ACTIVE_NOT_RECRUITING

VY7523-102: Randomized, Placebo-Controlled, Double-Blind, Multiple Ascending Dose Study in Participants With Early Alzheimer's Disease

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Conditions

Alzheimer's Disease (AD)

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Study Overview

This clinical trial focuses on testing the efficacy of different digital interventions to promote re-engagement in cancer-related long-term follow-up care for adolescent and young adult (AYA) survivors of childhood cancer.

Description

This study is to be conducted in participants with early Alzheimer's Disease to test VY7523, a new drug being researched for treatment of Alzheimer's Disease. This study will look at how safe the drug is and how it works in the brain. It was first tested in normal, healthy participants who volunteered to participate. The study will look at three different dose levels, starting with the lowest dose first and moving to higher doses and more participants after safety has been reviewed by doctors and researchers. Some patients will receive drug while others will receive placebo. This will help to better compare how the drug works between participants receiving drug and placebo. The study will last up to 6 months for the lower dose groups and 12 months for the highest dose group.

Official Title

VY7523-102: A Randomized, Placebo-Controlled, Double-Blind Study to Evaluate the Safety, Tolerability, Pharmacokinetics, and Preliminary Efficacy of Multiple Ascending Intravenous Doses of VY7523 in Participants With Early Alzheimer's Disease

Quick Facts

Study Start:2025-03-03
Study Completion:2027-05
Study Type:Not specified
Phase:Not Applicable
Enrollment:Not specified
Status:ACTIVE_NOT_RECRUITING

Study ID

NCT06874621

Participation Criteria

Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.

Ages Eligible for Study:50 Years to 90 Years
Sexes Eligible for Study:ALL
Accepts Healthy Volunteers:No
Standard Ages:ADULT, OLDER_ADULT
Inclusion CriteriaExclusion Criteria
  1. 1. Clinical diagnosis of early AD, defined as:
  2. 1. Meet the NIA-AA core clinical criteria for MCI due to AD or mild AD.
  3. 2. Mini Mental State Examination (MMSE) score between 18 and 30, inclusive, at Screening (Cohort 1 and 2) and score between 22 and 30, inclusive, at Screening (Cohort 3).
  4. 3. Report a history of subjective memory decline with gradual onset and slow progression over at least the last 6 months before Screening; must be corroborated by an informant/caregiver.
  5. 4. CDR Memory Box score ≥0.5 CDR global score of 0.5 for MCI due to AD or 0.5 or 1 for mild AD.
  6. 2. Evidence of pathology consistent with AD diagnosis:
  7. 1. For Cohort 1 and Cohort 2 only, by documented historical amyloid PET showing imaging agent uptake into the brain conducted within 24 months before screening OR elevated plasma pTau217/np-Tau217 ratio within the Screening Period.
  8. 2. For Cohort 3 only, evidence of pathology consistent with AD diagnosis by both:
  9. * Evidence of Tau PET imaging agent uptake into the brain by central read AND
  10. * Evidence of positive brain amyloid pathology as indicated by one of the following:
  11. 1. Documented historical amyloid PET showing imaging agent uptake into the brain conducted within 24 months before screening OR
  12. 2. CSF beta amyloid and tau levels consistent with AD diagnosis within the Screening Period.
  13. 3. Body mass index (BMI) ≥18 and ≤35 kg/m2 at Screening.
  14. 4. Apart from the clinical diagnosis of early AD, participant must be in good health, based on medical history and screening assessments.
  15. 5. If participant is receiving an approved symptomatic AD treatment such as but not limited to acetylcholinesterase inhibitor (AChEIs), memantine, rivastigmine, galantamine and tacrine for AD, participant must be on a stable dose for at least 8 weeks prior to Screening.
  16. 1. Treatment-naive participants for AD can be entered into the study.
  17. 2. Unless otherwise stated, participants must have been on stable doses of all other (non-AD-related) permitted concomitant medications for at least 4 weeks prior to Screening.
  18. 3. Participants currently on β amyloid therapies may not be enrolled.
  19. 6. Must have an identified reliable informant/caregiver (defined as a person able to support the participant for the duration of the study e.g., spouse, sibling, close friend, who spends at least 10 hours per week with the participant) who assented to:
  20. 1. Accompany the participant to clinic visits.
  21. 2. Provide information to study Investigator/staff about functioning, cognitive abilities and AEs.
  22. 3. Support participants returning for per-protocol follow-up visits and procedures.
  1. 1. Any medical or neurological/neurodegenerative or psychiatric condition (other than AD) that, in the opinion of the Investigator, may be contributing cause to cognitive impairment or could confound interpretation of drug effect, affect study assessments, or affect participant's ability to participate and complete the study or lead to safety concerns.
  2. 2. History of transient ischemic attack or stroke or any unexplained loss of consciousness within 1 year prior to Screening.
  3. 3. History of seizures within 10 years prior to screening or history of epileptic syndrome (except for history of febrile seizures in childhood)
  4. 4. Lifetime history of a major psychiatric disorder including schizophrenia or bipolar disorder. History of major depressive disorder that has resulted in 2 or more hospitalizations in a lifetime.
  5. 5. Presence of a clinically significant uncontrolled medical disorder involving one or more of these major organ systems: cardiovascular (including but not limited to a QTcF of \>470 ms for women and \>450 ms for men and uncontrolled hypertension), respiratory, renal, gastrointestinal, immunologic, hematologic including bleeding disorder, hepatic, or endocrine.
  6. 6. Contraindications to lumbar puncture, including but not limited to coagulation or bleeding disorders, unsafe suspension of anticoagulant, infections at the injection site, spinal deformities or previous spinal surgeries that may affect safe LP performance, or conditions associated with increased intracranial pressure.
  7. 7. Contraindications to MRI scanning, including but not limited to cardiac pacemaker/defibrillator, ferromagnetic metal implants (devices other than those approved as safe for use in MRI scanners).
  8. 8. History of a malignant disease (cancer) except for resected cutaneous squamous cell carcinoma in situ, basal cell carcinoma, cervical carcinoma in situ, in situ prostate cancer with a normal posttreatment prostate-specific antigen within the last five years or other cancers in remission for at least 5 years
  9. 9. Any immunological disease which is not adequately controlled, or which requires treatment with immunoglobulins, systemic mAbs (or derivatives of mAbs), systemic immunosuppressants, or plasmapheresis during the study.
  10. 10. History of severe allergies, or history of an anaphylactic reaction (nonactive hay fever is acceptable).
  11. 11. Participation in a clinical drug trial or device within 30 days (or 5 half-lives, whichever is longer and 3 months for a biologic) of screening, unless the study blind has been broken and the participant was known to be on placebo.
  12. 12. Last administration of B-secretase and gamma-secretase inhibitors in a study within 3 months or 5 half-lives (whichever is longer) prior to screening, unless it can be documented that the participant only received placebo.
  13. 13. Current use of an approved AD disease modifying or anti-amyloid therapy (including but not limited to any mAb therapies).
  14. 14. Presence of risk for increased or uncontrolled bleeding and/or risk of bleeding that is not managed optimally and could place a participant at an increased risk for intraoperative or postoperative bleeding.

