The orphan drug for Acanthamoeba keratitis (ODAK) trial: PHMB 0.08% (polihexanide) and placebo versus PHMB 0.02% and propamidine 0.1%
The orphan drug for Acanthamoeba keratitis (ODAK) trial: PHMB 0.08% (polihexanide) and placebo versus PHMB 0.02% and propamidine 0.1%
Purpose: to compare topical PHMB (polihexanide) 0.02% (0.2 mg/ml)+ propamidine 0.1% (1 mg/ml) with PHMB 0.08% (0.8 mg/ml)+ placebo (PHMB 0.08%) for Acanthamoeba keratitis (AK) treatment.
Design: prospective, randomized, double-masked, active-controlled, multicenter phase 3 study (ClinicalTrials.gov identifier, NCT03274895).
Participants: one hundred thirty-five patients treated at 6 European centers.
Methods: principal inclusion criteria were 12 years of age or older and in vivo confocal microscopy with clinical findings consistent with AK. Also included were participants with concurrent bacterial keratitis who were using topical steroids and antiviral and antifungal drugs before randomization. Principal exclusion criteria were concurrent herpes or fungal keratitis and use of antiamebic therapy (AAT). Patients were randomized 1:1 using a computer-generated block size of 4. This was a superiority trial having a predefined noninferiority margin. The sample size of 130 participants gave approximately 80% power to detect 20-percentage point superiority for PHMB 0.08% for the primary outcome of the medical cure rate (MCR; without surgery or change of AAT) within 12 months, cure defined by clinical criteria 90 days after discontinuing anti-inflammatory agents and AAT. A prespecified multivariable analysis adjusted for baseline imbalances in risk factors affecting outcomes.
Main outcome measures: the main outcome measure was MCR within 12 months, with secondary outcomes including best-corrected visual acuity and treatment failure rates. Safety outcomes included adverse event rates.
Results: one hundred thirty-five participants were randomized, providing 127 in the full-analysis subset (61 receiving PHMB 0.02%+ propamidine and 66 receiving PHMB 0.08%) and 134 in the safety analysis subset. The adjusted MCR within 12 months was 86.6% (unadjusted, 88.5%) for PHMB 0.02%+ propamidine and 86.7% (unadjusted, 84.9%) for PHMB 0.08%; the noninferiority requirement for PHMB 0.08% was met (adjusted difference, 0.1 percentage points; lower one-sided 95% confidence limit, -8.3 percentage points). Secondary outcomes were similar for both treatments and were not analyzed statistically: median best-corrected visual acuity of 20/20 and an overall treatment failure rate of 17 of 127 patients (13.4%), of whom 8 of 127 patients (6.3%) required therapeutic keratoplasty. No serious drug-related adverse events occurred.
Conclusions: PHMB 0.08% monotherapy may be as effective (or at worse only 8 percentage points less effective) as dual therapy with PHMB 0.02%+ propamidine (a widely used therapy) with medical cure rates of more than 86%, when used with the trial treatment delivery protocol in populations with AK with similar disease severity.
Financial disclosure(s): proprietary or commercial disclosure may be found in the Footnotes and Disclosures at the end of this article.
acanthamoeba, keratitis, Acanthamoeba keratitis, treatment trial outcomes
Dart, John K.G.
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Papa, Vincenzo
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Rama, Paolo
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Knutsson, Karl Anders
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Ahmad, Saj
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Hau, Scott
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Sanchez, Sara
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Franch, Antonella
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Birattari, Federica
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Leon, Pia
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Fasolo, Adriano
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Kominek, Ewa Mrukwa
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Jadczyk-Sorek, Katarzyna
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Carley, Fiona
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Hossain, Parwez
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Minassian, Darwin C.
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Dart, John K.G.
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Papa, Vincenzo
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Rama, Paolo
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Knutsson, Karl Anders
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Ahmad, Saj
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Hau, Scott
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Sanchez, Sara
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Franch, Antonella
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Birattari, Federica
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Leon, Pia
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Fasolo, Adriano
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Kominek, Ewa Mrukwa
a7069cc1-c1eb-4fa4-9355-707d046c454b
Jadczyk-Sorek, Katarzyna
88982015-4204-4064-acff-56afef3b5f7f
Carley, Fiona
fe19703d-9b0e-4da8-8287-233d0c158ef1
Hossain, Parwez
563de5fc-84ad-4539-9228-bde0237eaf51
Minassian, Darwin C.
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Dart, John K.G., Papa, Vincenzo, Rama, Paolo, Knutsson, Karl Anders, Ahmad, Saj, Hau, Scott, Sanchez, Sara, Franch, Antonella, Birattari, Federica, Leon, Pia, Fasolo, Adriano, Kominek, Ewa Mrukwa, Jadczyk-Sorek, Katarzyna, Carley, Fiona, Hossain, Parwez and Minassian, Darwin C.
