Atlas of Retinal Imaging in Alzheimer's Study

This will be a longitudinal, within-participants prospective natural history study.
Participants will be recruited on the basis of serial referrals to the memory disorders
centers at all three investigative sites, as well as by Institutional Review Board
(IRB)-approved radio, social media and print advertisements. All participants will meet
inclusion/exclusion criteria for one of the four (4) participant groups. All participants
will be recruited into the study over a 24-month enrollment period. Once enrollment closes,
participants will be followed for 3 years, with examinations at one of the four study
locations at baseline, 12 months post-enrollment, 24 months post-enrollment, and 36 months
post-enrollment. All exam and testing procedures are described below. All retinal imaging
will be completed on an FDA-approved clinical OCT imaging system by trained study personnel
(with quality assurance and participant safety managed by two Co-Principal Investigator
(PI)'s and their staff). Pupillometry and contrast sensitivity vision testing will rely on
FDA-approved and commercially widely available devices and standard clinical procedures. All
techniques are well-known to both PI's, and these techniques have been in regular use by
their clinical research and/or clinical care groups for the past 6+ years.

During the screening visit a cheek swab will be obtained to determine apolipoprotein (APOE)
genotype. Enrollment and group assignment will be established once the genotyping results are
received (i.e., approximately 55 minutes following cheek swab, and by the end of each
screening visit), at which point individuals who meet enrollment criteria will be scheduled
for their baseline visit. PIs may choose to include disclosure of APOE genotyping results in
their location-specific protocol, if they have the appropriate clinical resources and local
IRB approval for disclosure procedures. Genotyping results will not be released to
participants or their physicians except through the process of an IRB approved, site-specific
protocol for disclosure.

At each study visit (i.e., baseline, 12 months, 24 months, and 36 months) participants will
undergo an eye examination and screening for ophthalmic disease, a medical screening exam,
vital signs, neuropsychological assessment, a blood sample for measurement of plasma
biomarkers, and a full retinal imaging exam. All participants will be asked to provide
consent to allow review of medical records, including relevant imaging (including both
clinical reports and Digital Imaging and Communications in Medicine (DICOM) image files for
computerized tomography (CT)/ magnetic resonance imaging (MRI) and amyloid positron emission
tomography (PET) neuroimaging) and cerebrospinal fluid (CSF) biomarker evidence of AD, if
available. Additional clinical and experimental endpoints will include measures of gait,
sleep quality, social and psychological health, and pupillometry. Assessment of sleep
architecture (i.e., actigraphy measures) will be collected via wearable trackers over the
course of a 2-week period following the baseline and 36-month study visits. A subset of
participants, in each of the subject groups, will be asked to take an over-the-counter herbal
supplement (Longvida curcumin; Verdure Sciences, Inc., www.longvida.com) for two days prior
to their baseline exams.

Inclusion Criteria (ALL PARTICIPANTS):

- · Individuals between the ages of 55 and 80 years old (inclusive).

- Permitted medications stable for at least 1 month prior to screening. In
particular:

- Participants may take stable doses of antidepressants lacking significant
anticholinergic side effects (if they are not currently depressed and do not have
a history of major depression within the past year).

- Adequate visual and auditory acuity to allow neuropsychological testing, as
determined by the eye exam and the neuropsychologist's judgment. Hearing
augmentation by hearing aids is allowed.

- Good general health or without any clinically significant abnormalities (see
exclusion criteria) that would be expected to interfere with participation in the
study.

- Participants must be willing and able to provide written informed consent.

- Participants must have a study partner (i.e., family member, close friend, or
caregiver) who can attend study appointments with them and report on their level
of daily functioning.

- As this is entirely an observational study, without treatment intervention, we
will allow concurrent enrollment in other clinical trials for mild cognitive
impairment (MCI) or AD, including those that involved the use of investigational
drugs. Relevant information about other studies in which participants are
participating (e.g., study name, sponsor) will be collected and considered as a
potential statistical covariate in the statistical analysis plan (SAP).

Additional Inclusion Criteria - Healthy Control Participants

- Montreal Cognitive Assessment (MoCA) total score > 26 at screening

- Clinical Dementia Rating (CDR) 0 at screening

- An absence of substantial subjective memory complaints or worry

- No first degree relative with either diagnosed AD or suspicion of AD

- A screening genotype result showing non-carrier status for APOE ε4 allele

Additional Inclusion Criteria - High-Risk for Preclinical AD Participants

- MoCA total score > 26 at screening

- CDR 0 at screening

- No clinical diagnosis of MCI or dementia of any type

- Must have all of the following three risk factors for AD:

- Subjective memory complaints as ascertained on a standardized questionnaire (i.e.,
ECOG).

- A positive (suspected) first-degree family history for the disease.

