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  • New 'cocktail' drug could benefit up to

    From ScienceDaily@1:317/3 to All on Wed Feb 23 21:30:42 2022
    New 'cocktail' drug could benefit up to 45 per cent of patients with
    Duchenne muscular dystrophy

    Date:
    February 23, 2022
    Source:
    University of Alberta
    Summary:
    A new 'cocktail' drug under development could provide an effective
    and economical treatment to lessen symptoms for up to 45 per cent
    of patients with Duchenne muscular dystrophy (DMD), a chronic
    muscle-wasting disease.



    FULL STORY ==========================================================================
    A new "cocktail" drug being developed at the University of Alberta could provide an effective and economical treatment to lessen symptoms for
    up to 45 per cent of patients with Duchenne muscular dystrophy (DMD),
    a chronic muscle- wasting disease.


    ==========================================================================
    A team led by researcher Toshifumi Yokota, a professor of medical genetics
    in the Faculty of Medicine & Dentistry, created -- and is now testing --
    a cocktail of six treatments which would mean nearly half of patients
    with DMD could be treated with just one drug.

    DMD affects six of every 100,000 people -- usually boys. People with DMD
    have various mutations in the body's largest gene, dystrophin, which is
    a protein that cells need to stay intact. Dystrophin has 79 sections,
    or exons, and if even one is missing the body cannot produce the protein
    and the muscles degenerate.

    There is no cure for DMD, but a new class of drugs uses an approach
    called "exon skipping." It acts as a Band-Aid over the missing exons,
    so the body can skip over the damaged instructions and produce the
    protein needed to rebuild muscle tissue.

    The U.S Food and Drug Administration has already approved other
    similar treatments, including viltolarsen, which is based on Yokota's
    research. Each, however, has limited applicability. This new "cocktail" treatment could help many more patients.

    "Each of the previously developed exon-skipping molecules has been able to treat only around 10 per cent of DMD patients because they have different mutations to their exons in different locations within the gene," said
    Yokota, who is also the Friends of Garrett Cumming Research & Muscular Dystrophy Canada Endowed Research Chair.

    "Our approach is to skip over 11 exons all at once, which would allow
    us to treat approximately 45 per cent of patients," he explained.

    The research was published this week in the Proceedings of the National
    Academy of Sciences.

    Yokota's team tested the new synthetic drug in patient-derived muscle
    tissue in test tubes and in mice. They found signs of dystrophin
    production, muscle building and improved heart function.

    DMD often leads to extreme skeletal body weakness, yet most patients
    actually die from heart failure. Existing exon-skipping treatments do not penetrate the heart muscle -- a limitation this new cocktail addresses, according to Yokota.

    "Our cocktail combines the antisense oligonucleotides with a new peptide
    which allows the drug to penetrate the heart muscle," he said.

    The cocktail still needs to undertake toxicology testing and go through
    the regulatory steps to conduct clinical trials. Yokota and his colleagues recently launched a company to help commercialize the drug.

    ========================================================================== Story Source: Materials provided by University_of_Alberta. Original
    written by Gillian Rutherford. Note: Content may be edited for style
    and length.


    ========================================================================== Journal Reference:
    1. Kenji Rowel Q. Lim, Stanley Woo, Dyanna Melo, Yiqing Huang, Kasia
    Dzierlega, Md Nur Ahad Shah, Tejal Aslesh, Rohini Roy Roshmi,
    Yusuke Echigoya, Rika Maruyama, Hong M. Moulton, Toshifumi
    Yokota. Development of DG9 peptide-conjugated single- and
    multi-exon skipping therapies for the treatment of Duchenne muscular
    dystrophy. Proceedings of the National Academy of Sciences, 2022;
    119 (9): e2112546119 DOI: 10.1073/ pnas.2112546119 ==========================================================================

    Link to news story: https://www.sciencedaily.com/releases/2022/02/220223164606.htm

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