Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT02671539 |
| Other study ID # |
THOR-TUE-01 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 2
|
| First received |
|
| Last updated |
|
| Start date |
January 2016 |
| Est. completion date |
February 2018 |
Study information
| Verified date |
October 2020 |
| Source |
STZ eyetrial |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
An open label monocentric phase II trial in adult males with a clinical phenotype of
choroideremia and a confirmed molecular diagnosis of a null mutation in the gene encoding
REP1 to assess the anatomical and functional outcomes, as well as the safety of a single
subretinal injection of rAAV2.REP1 in 6 subjects with genetically confirmed choroideremia for
up to 24 months.
Description:
Study name: THOR - Tübingen Choroideremia gene therapy trial open label Phase 2 clinical
trial using an adeno-associated viral vector (AAV2) encoding Rab-escort protein 1 (REP1)
Phase: Phase II
Indication: Adult males with a clinical phenotype of choroideremia and a confirmed molecular
diagnosis of a null mutation in the gene encoding REP1
Aim of study: To assess the anatomical and functional outcomes, as well as the safety of a
single subretinal injection of rAAV2.REP1 in subjects with genetically confirmed
choroideremia for up to 24 months.
Primary Endpoint: Change from baseline in best corrected visual acuity in treated eye,
compared to untreated control eye
Study design: Open label monocenter study
Study population: 6 male adults affected by choroideremia
Inclusion Criteria
1. Participant is willing and able to give informed consent for participation in the study.
2. Male aged 18 years or above.
3. Genetically confirmed diagnosis of choroideremia. Patients without a confirmed mutation
in the CHM gene, but who have the clinical phenotype typical of choroideremia can only
be enrolled if they meet all the following three criteria: (i) family history consistent
with X-linked inheritance, (ii) absent REP1 protein on Western blot of a blood sample
and, (iii) normal RPE65 gene on sequencing.
4. Active disease visible clinically within the macula region
5. Best-corrected visual acuity equal to or worse than 6/9 (20/32; Decimal 0.63; LogMAR
0.2) but better than or equal to 6/60 (20/200; Decimal 0.1; LogMAR 1.0) in the study
eye.
Exclusion Criteria
1. Female and child participants (under the age of 18)
2. Participants with a history of amblyopia in the study eye
3. Men unwilling to use barrier contraception methods, if relevant
4. Absence of quantifiable visual function in the fellow eye or other ocular morbidity
which might confound use of the fellow eye as a long-term control.
5. Any other significant ocular and non-ocular disease/disorder or retinal surgery which,
in the opinion of the Investigator, may either put the participants at risk because of
participation in the study, or may influence the results of the study, or the
participant's ability to participate in the study. This would include not taking or
having a contraindication to oral prednisolone, such as a history of gastric ulcer or
significant side effects.
6. Participants who have participated in another research study involving an
investigational product in the past 12 weeks, or having had gene or cellular therapy at
any time prior to this study.
7. Patients with amblyopic eyes should be excluded in general, since the evaluation of the
primary endpoint presupposes the ability to fixate both eyes
8. Prior intraocular surgery within six months
9. Intolerance to local anesthesia and/or contraindication to IVT surgery (anemia Hb<8g/dl,
severe cardiovascular disease, severe coagulopathy, etc.)
10. High fever or high fever disease, patients with a history of autoimmune conditions/
other systemic diseases that may have ocular manifestations (e.g. sarcoidosis) or
neurodegenerative conditions (e.g. multiple sclerosis, neuromyelitis optica, Parkinson's
disease)
11. Patients suffering from other genetic mutations leading to pathological retinal
conditions
12. Patients treated by oral corticoids within 14 days prior inclusion at the study entry
Patient number: 6
Treatment: Each participant will receive a single treatment of the rAAV2.REP1 vector (0.1ml
containing 1011 AAV2 genome particles) administered by subretinal injection during a
vitrectomy operation. No placebo will be used. ln order to minimize selection bias both eyes
are randomized to either treatment or control.
Main criteria: Primary endpoint: Change from baseline in best corrected visual acuity in
treated eye, compared to untreated control eye up to 24 months after vector administration
Secondary endpoints: Absence of vector related adverse reactions 24 months after vector
administration. Demonstration of improved retinal anatomy and/or visual function other than
best corrected visual acuity in treated eye compared to the untreated control eye 24 months
after vector administration.
Statistical methods:
Summary statistics will be presented for both eyes (Treated Eye versus Control Eye groups).
No formal statistical comparison will be performed (no p-value will be computed). For
categorical/binary data, the number and proportion of patients in each category will be
presented with its 95% Confidence Interval (CI). For continuous data, mean (and its 95% CI)
and Standard Deviation (SD) will be presented.
The primary outcome measure will be the proportion of patients with a relative change from
baseline of > 5 in ETDRS letters (treated vs. untreated eye, change from BL). At each time
point, the change from baseline in ETDRS letters will be computed for each eye. The mean
change from baseline in ETDRS letters will be presented for both the treated eye and the
control eye groups.
At each time point, the change from baseline and the percentage change from baseline in the
area of autofluoresence will be computed for each eye and their mean will be presented for
both the treated eye and the control eye groups.
With regards to microperimetry, at each time point, the change from baseline in mean
sensitivity will be computed for each eye. The mean change from baseline in mean sensitivity
will be presented for both the treated eye and the control eye groups.
Adverse events will be listed. Other Investigator Sponsored Studies are expected to be run
with a similar protocol for the same indication and with the same intervention. A
meta-analysis on the Investigator Sponsored studies is planned. A separate Statistical
Analysis Plan describing the details of the meta-analysis will be developed.
Timetable:
Planned trial period: 24 month Follow-up duration: 36 month
The end of trial is the date on which the last treated patient completes the tests of their
planned close-out visit.
