For Immediate Release DIMERIX ANNOUNCES POSITIVE TOP-LINE RESULTS IN PHASE 2a CLINICAL STUDY OF DMX-200 IN FSGS Highlights • Primary and secondary endpoints met in the Phase 2a study of DMX-200 in FSGS patients • DMX-200 was found to be generally safe and well-tolerated in FSGS patients • 86% of patients demonstrated a reduction of proteinuria with DMX-200 versus placebo • A 29% reduction in proteinuria was observed across all patients receiving DMX-200 compared to placebo • 29% of patients achieved a >40% reduction in proteinuria on DMX-200 compared to placebo • Multiple patients from both FSGS and diabetic kidney disease studies continue on DMX-200 via TGA Special Access Scheme • Statistically powered Phase 2 study in diabetic kidney disease results due in 4 - 6 weeks MELBOURNE, Australia, 29 July 2020: Dimerix Limited (ASX: DXB), a clinical-stage drug development company, today announced positive top-line results from the Phase 2a ACTION study of DMX-200 for the treatment of focal segmental glomerulosclerosis (FSGS), a rare kidney disorder without an approved pharmacologic treatment that often leads to end-stage kidney failure. The study administered 240mg of oral DMX-200 to patients with FSGS already taking a stable 300 mg dose of the angiotensin receptor blocker irbesartan. The 240mg daily dose was administered as a 120mg capsule twice daily, which is an improved, more convenient transition from an 80mg capsule administered three times a day in the previous Phase 2a study in patients with chronic kidney disease. Teleconference at 11:00 (AEST) Wednesday 29 July Conference ID: 10009009 Pre‐registration: https://s1.c-conf.com/diamondpass/10009009-invite.html Dial‐in directly (toll free) Australia: 1800 455 963 (For more dial in options see the bottom of the release) Ten patients were enrolled in the study, with seven patients meeting all pre-defined criteria required for inclusion in the final analysis in accordance with the protocol. The primary endpoint for the study was safety, as measured by the number and severity of adverse events and clinically significant changes in the patient safety profile with the use of DMX-200 compared to placebo in participants with FSGS who are receiving irbesartan. The preliminary safety findings show DMX-200 was generally safe and well-tolerated, with no variation in the incidence or severity of adverse events between treatment with DMX-200 or placebo. There were no patient withdrawals from the study and there were no serious adverse events related to the drug reported. The secondary endpoints were the proportion of patients who achieved a response during treatment with DMX-200 compared to placebo as well as the percent change from baseline in 24-hour proteinuria after 16 weeks of treatment with DMX-200 as compared to placebo. Importantly, 86% (6/7) of patients demonstrated a reduction in proteinuria on treatment versus placebo, with an average 29% change from baseline in 24-hour proteinuria compared to placebo following treatment with DMX-200 based on protein/creatinine ratio (PCR) grouped analysis (an average reduction of 119mg/mmol (1052mg/g) proteinuria on DMX-200 versus an average reduction of 1mg/mmol (8.84mg/g) proteinuria on placebo). Furthermore, 29% (2/7) of the patients achieved a >40% reduction in proteinuria during treatment with DMX-200 compared to placebo. Unlike other investigational drugs currently in development for FSGS, patients stayed on the standard of care angiotensin receptor blockade. As a result, the reduction in proteinuria observed from DMX200 is in addition to any reduction in proteinuria expected from background therapy that would have occurred prior to starting on DMX-200. The Phase 2a study was a double-blind, randomised, placebo-controlled, crossover study designed to evaluate the safety and preliminary signs of efficacy of DMX-200 in patients with FSGS who are receiving a stable dose of standard of care, irbesartan. Patients must have been receiving irbesartan for at least 12 weeks prior to being included in the trial. As previously announced, each participant in the study received 16 weeks DMX-200 preceded or followed by 16 weeks placebo, separated by a 6-week washout period. Whilst this initial Phase 2a study in patients with FSGS was of a short duration and was not powered for statistical significance, it was designed to derive maximum insight from a small number of patients, while retaining the ability for a flexible number of patients to complete the study. As such, the study delivered encouraging data, which supports further development of DMX-200 in FSGS. “I believe that the results of this Phase 2a FSGS study, together with the positive outcomes of the Company’s prior Phase 2a