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21.12.2022 11:09

Obesity researchers discover new gene mutation in children

Medizinische Fakultät Anne Grimm Stabsstelle Universitätskommunikation / Medienredaktion
Universität Leipzig

    A research team at Leipzig University’s Faculty of Medicine has discovered a new mechanism that is associated with severe obesity in children. This genetic rearrangement leads to an unusual expression of a gene involved in hunger control and is not detected by most routine genetic tests for obesity. The findings were published in the journal Nature Metabolism.

    Obesity and diseases associated with obesity are among the leading causes of death worldwide, but its causes are not yet fully understood. However, it is known that several factors are responsible for the development and progression of the disease and that genetic factors also play a role. In most of the individuals affected, the combination of an unhealthy lifestyle and a genetic predisposition called a polygenic disorder leads to severe obesity. A polygenic disorder is one in which several genes are affected.

    Researchers at Leipzig University Hospital and the Helmholtz Institute for Metabolic, Obesity and Vascular Research (HI-MAG) at Helmholtz Munich also want to identify the rare cases of monogenic obesity. In these patients, defects in a single gene are the cause of the disease. Those affected often show a decreased sensation of satiety in early childhood and suffer from a constant feeling of hunger.

    While studying tissue samples from a girl with severe obesity, the Leipzig researchers found that a specific gene, the agouti-signalling protein (ASIP) gene, was produced at high levels in cells where it is not normally present (e.g. in fat cells, white blood cells and neuronal cells).

    Project head Antje Körner, professor of paediatric research and paediatrician said, “This discovery is a kind of missing piece of the puzzle in research on monogenic human obesity. It is also evidence for the importance of key molecular regulatory mechanisms of energy balance and body weight via melanocortin 4 receptor neurons in humans and provides us with a unique opportunity to study these mechanisms.”

    The type of mutation found in the current study escapes standard genetic screening algorithms, which means that it remains undetected in many affected patients. Thanks to targeted screening of the Leipzig Childhood Obesity cohort, Professors Körner’s team has identified four additional patients with the same mutation.

    “Given this discovery, I believe we need to rethink the strategies we use to identify patients with monogenic obesity. The ultimate goal of our research is to transfer the findings from genetic studies to future personalised treatment options for obesity,” said Professor Matthias Blüher, director of HI-MAG and spokesperson of the CRC 1052 "Obesity Mechanisms" in the Faculty of Medicine.

    Translation: Kerstin Gackle


    Wissenschaftliche Ansprechpartner:

    Professor Antje Körner, MD
    Phone: +49 341 97-26500
    Email: antje.koerner@medizin.uni-leipzig.de


    Originalpublikation:

    Original publication in Nature Metabolism: Aberrant expression of agouti signaling protein (ASIP) as a cause of monogenic severe childhood obesity. DOI: 10.1038/s42255-022-00703-9 https://www.nature.com/articles/s42255-022-00703-9


    Bilder

    Obesity is one of the Faculty of Medicine’s key research areas.
    Obesity is one of the Faculty of Medicine’s key research areas.
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    Professor Antje Körner in the research lab.
    Professor Antje Körner in the research lab.
    Swen Reichhold
    Universität Leipzig


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    Obesity is one of the Faculty of Medicine’s key research areas.


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    Professor Antje Körner in the research lab.


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