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    Home»Health»A “Silver Bullet” for Cancer? Scientists Uncover Secret Power of RNA
    Health

    A “Silver Bullet” for Cancer? Scientists Uncover Secret Power of RNA

    By University of ChicagoOctober 6, 202411 Comments6 Mins Read
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    Cancer Cells Illustration
    Researchers from the University of Chicago have uncovered a new role for RNA in how DNA is packaged, which sheds light on TET2-related mutations linked to cancer. This discovery offers new targets for drug therapies and suggests a broader role for RNA in regulating gene expression.

    RNA plays an increasingly significant role in human gene expression.

    Within each cell, inside every nucleus, your survival relies on an intricate and highly complex process. Proteins are continuously wrapping and unwrapping DNA, and even the smallest error in this delicate dance can result in cancer.

    A new study from the University of Chicago reveals a previously unknown part of this dance—one with significant implications for human health.

    In the study, published Oct. 2 in Nature, a team of scientists led by UChicago Prof. Chuan He, in collaboration with University of Texas Health Science Center at San Antonio Prof. Mingjiang Xu, found that RNA plays a significant role in how DNA is packaged and stored in your cells, via a gene known as TET2. This pathway also appears to explain a long-standing puzzle about why so many cancers and other disorders involve TET2-related mutations—and suggests a set of new targets for treatments.

    “This represents a conceptual breakthrough,” said He, who is the John T. Wilson Distinguished Service Professor in the Department of Chemistry and the Department of Biochemistry and Molecular Biology and an investigator of the Howard Hughes Medical Institute.

    “Not only does it offer targets for therapy for several diseases, but we are adding to the grand picture of chromatin regulation in biology,” he said. “We hope the real-world impact is going to be very high.”

    RNA revelations

    He’s lab has made several discoveries that shook up our picture of how genes are expressed. In 2011, they found that, in addition to modifications to DNA and proteins, modifications to RNA may also control what genes are expressed.

    Since then, He and his team have found more and more ways that RNA methylation is fundamentally involved in which genes are turned on and off in both the plant and animal kingdoms.

    With this lens, they turned their attention to a gene called TET2. For a long time, we’ve known that when TET2 or TET2-related genes are mutated, all sorts of problems follow. These mutations occur in 10-60% of different human leukemia cases, and pop up in other types of cancers as well. The problem was that we didn’t know why—which significantly hampers the search for treatments.

    The other members of the TET family act on DNA, so for years, researchers had been looking at TET2’s effects on DNA. But He’s lab found they’d been looking in the wrong place: TET2 actually affects RNA.

    When your cells print their own copies of your genetic material, they have to be neatly packaged up and folded for later reference; the packages are known as chromatin. If that doesn’t happen correctly, all sorts of issues can follow. It turns out that RNA is a key player in this process, and that its role is controlled by TET2 through a modification process called methylation.

    Through a clever set of experiments, removing genes, and seeing what happened, the He lab team showed how this works. They found that TET2 controls how often a type of modification known as m5C occurs on certain types of RNA, which attracts a protein known as MBD6, which in turn controls the packaging of chromatin.

    When you’re an infant and your cells are actively dividing into different types of cells, TET2 loosens up the reins so that chromatin can be more easily accessed and stem cells can turn into other cells. But once you’re an adult, TET2 is supposed to tighten up the reins. If that repressing force gets lost, MBD6 has free rein, and havoc can ensue.

    “If you have a TET2 mutation, you reopen this growth pathway that could eventually lead to cancer—especially in the blood and brain, because this pathway looks to be most important in blood and brain development,” said He.

    As a final confirmation, the team tested human leukemia cells in petri dishes. When the team removed the cells’ ability to create MBD6, effectively pulling on the reins, the leukemia cells all died.

    ‘A silver bullet’

    The most exciting part of this discovery to cancer researchers is that it gives them a whole new set of targets for drugs.

    “What we hope we can get from this is a silver bullet to selectively get rid of just cancer cells, by targeting this specific pathway activated because of TET2 or IDH loss,” said He, who is working with UChicago’s Polsky Center for Entrepreneurship and Innovation to found a startup company to create just such a drug.

    But we also know that TET2 mutations have consequences other than cancer. TET2 mutations also occur in a fraction of all adults older than 70 and contribute to an increased risk of heart disease, stroke, diabetes, and other inflammatory conditions, a condition known as CHIP.

    “These patients have TET2 mutant blood cells, but they haven’t yet caused cancer,” explained Caner Saygin, an oncologist and assistant professor of medicine at the University of Chicago Medicine who specializes in treating CHIP patients and is also working with the He lab on several projects. “But these TET2 mutant cells are more inflammatory, and as they circulate, they cause an increased risk for things like heart, liver, and kidney diseases. Right now, I cannot prescribe anything to these patients because they don’t have cancer yet, but if we could eliminate those mutant cells, we could improve their lives.”

    A radical change

    The finding is also a radical change in our understanding of chromatin—and hence gene expression as a whole.

    Previously, we knew that one form of RNA methylation called m6A affects gene expression—its placement and removal affect the packaging of chromatin, which directs which stretches of DNA are translated into reality.

    But if m5C is also in this category, that suggests this is a general mechanism to control chromatin and gene expression, and there could be more. “If there’s a second, you could have a third, fourth, fifth,” said He. “This says that RNA modification on chromatin is a major mechanism for chromatin and gene transcription regulation. We think this pathway is just the tip of the iceberg.”

