Retinal Disease Clinical Trial
Official title:
Phase II, Randomized, Placebo-Controlled Study for the Evaluation of Finasteride in the Treatment of Chronic Central Serous Chorioretinopathy
Background:
- Central serous chorioretinopathy (CSC) is a disease that causes fluid to collect under
the retina. It affects the macula, which is in the center of the retina and is needed
for sharp, clear vision. In many cases, CSC resolves on its own and does not need
treatment. However, in some cases it does not go away or comes back after treatment.
This is known as chronic CSC.
- Chronic CSC may be caused by hormones called androgens. Finasteride is a drug that can
alter the effects certain of androgens. Researchers want to compare finasteride with a
placebo to see if it is a safe and effective treatment for chronic CSC.
Objectives:
- To see if finasteride is a safe and effective treatment for chronic CSC.
Eligibility:
- Individuals at least 18 years of age who have chronic CSC in one or both eyes.
Design:
- Participants will be screened with a physical exam and medical history. A full eye exam
will be performed. Blood and urine samples will also be collected.
- Some participants may have photodynamic therapy (PDT), the standard treatment for CSC.
PDT helps to reduce the amount of fluid in the eye. Participants will need to wait for
3 months after PDT before starting the finasteride study.
- Participants will be separated into two groups. One group will take finasteride 5 mg
(formulated into capsules); the other group will take a placebo capsule. All
participants will take the capsules for 3 months.
- After 3 months on the assigned capsule (finasteride or placebo), all participants will
have the opportunity to take finasteride for at least another 4 years and 9 months.
This phase of the study is optional.
- Participants will have regular study visits. At each visit, they will have physical
exams and eye exams. They will also provide blood and urine samples.
- During the first 3 months, participants will have 2 study visits. After 3 months, if
the participant continues in the optional (or as needed) phase of the protocol, visits
will occur at Month 6, Month 12 and every 12 months thereafter. However, additional
visits may be needed.
Objective:
Central serous chorioretinopathy (CSC) is a chorioretinal disorder characterized by an
accumulation of serous fluid under the retina. Although acute CSC tends to resolve
spontaneously on its own with minimal sequelae, chronic CSC tends to persist and lead to
irreversible visual loss. The pathogenesis of CSC is complex. However, systemic androgens
have been implicated. Finasteride is an anti-androgen medication that is widely used in the
treatment of various conditions. A previous study performed at the NEI demonstrated a
reduction in the amount of subretinal fluid among participants treated with 5 mg of
finasteride. The objective of this study is to further investigate the efficacy of oral
finasteride as a treatment for chronic CSC.
Study Population:
Thirty-eight participants with chronic CSC are eligible. Up to an additional four
participants may be enrolled to account for participants who withdraw from the study prior
to Month 3.
Design:
In this Phase II, single-center, placebo-controlled, double-masked, randomized trial,
investigational product will be administered to two different groups. Half of the
participants will be randomized to 5 mg oral finasteride for the initial three months. The
other half of the participants will be randomized to placebo for the first three months. At
the end of three months of treatment, all participants may be followed for at least four
years and nine months. During this follow-up period, all participants will be able to
receive finasteride therapy pro re nata (PRN) if subretinal fluid re-emerges. The PRN phase
will last until the last participant completes the five years of follow-up. Other standard
care treatments, such as photodynamic therapy, will also be permitted after the primary
outcome at three months.
Outcome Measures:
The primary outcome for regulatory filing is the proportion of participants with an
improvement in best-corrected visual acuity (BCVA) ≥ 15 letters at three months compared to
baseline in the study eye. The primary outcome for publication of the study results is the
proportion of participants with a subretinal fluid volume decrease ≥ 50% at three months
compared to baseline in the study eye. Secondary efficacy outcomes include changes in BCVA,
changes in the maximum retinal volume as measured on optical coherence tomography (OCT),
changes in central retinal thickness on OCT, changes in leakage as seen on fluorescein
angiography (FA), changes in size of existing plaque(s) on indocyanine green (ICG)
angiography, changes in autofluorescence patterns seen on fundus autofluorescence (FAF)
imaging, changes in mean macular sensitivity as assessed by microperimetry, changes in serum
levels of testosterone and dihydrotestosterone (DHT), as well as changes in urine levels of
cortisol during the study period. Safety outcomes include the number and severity of adverse
reactions from the investigational product and the number of withdrawals.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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