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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00750282
Other study ID # 311741
Secondary ID 2007-002256-4231
Status Completed
Phase Phase 2
First received September 9, 2008
Last updated July 15, 2014
Start date August 2008
Est. completion date November 2010

Study information

Verified date July 2014
Source Piramal Imaging SA
Contact n/a
Is FDA regulated No
Health authority Germany: Federal Institute for Drugs and Medical DevicesSwitzerland: SwissmedicAustralia: Department of Health and Ageing Therapeutic Goods AdministrationJapan: Pharmaceuticals and Medical Devices AgencyUnited States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

The aim of this study is to evaluate the efficacy, safety of a single dose of BAY 94-9172 (ZK 6013443) as an investigational medicinal product (IMP) in detecting cerebral protein-plaque (amyloid beta) with positron emission tomography (PET). IMP binds to amyloidal beta protein accumulating in brain tissue already from early stages of Alzheimer's disease (AD). IMP is therefore a potential tracer to be used for detecting amyloid plaques. For each subject it is required to visit the study centre during the screening phase, on the PET imaging day and for 1 follow-up visit on the next day. A telephone call for safety follow-up will be performed 7 days after IMP administration. During the screening phase the subject's medical, neurological and surgical history, specific laboratory tests related to AD, MRI of the brain and certain neuro-psychiatric tests will be performed. Clinical safety measures (physical examinations, vital signs, electrocardiogram (ECG) and laboratory tests) will be performed on the PET imaging day before IMP injection and monitored during and after two PET imaging sessions. Clinical safety measures will be performed again on the follow-up visit next day. The results of PET imaging with IMP will be compared between probable AD patients and healthy volunteers (HV). The clinical diagnosis is based on international validated and accepted criteria and established after comprehensive clinical and neuro-psychiatric examinations


Recruitment information / eligibility

Status Completed
Enrollment 422
Est. completion date November 2010
Est. primary completion date November 2010
Accepts healthy volunteers No
Gender Both
Age group 55 Years and older
Eligibility Inclusion Criteria:

- Each subject / Healthy volunteer (HV) who meets the following criteria will be eligible for enrollment into the study:

- Is a man or woman and is > 55 of age, whereby females must be without childbearing potential (confirmed by either: age >/= 60; or history of hysterectomy, or last spontaneous bleeding at least 2 years prior to the study start)

- Has at least 6 years of education

- Is able to provide informed consent, understand the information provided on the purpose and conduct of the trial and to comply with study procedures

- Possesses a general health that permits adequate compliance with all study procedures

- The subject, or the subject and caregiver (for probable AD patients) will be compliant and have a high probability of completing the study

- Informed consent has been signed and dated (with time) by the subject and/or the subject's caregiver (for probable AD patients)

- Inclusion criteria for HV only:

- Has no evidence of cognitive impairment

- Has MRI brain scan that has been judged as "normal" (age- appropriate)

- Inclusion criteria for patients with AD only:

- Presents with positive assessment for dementia of Alzheimer's type

- Does not fulfill the criteria Dementia with Lewy Bodies (DLB) or Vascular Dementia (VaD)

- MRI brain scan findings that do not reveal changes indicative of stroke and/or generalized cerebrovascular disease

- Has a caregiver that is willing and able to attend all study visits and perform the psychometric tests requiring the presence of a caregiver

Exclusion Criteria:

- Has any contraindication to MRI examination scan

- Is scheduled for surgery and/or another invasive procedure within the time period of up to 24 hours following IMP application

- Is allergic to the IMP or any of its constituents and/or has a history of severe allergic reactions to drugs or allergens (e.g. patients / volunteers with allergic asthma)

- is critically ill and/or medically unstable and whose clinical course during the observation period is unpredictable

- Has a history of exposure to any radiation >15 milli Sieverts (mSv)/year (e.g. occupational or radiation therapy)

- Is receiving drug therapy or other treatment that is known to lead to greatly fluctuating values of the hematological or chemical laboratory parameters or to severe side effects (e.g. chemotherapy)

- Has been previously enrolled in this study or participated in a clinical study involving an investigational pharmaceutical product within 30 days prior to screening, and/or any radiopharmaceutical

- Has a brain tumor or other intracranial lesion, a disturbance of cerebro-spinal fluid (CSF) circulation (e.g., normal pressure hydrocephalus) and/or a history of head trauma or brain surgery

- Has an inflammatory or infectious central nervous system (CNS) disease, e.g. multiple sclerosis, HIV, syphilis, or Creutzfeldt-Jacob disease

