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Protein controls fat metabolism

Date:
March 17, 2020
Source:
Max Delbrück Center for Molecular Medicine in the Helmholtz Association
Summary:
A protein in the cell envelope influences the rate of fatty acid uptake in cells. This process also appears to be altered in overweight people.
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Many foods -- whether it's the mozzarella on your favorite pizza, the olive oil in salad dressing or hollandaise sauce during asparagus season -- contain lots of fat. The fatty acids in these foods are among the essential nutrients that people need to survive. When someone eats more fatty acids than the body can immediately convert into energy, the extra amount is stored in tissues -- often in the form of unwanted rolls of fat around the hips or stomach -- and serves as a kind of reserve supply.

The quantity of fatty acids transported by blood to the tissues and deposited there is determined by a wide range of factors. Researchers at the Max Delbrueck Center for Molecular Medicine in the Helmholtz Association (MDC) have now identified one of these factors as the protein EHD2.

If this protein is missing completely, fat-storing cells take up significantly more fatty acids from the cellular environment. Dr. Claudia Matthaeus first observed this phenomenon in the brown adipose tissue of mice during her work at the MDC. She finds it particularly exciting that EHD2 apparently plays a key role in human fat metabolism, too. "We have discovered that overweight people produce less EHD2 than people with normal weight," Matthaeus says. It is not clear yet why this is the case. Based on these new insights, Matthaeus and her colleagues, including researchers from the MDC research group led by Professor Oliver Daumke, assume that EHD2 controls a metabolic pathway that regulates fatty acid uptake in fat cells. This pathway is modified in obesity, the researchers write in the journal PNAS.

Cellular uptake of fat occurs when portions of the cell membrane pinch off

Oliver Daumke is long acquainted with EHD2. The structural biologist has been characterizing the structure and mechanimsm of this protein for more than ten years. As a membrane protein, EHD2 resides inside muscle and fat cells. During the inward folding of the cell envelope, small flask-shaped membrane structures called caveolae are formed. These invaginations either remain on the surface of the cell membrane or they pinch off and carry foreign material -- such as fatty acids -- into the cell. This process is known as endocytosis, Daumke explains. The researcher assumes that the EHD2 protein assembles into ring-like structures around the neck of the membrane vessel and thus stymies the pinch-off process. Daumke is convinced that if EHD2 is not present as a stabilizer, caveolae pinch off more frequently and the cell takes up more fat.

This is precisely what Matthaeus and her colleagues examined. The researchers worked with mice in which the EHD2 gene had been switched off. Using an electron microscope, Matthaeus observed that compared to normal mice, many more caveolae had become detached from the plasma membrane. She was also able to determine that fatty acid uptake was greater in cells lacking EHD2 and that the lipid droplets, which are intracellular accumulations of fat, were larger in these cells.

Obesity influences EHD2 production

Matthaeus asked herself if she would also be able to observe an influence of EHD2 on fat metabolism in humans. So she, together with a colleague from Leipzig University, studied tissue samples from men and women with different body weight. She quickly discovered that in people who were overweight (body mass index of 25 or higher), cells produce less EHD2 than in slim people. The researcher presumes that there is a correlation between frequent membrane pinch-off and the formation of fat depots. "During obesity, we observed that the number of caveolae and their detachment from the membrane get out of sync," Matthaeus says.

In November, Matthaeus left the MDC to take a position at the National Institutes of Health in the United States. There she plans to continue her research into caveolae and fat metabolism. "There are still many unanswered questions," Matthaeus says. She is now especially interested in investigating the transport of fatty acids within the cell and the formation of lipid droplets.


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Materials provided by Max Delbrück Center for Molecular Medicine in the Helmholtz Association. Note: Content may be edited for style and length.


Journal Reference:

  1. Claudia Matthaeus, Ines Lahmann, Séverine Kunz, Wenke Jonas, Arthur Alves Melo, Martin Lehmann, Elin Larsson, Richard Lundmark, Matthias Kern, Matthias Blüher, Hannah Olschowski, Julian Kompa, Britta Brügger, Dominik N. Müller, Volker Haucke, Annette Schürmann, Carmen Birchmeier, Oliver Daumke. EHD2-mediated restriction of caveolar dynamics regulates cellular fatty acid uptake. Proceedings of the National Academy of Sciences, 2020; 201918415 DOI: 10.1073/pnas.1918415117

Cite This Page:

Max Delbrück Center for Molecular Medicine in the Helmholtz Association. "Protein controls fat metabolism." ScienceDaily. ScienceDaily, 17 March 2020. <www.sciencedaily.com/releases/2020/03/200317103826.htm>.
Max Delbrück Center for Molecular Medicine in the Helmholtz Association. (2020, March 17). Protein controls fat metabolism. ScienceDaily. Retrieved December 25, 2024 from www.sciencedaily.com/releases/2020/03/200317103826.htm
Max Delbrück Center for Molecular Medicine in the Helmholtz Association. "Protein controls fat metabolism." ScienceDaily. www.sciencedaily.com/releases/2020/03/200317103826.htm (accessed December 25, 2024).

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