- A screening genotype result showing carrier status for at least one APOE ε4 gene
allele Additional Inclusion Criteria - Patients with Mild Cognitive Impairment

- MoCA total score > 19 at screening

- CDR 0.5 at screening

- A clinical diagnosis of MCI (amnestic type, but may include multiple domains) from
qualified specialist or from a memory disorders clinic or center

- Score of less than or equal to 85 (1.5 SD below age and education adjusted normative
data) on the RBANS Delayed Memory Index (DMI)

- Positive prior biomarker evidence of Alzheimer's disease (PET imaging or CSF study),
if available

Additional Inclusion Criteria - Patients with Mild Alzheimer's Disease

- MoCA total score > 15 and < 26 at screening

- CDR 1 at screening

- A clinical diagnosis of mild AD from qualified specialist or from a memory disorders
clinic or center

- Score of less than or equal to 85 (1.5 SD below age and education adjusted normative
data) on the RBANS Delayed Memory Index (DMI)

- Positive prior biomarker evidence of Alzheimer's disease (PET imaging or CSF study),
if available

- Informed consent provided from partner, caregiver or immediate family member, with
verbal assent provided by individual patient.

Exclusion Criteria:

- · Patients with histories of other ocular or neurologic disease that could affect the
results, such as unusually high refractive errors ( > or < 5.0 diopters native
spherical equivalent), age related macular degeneration, diabetic retinopathy,
hypertensive retinopathy, retinal vascular disease, glaucoma, optic nerve disease,
cystic macular edema, large cataracts or corneal disease that may preclude
visualization of the retinal fundus, substantial ocular media opacity, and/or
intraocular surgery within 90 days of any study visit will be excluded.

- History of severe brain injury or other known neurologic disease or insult,
which, as described by medical records, and/or as determined by the PI's clinical
judgment, has resulted in lasting cognitive sequelae that would confound the
assessment and staging of potential neurodegenerative disease.

- Geriatric Depression Scale Short Form (GDS-S 15 Items) score > 6.

- Poorly controlled major depression or another psychiatric disorder within the
past year.

- History of alcohol or substance abuse and/or dependence within the past 2 years
(DSM-V criteria).

- History of schizophrenia or a history of psychotic features, agitation or
behavioral problems within the last 3 months, which could lead to difficulty
complying with the protocol.

- Participants who, in the investigator's opinion, will not comply with study
procedures.

- Any significant systemic illness or unstable medical condition which could lead
to difficulty complying with the protocol including:

- History of systemic cancer within the past 5 years (non-metastatic skin cancers
are acceptable).

- History of clinically significant liver disease, coagulopathy, or vitamin K
deficiency within the past 2 years.

- History of myocardial infarction within the past six (6) months or unstable or
severe cardiovascular disease including angina or congestive heart failure (CHF)
with symptoms at rest.

- History of stroke(s) with lasting impairment to vision or the visual system,
coagulopathy, uncontrolled hypertension (i.e., systolic BP > 170 or diastolic BP
> 100) and uncontrolled or insulin requiring diabetes. Blood pressure will be
recorded on the day of each examination.

- Evidence of enlarged ventricles and/or normal pressure hydrocephalus on review of
medical records or inspection of CT/MRI of the brain based on previous clinical
diagnosis (MRI) as noted in their neurological history

- History of Parkinson's disease, Parkinsonism due to multiple system atrophy
(MSA), progressive supranuclear palsy (PSP), Shy Drager Syndrome (SDS) or other
neuro-degenerative dementias

- History of symptoms of narrow-angle glaucoma (warning signs include eye pain,
restricted vision, blurred vision)

- History of elevated intraocular pressure, or medical record evidence of
intraocular pressure > 20 mm Hg

- Regular (daily) use of narcotics or antipsychotic medications.

- New use of anti-Parkinsonian medications (e.g., sinemet, amantaine,
bromocriptine, pergolide and selegiline) within 2 months prior to screening.

- New use of anti-convulsants (e.g., phenytoin, phenobarbital, carbamazepine)
within 2 months prior to screening.

- New use of centrally active beta-blockers, narcotics, methyldopa and clonidine
within 4 weeks prior to screening.

- New use of neuroleptics or narcotic analgesics within 4 weeks prior to screening.

- New and chronic use of long-acting benzodiazepines or barbiturates within 4 weeks
prior to screening.

- Use of short-acting anxiolytics or sedative-hypnotics more frequently than 2
times per week within 4 weeks prior to screening (note: sedative agents should
not be used within 72 hours of the baseline and follow-up visits).

- Initiation or change in dose of an antidepressant lacking significant cholinergic
side effects within the 4 weeks prior to screening (use of stable doses of
antidepressants for at least 4 weeks prior to screening is acceptable)

- An anticholinergic burden score of >3 on the Anticholinergic Cognitive Burden
Scale (see appendix item 9.19).

- Known hypersensitivity to anticholinergic medications, including tropicamide eye
drops.