- Has a history, physical, laboratory or imaging findings indicative of a neurological or psychiatric illness

- Has another disease that can cause disturbance of brain function (e.g. vitamin B12 or folic acid deficiency, disturbed thyroid function)

- Has a history of alcohol or drug abuse

- Has history of severe persistent depression

Study Design

Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Diagnostic


Related Conditions & MeSH terms


Intervention

Drug:
Florbetaben (BAY94-9172)
Healthy volunteers and patients with probable Alzheimer's disease receiving single injection of investigational medicinal product BAY 94-9172 followed by subsequent PET imaging sessions

Locations

Country Name City State
n/a

Sponsors (1)

Lead Sponsor Collaborator
Piramal Imaging SA

Countries where clinical trial is conducted

United States,  Australia,  Germany,  Japan,  Switzerland, 

References & Publications (1)

Barthel H, Gertz HJ, Dresel S, Peters O, Bartenstein P, Buerger K, Hiemeyer F, Wittemer-Rump SM, Seibyl J, Reininger C, Sabri O; Florbetaben Study Group. Cerebral amyloid-ß PET with florbetaben (18F) in patients with Alzheimer's disease and healthy contro — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Specificity and Sensitivity of Florbetaben PET Scans Obtained in Part A Using Two Separate Algorithms and the Onsite Clinical Diagnosis as the Standard of Truth Part A: For the calculation of sensitivity/specificity, a patient with probable AD was expected to have a positive florbetaben PET scan which was considered a match for sensitivity. A HV was expected to have a negative florbetaben PET scan which was considered a match for specificity. Standard of truth was the onsite clinical diagnosis.
Two Beta-Amyloid Plaque Load (BAPL) algorithms for assessing the normality/abnormality of beta-amyloid plaque load in the brain scans were used.
Using algorithm A (Majority Read), a brain scan of a subject with a BAPL score of "1" (without beta-amyloid plaque load) or "2" (with minor beta-amyloid plaque load) was considered normal and a BAPL score of "3" (with significant beta-amyloid plaque load) was considered abnormal.
Using algorithm B (Average), a brain scan of a subject with a BAPL score of "1" was considered normal and a brain scan with a BAPL score of "2" or "3" was considered abnormal. Algorithm B was used in Part B and in the final
90 - 110 min after investigational medical product (IMP) injection No
Primary Specificity and Sensitivity of Florbetaben PET Scans Obtained in Part B Using Two Separate Algorithms and the Onsite Clinical Diagnosis as the Standard of Truth. Part B: For the calculation of sensitivity/specificity, a patient with probable AD was expected to have a positive florbetaben PET scan, ie,abnormal scan (BAPL scores "2" or "3") which was considered a match for sensitivity. A HV was expected to have a negative florbetaben PET scan, ie,normal scan (BAPL score "1") which was considered a match for specificity.
The clinical diagnosis was established by an independent consensus panel (CP) of experts in dementia.
Two independent sets of PET data reads were performed. The first set was performed by a panel of three readers who received live, instructor-led training on the visual assessment procedure. The second set was performed by a panel of five separate readers who were trained on the visual assessment procedure with electronic media.
90 - 110 min after IMP injection No
Secondary Sensitivity and Specificity for All Participants Using Two Additional Imaging Windows for the Visual Assessment PET scans from two additional imaging windows (45-60 min and 110-130 min) were visually assessed 45 - 60 min and 110 - 130 min after IMP injection No
Secondary Kappa Coefficient as a Measure of Agreement Between Readers Concerning the Visual Assessment of Abnormality of the Brain Scan (Based on BAPL Score) The agreement between 3 blinded readers concerning the visual assessment of abnormality of the brain scan (based on BAPL score) was measured by the kappa coefficient. Kappa values close to 1.0 indicate a high agreement while values close to 0 indicate random agreement. 45-60 min, 90-110 min, 110-130 min No
Secondary Standard Uptake Value Ratios for Florbetaben Signal The Standard Uptake Value Ratios for florbetaben signal in the frontal cortex, lateral temporal cortex, parietal cortex, anterior cingulate, posterior cingulate cortex, occipital cortex, and cerebellum (white matter) were determined as a quantitative measure of tracer uptake. The SUV is defined as the ratio of (1) the tissue radioactivity concentration c (in MBq/kg) at time point t, and (2) the injected activity (in MBq, extrapolated to the same time t) divided by the body weight (in kg). These SUV numbers from regions of interest were then used to derive SUV ratios (SUVR) using the SUV from the cerebellar cortex as reference.) 90-110 min post injection No
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