study in Chronic Kidney Disease, further validates Dimerix’ lead candidate, DMX-200, in sclerotic kidney diseases. The positive signals suggest that treatment with DMX-200 may indeed result in clinically meaningful improvements in kidney function when added to the standard of care in patients with FSGS. To have 86% of patients see a benefit on DMX-200 versus placebo in a disease is very impressive. I am very excited at what this may mean for future studies in patients with FSGS," commented Dr Hiddo Heerspink, Chair of the Dimerix Medical Advisory Board. Investigator on the study and Head of the Melbourne Renal Research Group, Associate Professor David Packham, commented “These are tremendous top line results and certainly very encouraging for all FSGS sufferers. I look forward to further analysis over the next several weeks, which I expect will equally be fascinating and informative.” "We are very pleased with the top-line results from the study, which suggest DMX-200 could be a significant advancement in the treatment of FSGS," said Dr Nina Webster, CEO and Managing Director of Dimerix. "FSGS patients today face poor outcomes with limited medical options, and we continue to progress our proposed development pathway forward that could deliver the first approved pharmacologic treatment to the FSGS community. In the meantime, we will soon be reporting on the larger diabetic kidney disease Phase 2 study that we hope will further support the growing evidence of DMX-200 efficacy in treating kidney diseases." It is anticipated that additional analyses of these FSGS data will be available in due course, following availability of additional data and review by the Medical Advisory Board. In the meantime, multiple patients from both the FSGS and the diabetic kidney disease study continue on treatment with DMX-200 through the TGA’s Special Access Scheme following respective study completion. Dimerix has received Orphan Drug Designation for DMX-200 in both the US and Europe for the treatment of FSGS. Dimerix established with the respective regulatory agencies that “the intention to treat FSGS with DMX-200 was justified based on preliminary non-clinical data which showed a reduction in the number of podocytes lost and an improvement in proteinuria.” Furthermore, as stated by the respective regulatory agencies, the orphan designation indicates that “Dimerix has provided sufficient justification that if approved, [DMX-200] is likely to be of significant benefit to those affected by the condition” and that “[DMX-200] would provide a clinically relevant advantage as an alternative to any currently marketed products”. Orphan designation also provides regulatory and financial benefits to help bring DMX-200 to market in the US and Europe faster, including reduced fees during the product development phase, protocol assistance from the regulatory authorities, and 7-year (US) and 10-year (Europe) market exclusivity following product approval. Dimerix is also awaiting the Phase 2 study results in diabetic kidney disease, which completed dosing in late July and has an expected data read-out in 4 - 6 weeks. In addition to the ongoing Phase 2 diabetic kidney disease study, the study in patients with COVID-19, and DMX-700 in Chronic Obstructive Pulmonary Disease, Dimerix continues to undertake planning for its proposed global Phase 3 pivotal program in FSGS. For further information, please visit our website at www.dimerix.com or contact: Dr Nina Webster, Dimerix Limited Chief Executive Officer & Managing Director Tel: +61 1300 813 321 E: [email protected] Rudi Michelson Monsoon Communications Tel: +61 3 9620 3333 Mob: +61 (0)411 402 737 Conference call details • Time: 11:00 (AEST) Wednesday 29 July • Conference ID: 10009009 Access the call by pre-registration (preferred option) or by direct dial-in (delays possible): 1. Pre‐registration Participants can pre‐register by navigating to: https://s1.c-conf.com/diamondpass/10009009-invite.html Registered participants will receive their dial in number upon registration to enter the call automatically on the day. 2. Dial‐in directly (toll free) Australia: 1800 455 963 Japan: 0066 3386 8000 Sydney: 02 9007 8048 Malaysia: 1800 816 441 New Zealand: 0800 452 795 Singapore: 800 101 2702 China: 10800 140 1776 South Africa: 0800 984 013 France: 0800 913 734 Spain: 900 823 322 Germany: 0800 183 0918 Switzerland: 0800 802 498 Hong Kong: 800 968 273 Taiwan: 0080 112 7377 India: 0008 0010 08070 UAE: 8000 3570 2706 Indonesia: 007 803 321 8057 UK: 0800 051 1453 Ireland: 1800 948 607 USA/Canada 1 855 624 0077 Other International (metered): +61 7 3145 4005 Authorised for lodgement by the Board of the Company
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