Contacts and Locations

Principal Investigator

Chief Medical Officer
STUDY_DIRECTOR
Voyager Therapuetics, Inc.

Study Locations (Sites)

VYGR Site 840018
Los Angeles, California, 90033
United States
VYGR Site 840016
Orange, California, 92866
United States
VYGR Site 840022
San Francisco, California, 94158
United States
VYGR Site 840008
Stamford, Connecticut, 06905
United States
VYGR Site 840005
Delray Beach, Florida, 33445
United States
VYGR Site 840021
Fort Myers, Florida, 33912
United States
VYGR Site 840010
Lady Lake, Florida, 32159
United States
VYGR Site 840015
Miami, Florida, 33126
United States
VYGR Site 840014
Miami, Florida, 33135
United States
VYGR Site 840024
Miami, Florida, 33137
United States
VYGR Site 840006
Orlando, Florida, 32803
United States
VYGR Site 840003
Stuart, Florida, 34997
United States
VYGR Site 840004
The Villages, Florida, 32162
United States
VYGR Site 840002
Wellington, Florida, 33414
United States
VYGR Site 840020
Winter Park, Florida, 32789
United States
VYGR Site 840007
Decatur, Georgia, 30030
United States
VYGR Site 840012
Toms River, New Jersey, 08755
United States
VYGR Site 840009
Matthews, North Carolina, 28105
United States
VYGR Site 840011
Plymouth Meeting, Pennsylvania, 19462
United States

Collaborators and Investigators

Sponsor: Voyager Therapeutics

  • Chief Medical Officer, STUDY_DIRECTOR, Voyager Therapuetics, Inc.

Study Record Dates

These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.

Study Registration Dates

Study Start Date2025-03-03
Study Completion Date2027-05

Study Record Updates

Study Start Date2025-03-03
Study Completion Date2027-05

Terms related to this study

Additional Relevant MeSH Terms

  • Alzheimer's Disease (AD)