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Eplerenone versus placebo for chronic central serous chorioretinopathy: the VICI RCT

Eplerenone versus placebo for chronic central serous chorioretinopathy: the VICI RCT
Eplerenone versus placebo for chronic central serous chorioretinopathy: the VICI RCT
Background: in chronic central serous chorioretinopathy, fluid accumulates in the subretinal space and causes permanent vision loss in $\approx$ 30{\%} of patients. There is no definitive treatment. Previous research suggests that the mineralocorticoid receptor antagonist eplerenone is effective but it is not licensed for chronic central serous chorioretinopathy.

Objectives: the objective was to evaluate whether or not eplerenone was safe and superior to placebo for treating chronic central serous chorioretinopathy. We also aimed to set up a biobank of DNA, serum and plasma samples from treatment-naive participants for future research. DESIGN: The trial was a parallel, randomised (1 : 1 ratio), multicentre, double-masked, placebo-controlled superiority trial comparing eplerenone plus usual care with placebo plus usual care. Participants were randomly allocated to eplerenone or placebo using a secure online system that returned a unique number corresponding to a bottle of the investigational medicinal product. Participants, clinical care teams, pharmacists, outcome assessors and the trial management group were masked. SETTING: The trial took place in 22 NHS hospitals in the UK. PARTICIPANTS: Eligible participants were patients aged 18--60 years with treatment-naive chronic central serous chorioretinopathy of at least 4 months' duration, a best corrected visual acuity score of 54--85 letters and no other conditions affecting visual acuity or contraindications to taking eplerenone or placebo.

Interventions: the intervention was oral eplerenone (25 mg/day for 1 week, increased to 50 mg/day for up to 12 months). Placebo was a lactose-filled capsule that appeared identical to the overencapsulated eplerenone tablets. To maintain blinding, participants in the placebo group followed the same dose escalation schedule as the eplerenone group. Usual care was included in both groups and was administered at the discretion of clinicians.

Main outcome measures: the primary outcome was best corrected visual acuity score at 12 months. Secondary outcomes were low-luminance visual acuity, central subfield retinal thickness, change in subretinal fluid thickness, systemic and ocular adverse events, macular atrophy of the retinal pigment epithelium, subfoveal choroidal thickness, choroidal permeability, resolution of subretinal fluid, time to recurrence of subretinal fluid, fundus fluorescein angiography phenotype, incidence of chronic central serous chorioretinopathy in the fellow eye, and patient-reported visual function. RESULTS: Between 11 January 2017 and 22 February 2018, 57 participants were randomised to eplerenone and 57 to placebo; 57 and 54 participants, respectively, were included in the analysis of the primary outcome. The modelled mean best corrected visual acuity score at 12 months in the eplerenone and placebo groups was 80.4 letters (standard deviation 4.6 letters) and 79.5 letters (standard deviation 4.5 letters), with an estimated difference between groups of 1.73 letters (95{\%} confidence interval --1.12 to 4.57 letters; p = 0.24). Hyperkalaemia occurred in eight participants in each group (14{\%}). No serious adverse events occurred in the eplerenone group; three unrelated serious adverse events occurred in the placebo group.

Limitations: limitations included the inability to prevent co-treatments and discontinuation of the investigational medicinal product in the event of resolution or hyperkalaemia.

Conclusions: eplerenone was safe but not superior to placebo in improving best corrected visual acuity in people with chronic central serous chorioretinopathy during 12 months of follow-up. In future work, ophthalmologists should investigate alternative treatments for this condition, which remains complicated to treat. TRIAL REGISTRATION: Current Controlled Trials ISRCTN92746680.
2050-4365
Lotery, Andrew
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Sivaprasad, Sobha
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O’Connell, Abby
978563ec-2791-42b0-b237-ecc198d2c479
Harris, Rosie A.
9a046171-b0f7-4a20-a0b9-13c4ac92d4c9
Culliford, Lucy
2ebe9e38-51e1-4390-985a-3519410f3856
Cree, Angela
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Madhusudhan, Savita
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Griffiths, Helen
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Ellis, Lucy
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Chakravarthy, Usha
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Peto, Tunde
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Rogers, Chris A.
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Reeves, Barnaby C.
3d10eab6-24a5-41c7-8ecc-8b5ace0f25ff
Lotery, Andrew
5ecc2d2d-d0b4-468f-ad2c-df7156f8e514
Sivaprasad, Sobha
6ae3de79-66b3-4fc5-a91d-7de5f5887038
O’Connell, Abby
978563ec-2791-42b0-b237-ecc198d2c479
Harris, Rosie A.
9a046171-b0f7-4a20-a0b9-13c4ac92d4c9
Culliford, Lucy
2ebe9e38-51e1-4390-985a-3519410f3856
Cree, Angela
6724b71b-8828-4abb-971f-0856c2af555e
Madhusudhan, Savita
d4ba51be-8292-4ce6-9953-503c1a6e5e3c
Griffiths, Helen
a097fdaa-d3d6-49a9-9c69-0e6e5a5d518b
Ellis, Lucy
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Chakravarthy, Usha
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Peto, Tunde
e5511bbd-2ef8-4465-a2b3-46c8cc3ce63e
Rogers, Chris A.
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Reeves, Barnaby C.
3d10eab6-24a5-41c7-8ecc-8b5ace0f25ff

Lotery, Andrew, Sivaprasad, Sobha, O’Connell, Abby, Harris, Rosie A., Culliford, Lucy, Cree, Angela, Madhusudhan, Savita, Griffiths, Helen, Ellis, Lucy, Chakravarthy, Usha, Peto, Tunde, Rogers, Chris A. and Reeves, Barnaby C. (2021) Eplerenone versus placebo for chronic central serous chorioretinopathy: the VICI RCT. Efficacy and Mechanism Evaluation, 8 (2). (doi:10.3310/eme08020).

