Alzheimer's Disease Clinical Trial
Official title:
Pilot Study That Investigates the Potential of Using OCT (Optical Coherence Tomography) Measurements of the Thickness of the Retinal Nerve Fiber Layer as a Biomarker for the Early Detection of Alzheimer's Disease.
The purpose of this study is to determine whether by measuring changes in the thickness of the retinal nerve fibre layer (the photosensitive layer at the back of the eye) you could predict if someone would develop Alzheimer's disease in the future. The measurement is made by OCT (ocular coherence tomography), a noninvasive and relatively inexpensive test that uses light waves to scan the back of the eye.
Alzheimer's Disease (AD) is a degenerative neurological disorder characterized by the
insidious onset of a progressive decline in cognitive function. It is the most common form
of dementia affecting an estimated 26 million people worldwide in 2006, a number that is
expected to quadruple by 2050 due to the anticipated increase in life expectancy. Difficulty
remembering names and recent events is often an early clinical symptom as is apathy and
depression. Later symptoms include impaired judgment, disorientation, confusion, behavior
changes and difficulty in swallowing and walking.
New criteria and guidelines for diagnosing Alzheimer's published in 2011 recommend that it
be considered a disease that begins well before the development of symptoms. Brain changes
in individuals with Alzheimer's are thought to begin 10 years or more before symptoms such
as memory loss occur - the asymptomatic preclinical phase of AD. Researchers believe that
treatment to slow down or stop progression of Alzheimer's and preserve brain function will
be most effective when administered early in the course of the disease. The pursuit of
biomarkers to detect asymptomatic preclinical AD is a current issue and potential biomarkers
such as: brain volume, level of glucose metabolism in the brain, levels of beta-amyloid and
tau in the CSF, detection of apoptosing retinal cells (DARC), are being investigated. In
this study we would like to propose the measurement of retinal nerve fiber layer thickness
as a potential key biomarker for the detection of asymptomatic preclinical Alzheimer's and
Mild Cognitive Impairment (MCI).
The eye can be considered a window to the brain and the retina exists as an extension of the
CNS. Changes that occur in the retina can be visualized non-invasively and directly with
increasingly sophisticated imaging techniques. It is now possible to detect changes in
single neurons in the eye. Historically the visual symptoms that have been reported in AD
patients have been attributed to neuronal damage to the visual pathways in the brain rather
than the retina. However there is increasing evidence that shows that the specific
pathological findings in the brain occur in the retina also.
The ocular manifestations in AD were first documented by Cogan in 1985, who documented
deficits in visual acuity, contrast sensitivity, colour vision and motion perception. In
more recent studies using optical coherence tomography (OCT), peripapillary thinning of the
retinal nerve fiber layer (RNFL) has been demonstrated, occurring initially superiorly and
causing inferior visual field loss.
The use of OCT as a non-invasive optical imaging technique has become an accepted method for
assessing the thickness of the RNFL due to its reproducibility and accuracy. Blanks et al.
provided ultrastructural studies that showed retinal ganglion cell degeneration in post
mortem retinas of patients with AD. He demonstrated that in AD extensive neuronal loss was
seen throughout the retina but most pronounced in superior and inferior quadrant and loss in
the central retina, the greatest decrease of neurons being in the temporal foveal region.
Results of a study by C. Paquet, M.Boissonnot et al demonstrated an abnormal RNFL thickness
in patients with amnestic Mild Cognitive Impairment (MMSE score of 25, with subjective
memory complaints), suggesting that the involvement of the retina is an early event in the
development of Alzheimer's.
MCI is generally defined as being problems with memory, language or another essential
cognitive ability that are severe enough to show up on cognitive tests but not to interfere
with daily life. Studies show that 10 -20 % of people aged 65 and older have MCI. 15% of
individuals with MCI progress to dementia each year. No significant difference was found
between RNFL thickness observed in MCI patients and in mild AD patients.
In light of these findings it is proposed that measurement of RNFL could be used to enable
early MCI diagnosis in patients suffering from subtle memory disturbances and as a biomarker
to detect asymptomatic pre-clinical Alzheimer's disease. In light of these findings this
study proposes to take investigations one step further and to see if patients suffering from
subjective memory loss but with normal cognitive tests have abnormal RNFL tests.
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