Alzheimer Disease Clinical Trial
Official title:
I2PETPG - Quantification and Localisation of Imidazoline2 Binding Sites in a Group of Participants Diagnosed With Alzheimer's Disease Using 11C-BU99008: a Positron Emission Tomography Study
The imdazoline2 binding site (I2BS) is known to reside inside astrocytes. Changes in the
numbers of I2BS in post mortem tissue has implicated them in a range of psychiatric
conditions such as depression and addiction, along with neurodegenerative disorders such as
Alzheimer's disease and Huntington's chorea. Preclinical studies have also demonstrated
functional interactions with the opioid system, where I2BS ligands have been shown to affect
tolerance to morphine and alleviate some of the morphine withdrawal syndrome in rats.
Recently the I2BS and I2BS ligands have been shown to have some interesting analgesic effects
in different models of pain.
The location of I2BS on astrocytic glial cells and the possibility that they may in some way
regulate glial fibrillary acidic protein have led to increased interest into the role of I2BS
and I2BS ligands in conditions characterised by marked gliosis. The number of I2BS has been
shown to increase in Alzheimer's disease post mortem, and it has also been suggested that
I2BS may be a marker for the severity and malignancy of human glioblastomas.
The lack of suitable imaging tools for the I2BS has meant that information regarding the
number and distribution of I2BS in the brain has come from preclinical species and in vitro
post-mortem studies. The recent development of [11C]BU99008 as a suitable PET ligand to
quantify I2BS in vivo, enables the direct quantification of I2BS availability and regional
distribution in the living human brain. In this study the investigators plan to utilise
[11C]BU99008 to quantify the regional brain availability of I2BS in the human brain in vivo
using PET.
Participants with Alzheimer's Disease (AD) (up to 8) will receive up to two PET/CT scans with
11C-BU99008, a tracer alone and then a tracer scan following the administration of idazoxan.
In addition, each participant will receive a structural MRI to enable anatomical registration
of the PET data. These will enable the determination of the number and regional location of
the I2BS in the brain of these conditions. These data will then be compared with that found
in healthy human brains. In order to realise this, 11C-BU99008 scans alone and in conjunction
with the mixed I2BS/α2-adrenoceptor drug idazoxan will be used. There is evidence that the
I2BS have an age related increase in density. In order to be confident that any changes in
the regional density and distribution of the I2BS that is seen is due to disease and not
merely aging our AD participants will be age matched with the healthy participants.
Potential participants that pass an initial telephone screen will be invited to a screening
visit where their eligibility to take part in the study will be determined and informed
consent taken. This will be at the Imperial CRF and Imanova Ltd. The screening will consist
of an interview where the study will be discussed and explained. The participants'
understanding of the procedure, requirements and commitments confirmed and any questions
answered before informed consent taken. In addition to this interview the participants
personal details and demographics will be recorded and a psychiatric and medical history
taken as well as the following:
- Semi-structured interviews/questionnaires will be completed: Mini International
Neuropsychiatric Interview 5 (MINI 5), Cognitive diagnostic test for dementia (CAMCOG)
- A medical examination and blood taken for clinical laboratory testing.
- A structural MRI.
- Review of your medical history and current state of health, including questions about
psychiatric symptoms and your use of prescription and non-prescription drugs, as well as
your use of illegal drugs and alcohol.
- Physical examination such as measurements of blood pressure and heart rate, ECG.
- Collecting a urine sample to check for presence of drugs.
- Alcohol breath test.
- An "Allen's Test" will be performed to check the blood supply to your hand.
- Other questionnaires: Hospital Anxiety and Depression Scale (HADS), Eysenck personality
(revised) (EPQ-R25), Spielberger Trait Anxiety Inventory (STAI), and MRI safety
Participants that are eligible will then be invited to take part in the study. The schedule
detailed below is the preferred scenario, however it may be necessary to perform the MRI and
PET/CT scans on separate days due to considerations of logistics or participant convenience.
If for some reason it is necessary to cancel or suspend a scan due to technical reasons (e.g.
radioligand production failure, scanner failure, etc.), the participant will be asked to
return on another day to repeat the scan/day. This will only happen if they have not had the
radioligand administered for that particular scan by the time the study is suspended. This
will mean that for those participants the days on which each of these scans takes place may
be different.
Each participant will receive up to two PET/CT scans and one MRI:
- Scanning Day; Morning (or Day 1) - structural MRI scan and baseline PET/CT scan with
11C-BU99008 alone to determine the total number of binding sites (total, PET signal).
- Scanning Day; Afternoon (or Day 2) - blocking PET/CT scan with 11C-BU99008 in
combination with a single dose of idazoxan (I2BS block)
The combination of these two scans will allow the dissection of the regional contribution of
the I2BS to the 11C-BU99008 specific signal, in order to get an accurate determination of the
regional I2BS density.
Scanning day - The participants will arrive at Imanova's scanning facility in the Burlington
Danes Building, Hammersmith Hospital in the early morning. The exact time will be determined
by the logistical constraints of the productions of 11C-BU99008. On arrival, participants
will be asked if they agree to carry on participating in the study and their general health
and compliance to study specific restrictions assessed by interview, urine drugs of abuse
screen and breathalyser (for alcohol). Once it is confirmed they are eligible to proceed,
they will undergo the procedures.
The participants will be given a structural MRI scan and will then be cannulated in the
radial artery and have a venous cannula inserted in the forearm or cubital veins. The
arterial cannula is required for the collection of arterial blood sampling throughout the
scan, to measure the concentration of the tracer in the arterial plasma for quantitative
analysis of the PET signal. A venous cannula is required for the administration of
11C-BU99008. Baseline subjective (e.g. Spielberger State Anxiety Inventory (SSAI) and visual
analogue scales (VAS)) and objective measures (e.g. heart rate (HR) and blood pressure (BP))
will be taken before they are prepared and positioned in the scanner for PET/CT scan 1. The
scan will be up to 120 min in length, during which time HR and BP will be monitored. At the
end of the scan, the participants will be removed and another set of subjective and objective
measures taken. They will be given an acute dose of idazoxan (up to 80 mg; p.o.) about 120
min before the start of the PET/CT scan 2 and another round of subjective and objective
measures and arterial blood samples taken as in PET/CT scan 1. At the end of the last PET/CT
scan of the day, the participant will be removed from the scanner, any indwelling cannulae
removed, a final round of subjective and objective measures recorded, and their fitness to be
sent home assessed by the attending clinician. If the participants are scanned on separate
days, this assessment of fitness to be sent home will occur after that days scanning. When
they are fit to leave they will be sent home in a taxi.
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