Record type: Article

Abstract

Background: in chronic central serous chorioretinopathy, fluid accumulates in the subretinal space and causes permanent vision loss in $\approx$ 30{\%} of patients. There is no definitive treatment. Previous research suggests that the mineralocorticoid receptor antagonist eplerenone is effective but it is not licensed for chronic central serous chorioretinopathy.

Objectives: the objective was to evaluate whether or not eplerenone was safe and superior to placebo for treating chronic central serous chorioretinopathy. We also aimed to set up a biobank of DNA, serum and plasma samples from treatment-naive participants for future research. DESIGN: The trial was a parallel, randomised (1 : 1 ratio), multicentre, double-masked, placebo-controlled superiority trial comparing eplerenone plus usual care with placebo plus usual care. Participants were randomly allocated to eplerenone or placebo using a secure online system that returned a unique number corresponding to a bottle of the investigational medicinal product. Participants, clinical care teams, pharmacists, outcome assessors and the trial management group were masked. SETTING: The trial took place in 22 NHS hospitals in the UK. PARTICIPANTS: Eligible participants were patients aged 18--60 years with treatment-naive chronic central serous chorioretinopathy of at least 4 months' duration, a best corrected visual acuity score of 54--85 letters and no other conditions affecting visual acuity or contraindications to taking eplerenone or placebo.

Interventions: the intervention was oral eplerenone (25 mg/day for 1 week, increased to 50 mg/day for up to 12 months). Placebo was a lactose-filled capsule that appeared identical to the overencapsulated eplerenone tablets. To maintain blinding, participants in the placebo group followed the same dose escalation schedule as the eplerenone group. Usual care was included in both groups and was administered at the discretion of clinicians.

Main outcome measures: the primary outcome was best corrected visual acuity score at 12 months. Secondary outcomes were low-luminance visual acuity, central subfield retinal thickness, change in subretinal fluid thickness, systemic and ocular adverse events, macular atrophy of the retinal pigment epithelium, subfoveal choroidal thickness, choroidal permeability, resolution of subretinal fluid, time to recurrence of subretinal fluid, fundus fluorescein angiography phenotype, incidence of chronic central serous chorioretinopathy in the fellow eye, and patient-reported visual function. RESULTS: Between 11 January 2017 and 22 February 2018, 57 participants were randomised to eplerenone and 57 to placebo; 57 and 54 participants, respectively, were included in the analysis of the primary outcome. The modelled mean best corrected visual acuity score at 12 months in the eplerenone and placebo groups was 80.4 letters (standard deviation 4.6 letters) and 79.5 letters (standard deviation 4.5 letters), with an estimated difference between groups of 1.73 letters (95{\%} confidence interval --1.12 to 4.57 letters; p = 0.24). Hyperkalaemia occurred in eight participants in each group (14{\%}). No serious adverse events occurred in the eplerenone group; three unrelated serious adverse events occurred in the placebo group.

Limitations: limitations included the inability to prevent co-treatments and discontinuation of the investigational medicinal product in the event of resolution or hyperkalaemia.

Conclusions: eplerenone was safe but not superior to placebo in improving best corrected visual acuity in people with chronic central serous chorioretinopathy during 12 months of follow-up. In future work, ophthalmologists should investigate alternative treatments for this condition, which remains complicated to treat. TRIAL REGISTRATION: Current Controlled Trials ISRCTN92746680.

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Published date: 1 January 2021

Identifiers

Local EPrints ID: 493791
URI: http://eprints.soton.ac.uk/id/eprint/493791
ISSN: 2050-4365
PURE UUID: d0788935-c439-4f7f-80ea-e0f93ae8c4f2
ORCID for Andrew Lotery: ORCID iD orcid.org/0000-0001-5541-4305
ORCID for Angela Cree: ORCID iD orcid.org/0000-0002-1987-8900

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Date deposited: 12 Sep 2024 16:56
Last modified: 13 Sep 2024 01:40

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Contributors

Author: Andrew Lotery ORCID iD
Author: Sobha Sivaprasad
Author: Abby O’Connell
Author: Rosie A. Harris
Author: Lucy Culliford
Author: Angela Cree ORCID iD
Author: Savita Madhusudhan
Author: Helen Griffiths
Author: Lucy Ellis
Author: Usha Chakravarthy
Author: Tunde Peto
Author: Chris A. Rogers
Author: Barnaby C. Reeves

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