The Muscular Dystrophy Association (MDA) today celebrated the decision by the US Food and Drug Administration (FDA) to grant accelerated marketing approval to casimersen (Amondys 45) for the treatment of Duchenne muscular dystrophy (DMD) in patients amenable to skipping exon 45.
NEW YORK, Feb. 25, 2021 /PRNewswire/ -- The Muscular Dystrophy Association (MDA) today celebrated the decision by the US Food and Drug Administration (FDA) to grant accelerated marketing approval to casimersen (Amondys 45) for the treatment of Duchenne muscular dystrophy (DMD) in patients amenable to skipping exon 45. It is the fourth exon-skipping, disease-modifying drug to treat DMD, the most common childhood form of muscular dystrophy. Amondys 45 will be made available in the United States and marketed by Sarepta Therapeutics. In the last five years, three targeted exon-skipping drugs have been approved by the FDA to treat DMD: Exondys 51 and Vyondys 53 from Sarepta Therapeutics and Viltepso from NS Pharma. Exondys 51 was the first targeted therapy approved to treat DMD in a subset of patients with a genetic mutation amenable to skipping exon 51, while Vyondys 53 and Viltepso were approved in December 2019 and August 2020, respectively, to treat another subset of patients with a mutation amenable to skipping exon 53. Amondys 45 is designed to treat a third subset of patients with DMD, specifically those with a mutation amenable to skipping of exon 45. Approval of Amondys 45 represents another significant step forward in the development of therapies for DMD that target the root cause of the disease. “We celebrate the approval of Amondys 45, which represents the third exon-skipping drug from Sarepta, and the fifth drug approved for Duchenne muscular dystrophy,” says MDA’s Executive Vice President and Chief Research Officer Sharon Hesterlee, PhD. “MDA funded the development of this technology in the laboratory of Dr. Steve Wilton in the 1990’s and it’s very gratifying to see that technology being extended by Sarepta to benefit more and more Duchenne families.” DMD is caused by mutations in the dystrophin gene (DMD) on the X chromosome that result in little or no production of dystrophin, a protein essential to keeping muscle cells intact. Amondys 45 is called an “exon-skipping” drug in that it is designed to target and promote skipping over a section of genetic code in order to avoid the gene mutation and produce more of the dystrophin protein. It is estimated that up to 8% of patients with DMD have mutations amenable to treatment with Amondys 45. Although treatment with Amondys 45 will not cure DMD, it could slow progression of the disease, which, in turn, could extend the length of time individuals with DMD could walk, eat independently, and breathe without assistance. The FDA’s decision to approve Amondys 45 highlights the importance of years of commitment to supporting and funding breakthrough research by MDA and others into gene identification and unlocking the cause of DMD. MDA-supported research has been central to the development of the exon-skipping approach behind the currently approved therapies. MDA has funded foundational work upon which the strategy was built, as well as extensive research into the strategy over subsequent years. Laboratory development of exon-skipping therapies began in the 1990s, including the notable, MDA-funded work by Steve Wilton, PhD, and colleagues. Their work led to the invention of what would later become Exondys 51, Vyondys 53, Viltepso, and Amondys 45. Since its inception, MDA has committed more than $218 million to DMD and Becker muscular dystrophy research and more than $1 billion across the spectrum of neuromuscular diseases. While this may be the fourth exon-skipping therapy for treating DMD, the increasing pace of drug development holds immense promise for the future of all neuromuscular diseases. Of the now 14 approved therapies for treating neuromuscular diseases, 12 have been approved by the FDA in the past decade alone. Clinical trials support approval of Amondys 45 About SareptAssist MDA’s Resource Center provides support, guidance, and resources for patients and families, including information about the approval of Amondys 45, open clinical trials, and other services. Contact the MDA Resource Center at 1-833-ASK-MDA1 or ResourceCenter@mdausa.org. About DMD About Amondys 45 Just as individuals with DMD caused by a mutation that would be amenable to skipping exon 51 could benefit from treatment with Exondys 51, those with DMD caused by a mutation that would be impacted by skipping exon 45 potentially could benefit from treatment with Amondys 45. About the Muscular Dystrophy Association View original content to download multimedia:http://www.prnewswire.com/news-releases/mda-celebrates-fda-approval-of-amondys-45-for-treatment-of-dmd-amenable-to-exon-45-skipping-301236136.html SOURCE The Muscular Dystrophy Association |