(2023)
The orphan drug for Acanthamoeba keratitis (ODAK) trial: PHMB 0.08% (polihexanide) and placebo versus PHMB 0.02% and propamidine 0.1%.
Ophthalmology.
(doi:10.1016/j.ophtha.2023.09.031).
Abstract
Purpose: to compare topical PHMB (polihexanide) 0.02% (0.2 mg/ml)+ propamidine 0.1% (1 mg/ml) with PHMB 0.08% (0.8 mg/ml)+ placebo (PHMB 0.08%) for Acanthamoeba keratitis (AK) treatment.
Design: prospective, randomized, double-masked, active-controlled, multicenter phase 3 study (ClinicalTrials.gov identifier, NCT03274895).
Participants: one hundred thirty-five patients treated at 6 European centers.
Methods: principal inclusion criteria were 12 years of age or older and in vivo confocal microscopy with clinical findings consistent with AK. Also included were participants with concurrent bacterial keratitis who were using topical steroids and antiviral and antifungal drugs before randomization. Principal exclusion criteria were concurrent herpes or fungal keratitis and use of antiamebic therapy (AAT). Patients were randomized 1:1 using a computer-generated block size of 4. This was a superiority trial having a predefined noninferiority margin. The sample size of 130 participants gave approximately 80% power to detect 20-percentage point superiority for PHMB 0.08% for the primary outcome of the medical cure rate (MCR; without surgery or change of AAT) within 12 months, cure defined by clinical criteria 90 days after discontinuing anti-inflammatory agents and AAT. A prespecified multivariable analysis adjusted for baseline imbalances in risk factors affecting outcomes.
Main outcome measures: the main outcome measure was MCR within 12 months, with secondary outcomes including best-corrected visual acuity and treatment failure rates. Safety outcomes included adverse event rates.
Results: one hundred thirty-five participants were randomized, providing 127 in the full-analysis subset (61 receiving PHMB 0.02%+ propamidine and 66 receiving PHMB 0.08%) and 134 in the safety analysis subset. The adjusted MCR within 12 months was 86.6% (unadjusted, 88.5%) for PHMB 0.02%+ propamidine and 86.7% (unadjusted, 84.9%) for PHMB 0.08%; the noninferiority requirement for PHMB 0.08% was met (adjusted difference, 0.1 percentage points; lower one-sided 95% confidence limit, -8.3 percentage points). Secondary outcomes were similar for both treatments and were not analyzed statistically: median best-corrected visual acuity of 20/20 and an overall treatment failure rate of 17 of 127 patients (13.4%), of whom 8 of 127 patients (6.3%) required therapeutic keratoplasty. No serious drug-related adverse events occurred.
Conclusions: PHMB 0.08% monotherapy may be as effective (or at worse only 8 percentage points less effective) as dual therapy with PHMB 0.02%+ propamidine (a widely used therapy) with medical cure rates of more than 86%, when used with the trial treatment delivery protocol in populations with AK with similar disease severity.
Financial disclosure(s): proprietary or commercial disclosure may be found in the Footnotes and Disclosures at the end of this article.
Text
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More information
Accepted/In Press date: 27 September 2023
e-pub ahead of print date: 5 October 2023
Additional Information:
Funding Information:
Funding support by SIFI S.p.A., Aci S.Antonio, Italy; European Union (EU grant: FP7-HEALTH-2012-INNOVATION-1 Proposal No: 305661-2); and the National Institute of Research Biomedical Research Centre at Moorfields Eye Hospital and the UCL Institute of Ophthalmology, London, United Kingdom (J.K.G.D.).
Funding Information:
Obtained funding: N/A; The study was perfomed as part of regular employment duties (Employer's research funding from SIFI S.p.A. with part funding from EU Grant FP7-HEALTH-2012-INNOVATION-1 Proposal No: 305661-2 Orphan Drug for Acanthamoeba keratitis [ODAK; 2012-2017]).
Publisher Copyright:
© 2023 American Academy of Ophthalmology
Keywords:
acanthamoeba, keratitis, Acanthamoeba keratitis, treatment trial outcomes
Identifiers
Local EPrints ID: 484817
URI: http://eprints.soton.ac.uk/id/eprint/484817
ISSN: 0161-6420
PURE UUID: 7cf10f8f-271b-433e-b53f-fdcc3771c9b9
Catalogue record
Date deposited: 22 Nov 2023 17:35
Last modified: 18 Mar 2024 03:02
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Contributors
Author:
John K.G. Dart
Author:
Vincenzo Papa
Author:
Paolo Rama
Author:
Karl Anders Knutsson
Author:
Saj Ahmad
Author:
Scott Hau
Author:
Sara Sanchez
Author:
Antonella Franch
Author:
Federica Birattari
Author:
Pia Leon
Author:
Adriano Fasolo
Author:
Ewa Mrukwa Kominek
Author:
Katarzyna Jadczyk-Sorek
Author:
Fiona Carley
Author:
Darwin C. Minassian
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