion with the investigator, may not be exclusionary.
  • 12. Contraindications to tau and/or amyloid PET scan imaging and/or use of MK6240 and/or 18F-NAV-4694 (Flutafurnanol).
  • 13. For participants undergoing an lumbar puncture (LP) as part of the optional longitudinal CSF biomarker sub-study, contraindication to undergoing an LP including, but not limited to: inability to tolerate an appropriately flexed position for the time necessary to perform an LP; international normalized ratio (INR) \>1.4 or other coagulopathy; platelet count of \<120,000/microliter (μL); infection at the desired lumbar puncture site; taking anti-coagulant medication within 90 days of LP. NOTE: low dose aspirin is permitted; degenerative arthritis of the lumbar spine; suspected non-communicating hydrocephalus or intracranial mass; prior history of spinal mass or trauma.
  • 14. Any unstable and/or clinically significant medical condition likely to hamper the evaluation of safety and/or efficacy of study drug (e.g., 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 the site PI's judgement.
  • 15. History of severe allergic reaction (e.g., anaphylaxis) including, but not limited to: severe allergic reaction to previous vaccines, foods, and/or medications.
  • 16. Hospitalization within 30 days prior to screening or baseline.
  • 17. Clinically significant infections or major surgical operation within 3 months prior to screening.
  • 18. History of chronic or recurrent infections judged to be clinically significant by the site PI and which would potentially hamper the evaluation of efficacy and safety assessments.
  • 19. Myocardial infarction within 1 year prior to baseline, unstable angina pectoris, or significant coronary artery disease.
  • 20. History of cancer within the past 5 years other than treated squamous cell carcinoma, basal cell carcinoma and melanoma in-situ, in-situ prostate cancer, or in-situ breast cancer, which have been fully removed and are considered cured.
  • 21. History of inflammatory neurological disorders.
  • 22. History or presence of immunological or inflammatory conditions, including neurological disorders, judged to be clinically significant by the site PI.
  • 23. History of meningitis or meningoencephalitis.
  • 24. History of moderate or severe traumatic brain injury.
  • 25. History or presence of uncontrolled seizures. If history of seizures, they must be well controlled with no occurrence of seizures in the 2 years prior to study screening. The use of antiepileptic medications is permitted.
  • 26. Concomitant or past history of psychiatric or neurologic disorder other than those considered to be related to Alzheimer's disease (AD) (e.g., head injury with loss of consciousness, symptomatic stroke, Parkinson's disease, severe carotid occlusive disease, transient ischemic attacks, hemorrhagic and/or non-hemorrhagic stroke).
  • 27. Fifth Edition of the Diagnostic and Statistical Manual of Mental Disorders (DSM-5) criteria for drug or alcohol abuse or dependence currently met within the past 5 years.
  • 28. Significant risk of suicide defined, using the Columbia-Suicide Severity Rating Scale (C-SSRS), as the participant answering "yes" to suicidal ideation questions 4 or 5 or answering "yes" to suicidal behavior within the past 12 months.
  • 29. Clinically significant abnormal vital signs including sustained sitting blood pressure \>160/90 millimeters of mercury (mm Hg).
  • 30. Participants with diabetes mellitus with hemoglobin A1c (HbA1c) levels of \>7.5%.
  • 31. In the opinion of the site PI, clinically significant deviations from normal values for hematologic parameters, liver function tests, and other biochemical measures.
  • 32. Participants with a known history of human immunodeficiency virus infection (HIV-1 and 2).
  • 33. Participants with known history of acute/chronic hepatitis B or C.
  • 34. Clinically significant arrhythmias or other clinically significant abnormalities on electrocardiogram (ECG) at screening (minor abnormalities documented as clinically insignificant by the site PI are allowed).
  • 35. Any condition, which in the opinion of the site PI, Coordinating Center, regulatory sponsor, or Project Lead/Protocol PI, makes the participant unsuitable for inclusion.

About University Of Southern California

The University of Southern California (USC) is a prestigious research institution located in Los Angeles, California, known for its commitment to advancing knowledge and innovation in various fields, including medicine and health sciences. As a clinical trial sponsor, USC leverages its extensive resources, interdisciplinary expertise, and state-of-the-art facilities to conduct cutting-edge research aimed at improving patient outcomes and public health. The university fosters collaboration among its diverse faculty and students, ensuring a dynamic environment for the development and implementation of clinical studies that adhere to the highest ethical and scientific standards. Through its clinical trials, USC aims to contribute to the advancement of medical science and the translation of research findings into practical applications that benefit communities locally and globally.

Locations

Patients applied

0 patients applied

Trial Officials

Paul Aisen, MD

Principal Investigator

University of Southern California (USC) Keck School of Medicine, Alzheimer's Therapeutic Research Institute (ATRI)

Timeline

First submit

Trial launched

Trial updated

Estimated completion

Not reported