A recently published clinical trial report reviewing the first completed Phase III study in the ODYSSEY development program has shown that alirocumab showed significantly better LDL-C lowering than ezetimibe, with a comparable safety profile to ezetimibe. [1]
The report, which is published in the January issue of Future Cardiology, provides a comprehensive overview of the ODYSSEY MONO trial, including detail on the study design, data analysis, results and discussion on the implications of the findings, authored by lead investigator of the trial Eli M Roth.
LDL-cholesterol (LDL-C) is considered to be a major modifiable risk factor for the development of atherosclerosis and cardiovascular disease (CVD), the leading cause of death worldwide. LDL-C is identified as the primary target of cholesterol-lowering therapy in both North American and European guidelines. Statins are the recommended first-line therapy for lowering LDL-C.
Alirocumab (formerly SAR236553/REGN727) is a fully human mAb to PCSK9 - the first in this class of drugs to complete a Phase III trial, and reported to have a significant role in the regulation of LDL-C - being developed jointly by Sanofi (France) and Regeneron (NY, USA).
This first completed Phase III study, entitled ODYSSEY MONO, tested the new lower 75-mg dose of alirocumab subcutaneously every 2 weeks as a monotherapy versus ezetimibe 10 mg per os every day as a control. Inclusion criteria included patients with an LDL-C between 100 mg/dl (?2.6 mmol/l) and 190 mg/dl (<4.9 mmol/l; inclusive) and not on LLT. In addition, patients needed to have moderate CV risk defined as a 10-year risk of fatal CV events ?1% and <5% based on the European Systematic Coronary Risk Estimation (SCORE).
These data from the study suggest that the 75-mg dose of alirocumab subcutaneously every 2 weeks may be appropriate for adequate lowering of LDL-C in a large portion of patients with primary hypercholesterolemia at moderate CV risk who are not receiving statin therapy.
The safety parameters, adverse events and study discontinuation rates were similar between both treatment arms.
"Since ODYSSEY MONO, we have seen several phase III trials that have confirmed the ability of alirocumab to lower LDL-C in moderate to high risk cardiovascular patients," said Eli M. Roth Medical Director, Sterling Research Group & Professor of Clinical Medicine University of Cincinnati, and lead author of the article published in Future Cardiology. "These completed trials show that PCSK9 inhibitors are proving to be effective in different patient populations."
Sean Fitzpatrick, Commissioning Editor of Future Cardiology, commented: "Following the presentation of Sanofi/Regeneron's positive top-line results at the end of 2014, we feel it is important for our readers to have a comprehensive, accessible overview of this important topic. The review article helps in providing context for clinicians and researchers framing the results in terms of the current state of the art in lipid-lowering therapy."
###
[1] Roth EM, McKenney JM. ODYSSEY MONO: effect of alirocumab 75 mg subcutaneously every 2 weeks as monotherapy versus ezetimibe over 24 weeks. Future Cardiol 2015; 11(1): 27-37
About Future Cardiology
Future Cardiology reflects a new era of cardiology and highlights the new molecular approach to advancing cardiovascular therapy. Coverage also reflects the major technological advances in bioengineering in cardiology in terms of advanced and robust devices, miniaturization, imaging, system modeling and information management issues. The journal takes a new approach to the way information is structured and delivered, so that its value is maximized to the reader.
Coverage includes:
- Molecular basis of cardiovascular disease
- Therapeutic overviews highlighting optimal therapy and future options
- Prevention in cardiovascular disease
- Summaries evaluating newly approved cardiovascular therapeutic agents
- Personalized medicine in cardiology
- Advanced device and imaging technologies
- Interventional and surgical approaches
- Psychosocial aspects of cardiovascular disease
- Epidemiological studies and trends
- New diagnostic approaches, screening and patient stratification
- Pharmacoeconomic and outcomes issues in cardiology
About Future Science Group
Founded in 2001, Future Science Group (FSG) is a progressive publisher focused on breakthrough medical, biotechnological, and scientific research. FSG's portfolio includes two imprints, Future Science and Future Medicine. Both publish eBooks and journals.
In addition to this core publishing business FSG develops specialist eCommunities. Key titles and sites include Bioanalysis Zone, Epigenomics, Nanomedicine and the award-winning Regenerative Medicine.
The aim of FSG is to service the advancement of clinical practice and drug research by enhancing the efficiency of communications among clinicians, researchers and decision-makers, and by providing innovative solutions to their information needs. This is achieved through a customer-centric approach, use of new technologies, products that deliver value-for-money and uncompromisingly high standards. http://www.futuresciencegroup.com
Journal
Future Cardiology