Evaluate the Agreement and Precision of Device SS-1000 and the Predicate Device the Pentacam in a Reproducibility and Repeatability Trial Clinical Trial
Official title:
To Investigate the Precision and Agreement of SS-1000 and the Predicate Device Pentacam in a Repeatability and Reproducibility Trial (PASP)
This study is to support the substantial equivalence of the SS-1000 to the predicate device
Pentacam.
Primary Objective -The primary objective of the trial is to evaluate the precision of the
SS-1000 and Pentacam in measuring the anterior segment parameters in an eye, including
Corneal Curvature, Corneal Thickness, Anterior Chamber Depth and Cornea Volume.
Secondary Objectives
- To investigate the repeatability (intra-instrument) of SS-1000 and Pentacam in measuring
the anterior segment parameters in an eye
- To investigate the reproducibility (inter-instrument) of SS-1000 and Pentacam in
measuring the anterior segment parameters in an eye
- To investigate the agreement between SS-1000 and Pentacam in measuring the anterior
segment parameters in an eye
Study design
-The trial design is a prospective precision trial with the following factors: The trial will
be conducted at one investigational site. The site will have three SS-1000 devices and three
Pentacam devices available. Three certified operators (#1, #2 and #3) will be randomly
assigned to one set of devices (one SS-1000 and one Pentacam), such that operator effect are
confounded with instrument effect. All participants will have one visit and undergo the same
set of assessments. Each assessment will consist of 2 consecutive readings (M1, M2).
1. Nonsignificant Risk (NSR) Devices
The two devices SS-1000 and Pentacam are considered non-significant risk devices and the
conduct of the trial will adhere to the abbreviated requirements of Investigational
Device Exemption (21CFR812.2, 2011).
2. Overall Trial Design
The trial design is a prospective precision trial with the following factors:
The trial will be conducted at one investigational site. The site will have three
SS-1000 devices and three Pentacam devices available. Three certified operators (#1, #2
and #3) will be randomly assigned to one set of devices (one SS-1000 and one Pentacam),
such that operator effect are confounded with instrument effect. All participants will
have one visit and undergo the same set of assessments. Each assessment will consist of
2 consecutive readings (M1, M2).
To ensure the highest physiological stability of the eyes all measurements will be done
at least 3 hours after subject awake (Lattimore MR, 1999). To decrease the diurnal
variation each subject will have, all measurements excluding screening measurements are
performed within a 2 hour window. All measurements are performed in constant dim
lighting conditions.
Subject will be advised to keep eyes closed between scans to prevent eye dryness. If
subject experience eye dryness subject will be allowed extra time to recover between
measurements.
3. Randomization
3.1 Trial eye
If subject has one eligible eye with pathology, that eye will be selected as the trial
eye.
If subject has two eligible eyes, with or without pathology, the trial eye will be
randomly selected by tossing a coin (Head=right eye, Tail=left eye).
The same eye will be used for all measurements.
3.2 Order of examination
Randomization schedule will be generated using a computer and will be used to determine
the order of the devices (SS-1000 vs. Pentacam) and the order of the
instruments/operators (instrument set #1, instrument set #2 or instrument set #3).
4. Masking
The corneal condition (thin, normal and thick) will not be available to the operators
while obtaining data for determination of repeatability and reproducibility.
5. Discussion of Design
The trial design serves the purpose to evaluate the agreement and precision (total
precision / repeatability / reproducibility) performance characteristics for SS-1000 and
Pentacam. The precision results will be used for the evaluation of substantial
equivalence between SS-1000 and Pentacam.
This trial is designed to use the same cohort of subjects to minimize between subject
variability. Each subject undergoes examination by 3 operators with 3 instruments each
and 2 replicates in each condition. This design will provide a head-to head comparison
in total precision, agreement, repeatability and reproducibility.
The between-operators will be confounded but all assessments in the trial are objective
and automatically assessed by both investigational devices. Hence, potential biases
should be at a minimum in terms of interpretation of trial results. Potential biases may
occur due to the fatigue of subjects and/or the operators. Thus, to minimize biases the
order of the devices will be randomly assigned.
