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Status:

ACTIVE_NOT_RECRUITING

Study to Assess Safety and Efficacy of PRI-002 in Patients With MCI to Mild Dementia Due to Alzheimer's Disease (AD)

Lead Sponsor:

PRInnovation GmbH

Collaborating Sponsors:

Priavoid

Federal Agency for Disruptive Innovation - SPRIN-D

Conditions:

Mild Cognitive Impairment Due to Alzheimer's Disease

Alzheimer's Disease, Early Onset

Eligibility:

All Genders

55-80 years

Phase:

PHASE2

Brief Summary

Alzheimer's disease (AD) is the most common form of dementia. In the brains of people with AD, certain small substances stick together. This leads to changes in thinking and behaviour. The company PRI...

Detailed Description

Alzheimer's disease (AD) is a progressive neurodegenerative disorder and the most common form of dementia. The post-mortem pathology of AD is mainly characterised by neurodegeneration as well as extra...

Eligibility Criteria

Inclusion

  • Signed and dated written informed consent obtained from the subject and study companion in accordance with applicable regulations.
  • Male or female, aged 55 to 80 years, inclusive.
  • For female subjects: not being of child-bearing potential. This is defined as either permanently sterilised (via hysterectomy, bilateral salpingectomy, or bilateral oophorectomy) or postmenopausal (defined as no menses for 12 months without an alternative medical cause).
  • For male subjects who are sexually active with women of child-bearing potential: agreeing to use acceptable contraception (using a condom or having demonstrated successful vasectomy) and not donate sperm from Screening until 12 weeks after the last dose of study treatment.
  • Body mass index (BMI) between 18.5 and 30.0 kg/m2, inclusive.
  • Diagnosed with MCI due to AD or mild dementia due to AD, according to the NIA-AA criteria.
  • MMSE score of 22 to 30, inclusive.
  • Repeatable battery for the assessment of neuropsychological status - delayed memory index (RBANS-DMI) score ≤85.
  • CDR global score of 0.5 or 1 with a memory score ≥0.5.
  • Confirmation of AD diagnosis, by
  • CSF biomarker profile reflecting AD, according to NIA-AA, or
  • existing positive amyloid positron emission tomography (PET) evidence.
  • Fluency in local language and evidence of adequate intellectual functioning in the opinion of the investigator.
  • Having a reliable informant or caregiver who is willing and able to act as the study companion throughout the duration of the subject's participation. The subject and the study companion must have frequent interaction (defined as a minimum of 6 hours/week on average) according to subject's report.

Exclusion

  • Unable to give informed consent in accordance with applicable regulations.
  • Diagnosed with moderate or severe dementia due to AD according to NIA-AA.
  • History or evidence of any other central nervous system (CNS) disorder(s) that could be interpreted as a cause of cognitive impairment or dementia.
  • History of known or suspected seizures, loss of consciousness, or significant head trauma within 2 years before Screening.
  • History of known or suspected stroke or transient ischaemic attack (TIA) within 2 years before Screening.
  • Evidence of other clinically significant lesions on brain MRI (Fazekas score 3).
  • History or presence of clinically evident cerebrovascular disease (diagnosis of possible, probable, or definite vascular dementia).
  • Other significant pathological findings on brain MRI (for example more than 10 microhaemorrhages or a single macrohaemorrhage \>10 mm at the greatest diameter).
  • Unstable medical, neurological, or psychiatric condition, or presence of major depressive episode at Screening.
  • Life-time history of schizophrenia or history of uncontrolled bipolar disorder within 5 years before Screening.
  • Having a bleeding disorder that is not under adequate control (defined as a platelet count \<50000 or international normalised ratio \[INR\] \>1.5). Participants who are on anticoagulant therapy (for example, warfarin), should have their anticoagulant status optimised and be on a stable dose for 30 days before Screening. Anticoagulant therapy (e.g., clopidogrel bisulfate, carbasalate calcium 100 mg/day, or aspirin 325 mg/day or less) is permitted provided this therapy does not represent a contraindication for a lumbar puncture and CSF sampling (if CSF sampling is required in the absence of historical PET evidence).
  • Having significant kidney disease as indicated by either of the following:
  • Creatinine clearance (eGFR) ≤30 mL/min/1.73m2) as estimated using the modification of diet in renal disease (MDRD) method, or
  • Creatinine ≥2 mg/dL.
  • Having impaired hepatic function as indicated by aspartate amino transferase (AST) or alanine amino transferase (ALT) \>3-fold the upper limit of normal (ULN), or total bilirubin \>2-fold ULN, at Screening.
  • Known to be human immunodeficiency virus (HIV) positive.
  • Known to be hepatitis C or chronic hepatitis B positive.
  • Having any other clinically significant abnormalities in physical examination, vital signs, laboratory tests, MRI, or ECG at Screening or Baseline which in the opinion of the investigator requires further investigation or treatment or which may interfere with study procedures or safety.
  • Use of licensed symptomatic AD medication for less than 90 days or at a non-stable dose over the past 90 days at Baseline (for example acetylcholinesterase inhibitors, memantine, ginkgo).
  • Use of anti-Aβ monoclonal antibody therapy at Baseline.
  • Treatment with one of the following substances:
  • Typical antipsychotic or neuroleptic medication within 90 days before Screening (except for
  • ≤1 mg risperidon, and ≤300 mg quetiapin).
  • Chronic use of opiates or opioids (including long-acting opioid medication) within 90 days before Screening.
  • Stimulant medications (amphetamine, methylphenidate preparations, or modafinil) within 30 days before Screening.
  • Chronic use of benzodiazepines, barbiturates, or hypnotics within 90 days before Screening.
  • Contraindication to MRI. Patients with MRI compatible pacemakers may be allowed to enter the study.
  • Prior or current participation in a clinical trial testing active immunisation against Aβ or tau.
  • Participation in a clinical trial and having taken at least 1 dose of the investigational medicinal product (IMP), within 5 times the IMP half-life time before Baseline, unless confirmed as having been on placebo.

Key Trial Info

Start Date :

December 1 2023

Trial Type :

INTERVENTIONAL

Allocation :

ACTUAL

End Date :

April 30 2026

Estimated Enrollment :

304 Patients enrolled

Trial Details

Trial ID

NCT06182085

Start Date

December 1 2023

End Date

April 30 2026

Last Update

December 30 2025

Active Locations (38)

Enter a location and click search to find clinical trials sorted by distance.

Page 1 of 10 (38 locations)

1

Neuro Health Centrum ltd.

Brno, Czechia, 62800

2

NeuropsychiatrieHK, s.r.o.

Hradec Králové, Czechia, 50341

3

A-Shine, s.r.o.

Pilsen, Czechia, 30100

4

CLINTRIAL, s.r.o.

Prague, Czechia, 10000