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World Community Grid Forums
Category: Completed Research
Forum: Help Cure Muscular Dystrophy
Thread: Interesting News About Muscular Dystrophy Research |
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Thread Status: Active Total posts in this thread: 5
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MD-Crusher
Advanced Cruncher Joined: Jul 23, 2007 Post Count: 52 Status: Offline |
Muscular dystrophy trial to start
A gene therapy trial for the fatal disorder Duchene muscular dystrophy (DMD) is about to begin in London. In a world first, a small group of patients will be injected with an experimental drug which it is hoped will extend their lives. DMD, which affects boys, is caused by a single faulty gene, and results in progressive muscle wasting. |
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robertmiles
Senior Cruncher US Joined: Apr 16, 2008 Post Count: 445 Status: Offline Project Badges: 
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Former Member
Cruncher Joined: May 22, 2018 Post Count: 0 Status: Offline |
Is about to start in these days (late July 2008) a multicentric and transnational clinical trial on muscular dystrophy. This clinical trial is for the drug PTC 124 (PTC Therapeutics). It could be useful for the Point Mutation only causing Stop Codon called NONSENSE MUTATION
My son has a Point Mutation in Exon 14 of Dystrophin Gene, but we're still waiting to know if it is a NONSENSE MUTATION or a MISSENSE MUTATION. If it were a MISSENSE MUTATION this drug would not be able to correct the error in the dystrophin gene. |
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Sekerob
Ace Cruncher Joined: Jul 24, 2005 Post Count: 20043 Status: Offline |
This may hook into MD. There are some follow through links in the right margin:
----------------------------------------New hope for treating common form of inherited neuromuscular disease Treatments that ramp up production of the tiny "motors" that power cells may have promise for treating one of the most common forms of inherited neuromuscular disease, according to a report in the September Cell Metabolism, a Cell Press publication. Neuromuscular disorders caused by defects in those mitochondrial motors affect a large number of children and adults worldwide, but today remain without treatment, the researchers said. continued http://www.physorg.com/news139579038.html Investigational drug tested for preventing muscle fiber death in muscular dystrophy Medicine & Health / Research An investigational antiviral drug currently undergoing human trials in Europe for treating Hepatitis C infections may have potential to reduce muscle cell damage in Duchenne and other forms of muscular dystrophy (MD). A research team led by Cincinnati Children’s Hospital Medical Center reported their results using three different mouse models of MD in a letter posted online March 16 by the journal Nature Medicine. continue http://www.physorg.com/news124897458.html
WCG
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Sekerob
Ace Cruncher Joined: Jul 24, 2005 Post Count: 20043 Status: Offline |
Our Canines may carry the answer:
----------------------------------------Fixing a Genetic Flaw A genetic technique successfully treats Duchenne muscular dystrophy in dogs. http://www.technologyreview.com/biomedicine/22327/ An international team of researchers has successfully treated dogs with the canine form of Duchenne muscular dystrophy (DMD), a rapidly progressing and ultimately fatal muscle disease that afflicts one out of every 3,600 boys. The researchers used a novel technique called exon skipping to restore partial function to the gene involved in Duchenne. The study, published in Annals of Neurology, gives hope that a similar approach could work in humans. DMD is caused by an aberration in the gene that encodes dystrophin, an important structural protein in muscle cells. Patients with DMD are unable to produce functional dystrophin, which leads to holes in the outer membranes of their muscle cells. Eventually, their muscles degenerate faster than they can be rebuilt, and few patients survive beyond their early 30s. Unlike traditional gene therapy, which attempts to replace a mutated gene with a functional copy, exon skipping relies on a variation of a technique called antisense, in which short synthetic DNA or RNA molecules are designed to bind to a region of DNA or RNA and block its function. Companies are developing antisense therapies for cancer, diabetes, heart disease, and autoimmune diseases, among others. The approach grew out of studies comparing DMD to a milder form of disease called Becker muscular dystrophy (BMD). Both diseases arise when patients are missing portions of the dystrophin gene's exons, the areas of DNA that code for protein. Paradoxically, some BMD patients are missing much larger pieces of the gene yet are far healthier than patients with DMD. Several years ago, scientists found that the difference is not in how much of the gene is missing, but in how those missing portions affect the remaining gene sequence. Most Duchenne patients have frameshift mutations, which interfere with the cell's reading of three-letter DNA code. These deletions shift the remaining DNA sequence into different triplet groupings, rendering the gene unreadable. In Becker patients, the remaining DNA can still be read normally, allowing them to produce a smaller but still functional version of dystrophin. Eric Hoffman, a lead author of the study at Children's National Medical Center, in Washington, DC, says that scientists realized they might help DMD patients by creating a "patch" that blocks transcription of a portion of the gene in a way that puts the remaining code back into sequence--essentially recreating the milder Becker muscular dystrophy.
WCG
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