To avoid other confounding factors (e.g. visit) subjects will have all assessments done
at one visit, each subject undergoes 12 measurements. The duration of the tests are
estimated to last at least 1 hour which we considered as the upper limit for a subject
before fatigue and eye irritation due to dryness. Once a subject starts to experience
dryness in the eyes, subject will not be able to fixate and keep the eye open without
blinking while the measurement takes place. To prevent eye dryness subject should have
his eyes closed between measurements.
All devices are evaluated using the same set of subjects and allows for direct
comparison of the investigational device and the predicate device.
6. Trial Population
A total of 66 eyes from 66 subjects meeting all of the following inclusion criteria and none
of the exclusion criteria will be recruited:
6.1 Inclusion Criteria
Subjects/eyes who meet each of the following criteria are eligible for the trial:
- Subject Inclusion Criteria
1. Female or male age 22 years or older at time of screening
2. Able to fixate at the internal fixation
3. Able to open eyes sufficiently to enable a full image area
4. Written informed consent obtained from subject before any investigational
assessment
- Eye Inclusion Criteria
5.Eyes with one of the following cornea conditions (Francis BA, 2008):
1. Normal cornea (CCT between 511-580 µm with or without pathology)
2. Thin cornea, i.e. previous refractive surgery, corneal ectasia, keratoconus (CCT
≤510 µm with or without pathology)
3. Thick cornea, i.e. Fuchs' dystrophy, bullous keratopathy, corneal edema (CCT >580
µm with or without pathology)
6.2 Exclusion Criteria
Eyes who meet one or more of the following criteria are excluded from the trial:
1. Use of rigid contact lenses within one week from start of trial 2. Use of soft
contact lenses within 24 hours of any trial measurement 3. Aphakic eyes 4. Eyes
with a history of intraocular, corneal surgery, except refractive surgery 5.
Currently on mydriatic and/or miotic medication that can affect ocular physiology
6. Seriously ill or unconscious subject, mentally ill person, mentally handicapped
person, person who is unable to read or write
When both eyes of a subject are eligible, one eye will be randomly selected.
To ensure recruitment of eyes with a range of corneal thicknesses, inclusion
criterion no. 5 will be controlled:
1. Normal cornea (22 eyes)
2. Thin cornea (22 eyes)
3. Thick cornea (22 eyes).
6.3 Subject identification
All subjects enrolled must be identifiable throughout the trial. This will be
done by using a 3-digit subject number starting at 001 allocated to the
subject when enrollment is determine by the investigator.
6.4 Subject Withdrawal
The subject will be advised in the informed consent form that he/she has the
right to withdraw from the trial at any time without reason. The subject may
also be withdrawn from the trial at the investigator's or Tomey's discretion
at any time. In case a subject drops out of the trial or is withdrawn from the
trial, the withdrawal page in the case report form (CRF) should be completed.
On the withdrawal page the investigator should record the date of the
withdrawal, the person initiating the withdrawal and the primary reason for
withdrawal.
Subjects withdrawn during trial will not be replaced.
7. Visit Schedule and Assessments
7.1 Visit
The following procedures will be performed at the visit:
• Obtain written informed consent before any trial procedures are performed
• Obtain demographic data (age, race, and sex).
• Obtain corneal characteristics and pathology.
• Screening with SS-1000 and Pentacam.
• Recording of concomitant medication.
• Assess compliance with inclusion and exclusion criteria.
- Imaging by 3 devices and 3 instruments/operators in a random order o Two
readings with SS-1000 (1) by Operator #1 o Two readings with Pentacam (1) by
Operator #1
o Two readings with SS-1000 (2) by Operator #2
- Two readings with Pentacam (2) by Operator #2
- Two readings with SS-1000 (3) by Operator #3
- Two readings with Pentacam (3) by Operator #3
- AE recording if any has occurred in relation to trial procedures.
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