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  • Heart toggles between maintenance and en

    From ScienceDaily@1:317/3 to All on Tue Mar 7 21:30:28 2023
    Heart toggles between maintenance and energy-boost mode using ribosomes
    New mechanism found which can be exploited to prevent or heal damage to
    the heart

    Date:
    March 7, 2023
    Source:
    Center for Genomic Regulation
    Summary:
    Researchers reveal that cardiomyocytes and skeletal muscle cells
    replace their existing stock of ribosomes with a different type
    which can make physical contact with mitochondria, the batteries
    of the cells, and significantly boost the production of ATP. In the
    heart, the natural mechanism is triggered in response to myocardial
    infarction, as well as cardiac hypertrophy. The findings establish
    ribosomes as a new frontier for therapeutic strategies that prevent
    or heal damage to the heart.


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    FULL STORY ========================================================================== Researchers at the Centre for Genomic Regulation (CRG) in Barcelona
    have discovered a mechanism involving ribosomes which helps the heart
    toggle between a 'regular maintenance mode' for day-to-day function and
    an 'energy-boost mode' which aids recovery for high-demand situations
    including heart attacks. The findings are published in a 'Breakthrough
    Article' in the journal Nucleic Acids Research.


    ========================================================================== Ribosomes are the molecular factories that manufacture proteins in all
    living cells. Historically, they have been perceived as simple but vital workhorses which lack the ability to regulate a cell's function. However,
    there is increasing evidence that these fundamental units -- which come
    in different shapes and forms -- carry out specialised tasks, which are
    yet to be discovered.

    Using different experimental techniques and latest-generation sequencing technologies, the researchers found that cardiomyocytes, the cells
    responsible for the heart contracting, and skeletal muscle cells, which
    are connected to bones and are critical for strength and movement,
    have different types of ribosomes compared to all other types of cells
    in the body.

    "For a long time, we thought that ribosomes were the same in every single
    cell of the human body. This makes them impractical drug targets as you
    could be healing one body part while damaging many others. The existence
    of specialised ribosomes and their specificity to heart and muscle cells
    is a turning point because it means it is possible to develop medicines
    that target specific ribosomes for the purpose of treating cardiovascular disease," explains Dr. Eva Novoa, corresponding author of the study and researcher at the Centre for Genomic Regulation.

    Ribosomes are made of proteins. While the ribosomes in most human cells
    contain ribosomal protein L3 (RPL3), the ribosomes in cardiomyocytes
    and skeletal muscle cells contain ribosomal protein L3-like (RPL3L). The crucial difference between the proteins, which share 77% of their amino
    acid sequence, is their tail. The study shows that cells will exclusively
    use one protein or the other.

    Whichever protein ends up being used, the corresponding tail sticks
    out on the surface of the ribosome, changing its shape and surface,
    which in turn affects how it binds to other proteins and receptors.

    The researchers found that cardiomyocyte and skeletal muscle ribosomes
    showed no benefit in terms of protein synthesis compared to other
    ribosomes. However, the researchers were surprised to find that knocking
    the RPL3L gene out in mice showed both cardiomyocytes and skeletal
    muscle cells creating ribosomes with RPL3 instead. In stark contrast,
    knocking out RPL3 was lethal.

    Researchers found that this newfound compensation mechanism also naturally occurred in response to a heart attack or myocardial infarction, with cardiomyocytes replacing all their existing stock of RPL3L-containing
    ribosomes with ribosomes containing RPL3 instead. The different shape of
    the new ribosomes enables them to make physical contact with mitochondria,
    the batteries of the cells, and significantly boosts the production of
    ATP, the universal currency used for energy. The effect was detected
    within six hours after infarction and peaked after 72 hours.

    This ribosome replacement mechanism also occurs during cardiac
    hypertrophy, a response of the heart to increased workload which can
    be either physiological, such as after exercise, or pathological, due
    to disease. RPL3-containing ribosomes in cardiomyocytes peak after 96
    hours in response to cardiac hypertrophy.

    The study provides some clues for why the heart and muscle use RPL3L for ribosomes in the first place. The researchers found that RPL3L is only
    present in the ribosomes of adult cardiomyocytes, while fetal tissues exclusively use RPL3. At the same time, mice lacking RPL3L had lower
    lean muscle mass at 55- weeks old compared to mice with RPL3L.

    "When we are born, our hearts need lots of energy to grow. At this point, cardiomyocytes only express RPL3, swapping to RPL3L only once the heart
    is fully mature. We don't know exactly why, but the cells could be making
    the switch to fine tune the mitochondrial activity in resting conditions
    and possibly decrease levels of free radicals, dangerous by-products of mitochondrial metabolism. This could explain how the heart delicately
    balances two different modes -- one where ribosomes boost energy levels
    and one where the heart is kept in maintenance mode," explains first
    author of the study and PhD candidate Ivan Milenkovic.

    The discovery of this mechanism can be exploited to improve cardiac
    health and function, and establishes ribosomes as a new frontier for therapeutic strategies that prevent or heal damage to the heart. The researchers are now researching the molecular mechanisms in further
    detail to distinguish pathological and physiological cardiac hypertrophy, including exercise experiments with mice to assess how the presence or
    absence of RPL3L in cardiomyocytes affects physical performance.

    * RELATED_TOPICS
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    ========================================================================== Story Source: Materials provided by Center_for_Genomic_Regulation. Note: Content may be edited for style and length.


    ========================================================================== Journal Reference:
    1. Ivan Milenkovic, Helaine Graziele Santos Vieira, Morghan C Lucas,
    Jorge
    Ruiz-Orera, Giannino Patone, Scott Kesteven, Jianxin Wu, Michael
    Feneley, Guadalupe Espadas, Eduard Sabido', Norbert Hu"bner,
    Sebastiaan van Heesch, Mirko Vo"lkers, Eva Maria Novoa. Dynamic
    interplay between RPL3- and RPL3L-containing ribosomes modulates
    mitochondrial activity in the mammalian heart. Nucleic Acids
    Research, 2023 DOI: 10.1093/nar/gkad121 ==========================================================================

    Link to news story: https://www.sciencedaily.com/releases/2023/03/230307144344.htm

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