    Reference: “RNA m5C oxidation by TET2 regulates chromatin state and leukaemogenesis” by Zhongyu Zou, Xiaoyang Dou, Ying Li, Zijie Zhang, Juan Wang, Boyang Gao, Yu Xiao, Yiding Wang, Lijie Zhao, Chenxi Sun, Qinzhe Liu, Xianbin Yu, Hao Wang, Juyeong Hong, Qing Dai, Feng-Chun Yang, Mingjiang Xu and Chuan He, 2 October 2024, Nature.
    DOI: 10.1038/s41586-024-07969-x

    The study was funded by the National Institute of Health.

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    Cancer DNA Genetics Molecular Biology Popular University of Chicago
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    11 Comments

    1. MC on October 6, 2024 3:57 pm

      DNA is where you came from
      RNA is how you got here from there.
      CRC is who you are today.

      Reply
      • Keith Ashelin on October 6, 2024 9:40 pm

        “RNA Plays an Increasingly Significant Role in Gene Expression”. I find paragraph titles like these rather humorous. No, actually, RNA plays exactly the same role that it has ever played. It is we crude humans whose understanding has changed. I have long maintained that we and our entire medical industry are just groping, trying to understand our current state of creation, and it will probably take another 10,000 years before we know enough to speak intelligently about it.

        Reply
      • John Delphia on October 7, 2024 12:11 am

        Hopefully a way of genetic engineering of mitochondria can produce a treatment to insert mitochondria that can stabilize TET2 control in the cell.

        This would allow an easy way to deliver a permanent minimally invasive treatment.

        Reply
    2. Dlowe on October 6, 2024 8:15 pm

      Antineoplastones have been the silver bullet for decades already. Don’t trust RNA!

      Reply
    3. Richard on October 6, 2024 9:42 pm

      More American-controlled technology created by ethnic Chinese.

      Reply
    4. Chad on October 6, 2024 10:41 pm

      This is BS it should read frequency and light spectrums . Period the sad part is I believe most doctors if worthy of their title should know this . If they do not I question their title and should probably get a new career.

      Reply
    5. Lester Perry on October 7, 2024 1:05 am

      My wife died from lymphoblastic leukemia. Cancer developing in the bone marrow. She was given two bone biopsies that confirmed cancer cells in her bone marrow. The Hematologist that treated her does bone marrow transplants. But never performed this treatment on her, which could have extended her life. But instead kept giving her massive amounts of conventional chemo and radiation until her blood cells could not regenerate anymore that permanently damaged her liver and died of liver failure. In addition to his gross negligence he decides to give her a trial version of the Car-T therapy that did not work. Ultimately taking her life. I live in California and California’s law states that a doctor would need to violate what is considered standard of practice. The Hematoligy department where she was treated performs bone marrow transplants as a standard practice. So the way I see it, this doctor violated this standard of practice and I hope I can make him accountable for this some day

      Reply
    6. Valerie on October 7, 2024 4:15 am

      AUTISM CANCER – AUTOIMMUNE MEDIATED INFLAMMATORY DISORDER CONTRAVERSIALLY ASSOCIATED WITH THE TOXIC ACCUMULATIVE VIRAL TOXIC ASSAULT WITH MULTIPLE LIVE VIRUS VACCINES PLUS ADJUVANTS ( CHEMICAL COMPOUNDS USED TO STIMULATE THE IMMUNE SYSTEM) IN EARLY INFANCY OF AN IMMATURE DEVELOPING CNS CENTRAL NERVOUS SYSTEM & BRAIN LEADING TO DEVESTATING DEMYLINATING NEUROPATHY.
      A VIRAL INFECTION OFTEN PRECEEDS CANCER DEVELOPMENT.
      LIVE VIRUS VACCINES ARE ‘CONTRAINDICATED FOR USE IN THE IMMUNOCOMPROMISED’ FOR THIS EXACT REASON.
      PROBLEM IS WE DO NOT PROMOTE
      “SCREENINGB4VACCINES”
      FOR
      “CONTRAINDICATION” PRIOR TO COMMENCEMENT OF THE CURRENT EXPANSIVE PROGRAMME OF CHILDHOOD VACCINES.
      REMOVAL OF GOVERNMENT AWARDED
      “INDEMNITY” AGAINST LITIGATION FOR DIRECT VACCINE ASSOCIATED INJURY TO THE COLLECTIVE PHARMACUTICAL/ MEDICAL / RESEARCH INDUSTRY
      NEEDS TO BECOME A GLOBAL HEALTH PRIORITY.
      AS EVERY SECOND PERSON IS ANTICIPATED TO DEVELOP CANCER IN THIS LIFE TIME AND UP TO 5% OF TODAYS INFANTS CARRY AN OFFICIAL DIAGNOSIS OF AUTISM WHICH PREDISPOSES THE PERSON TO LATER DEVELOPMENT OF CANCER.
      FACT.

      Reply
      • Helen on October 7, 2024 6:52 am

        Wow, you needed all caps for this nonsense?

        Reply
      • John on October 7, 2024 7:15 am

        As someone who was injured by the RNA covid “vax”, I’ll take a hard pass on any more gene therapies

        Reply
    7. Sydney Ross Singer on October 7, 2024 4:56 am

      Does this mean that RNA vaccines can affect DNA? Sounds like RNA vaccines may have side effects they never anticipated, since they are still discovering the role of RNA in controlling the genome.

      Reply
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