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  • Targeting iron uptake to create a new cl

    From ScienceDaily@1337:3/111 to All on Mon Aug 17 21:30:36 2020
    Targeting iron uptake to create a new class of antibiotics against UTIs


    Date:
    August 17, 2020
    Source:
    American Chemical Society
    Summary:
    At least half of all women will have a urinary tract infection
    during their lifetimes, and many of the infections -- which have
    increasingly become resistant to a wide array of antibiotics --
    recur. Now, researchers report early progress toward developing
    a new class of antibiotics that would fight these infections by
    starving the causative bacteria of iron.



    FULL STORY ==========================================================================
    At 11 million cases annually, urinary tract infections (UTIs) are
    the most common outpatient infections in the U.S., according to the
    U.S. Department of Health and Human Services. At least half of all women
    will have a UTI during their lifetimes, and many of the infections --
    which have increasingly become resistant to a wide array of antibiotics
    -- recur. Now, researchers report early progress toward developing a
    new class of antibiotics that would fight these infections by starving
    the causative bacteria of iron.


    ==========================================================================
    The researchers will present their results today at the American Chemical Society (ACS) Fall 2020 Virtual Meeting & Expo. "You can't stop bacteria
    from evolving and developing resistance to antibiotics," says Mary
    Rose Ronquillo, an undergraduate student who works in the lab of Scott
    C. Eagon, Ph.D. "The aim of our research is to develop a drug that acts
    in a different way from current drugs -- by depriving the bacteria of
    iron, a key nutrient essential to their survival." Currently, most drugs
    that treat UTIs caused by uropathogenic E. coli (UPEC) either disrupt
    synthesis of the bacterial cell wall or interfere with bacterial DNA replication. Since the urinary tract is an iron-deficient environment,
    UPEC have evolved several ways to obtain iron, such as by producing
    molecules called siderophores that sop up iron bound to host proteins.

    The researchers, who are at California Polytechnic State University, have collaborated on this project with other scientists at the University of Michigan School of Medicine. The collaborators previously showed that the
    iron acquisition process can be a target for small molecules for possible
    UTI treatment. In that study, they screened nearly 150,000 compounds and identified 16 that stop these bacteria from growing under iron-limiting conditions. Of these 16, two compounds were linked to disruption of the bacterial TonB system, which consists of three transmembrane proteins
    that help UPEC take up iron.

    Eagon's group is focusing on these two compounds for further study.

    "We selected one of these compounds as a scaffold to modify into
    potential small molecule inhibitors of the TonB system," M. Cole Detels,
    an undergraduate student in Eagon's lab, explains. The molecule is called 2-{[(3-chloro-4- methoxyphenyl)amino]methyl}quinolin-8-ol, or more simply,
    the "hydroxyquinoline scaffold." After they made the scaffold molecule,
    Detels and Ronquillo prepared five variations, and another three are now
    in the purification stage. "While the synthesis of the potential drugs
    is relatively straightforward, purifying them from the soup of other
    chemicals used in their preparation has been challenging," Detels says.

    The team says that the goal is to prepare a library of inhibitors in
    which the hydroxyquinoline scaffold is modified with various functional
    groups. "With this library in hand, we will work with our collaborators to screen them against UPEC and human cell lines to look for broad toxicity," Eagon says.

    "After that, the compounds will be tested in animal models to see if
    they kill the bacteria in vivo." Once Eagon's team finishes preparing
    the complete hydroxyquinoline library, they plan to make variations of
    the second scaffold molecule.

    Because they target iron uptake, this new class of drugs is expected
    to have no effect on beneficial E. coli strains in other regions of the
    body. Iron is plentiful in the body in non-urinary tract locations, so hindering iron uptake shouldn't cause a problem for these bacteria. Most current antibiotics, however, wipe out all strains, including beneficial
    gut flora. And because there is no TonB homolog found in humans, the possibility of toxic side effects would also be reduced compared to
    other antibiotics.


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


    ==========================================================================


    Link to news story: https://www.sciencedaily.com/releases/2020/08/200817104317.htm

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