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    Home » News » Undigested fructose linked to increased anxiety and inflammation
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    Undigested fructose linked to increased anxiety and inflammation

    healthadminBy healthadminMarch 11, 2026No Comments7 Mins Read
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    Recent research published in journals Brain behavior and immunity Studies have shown that the inability to properly digest fructose is associated with increased anxiety and inflammation throughout the body. This study suggests that unabsorbed fructose changes the bacterial community in the gastrointestinal tract, which triggers an immune response that can affect the brain. These findings provide new insight into how modern sugar-rich diets are affecting our mental health.

    Historically, humans ingested very small amounts of fructose each day. This sugar was obtained mainly from seasonal fruits and honey. Today, modern food processing has made fructose incredibly abundant, and people consume large amounts of this sugar through soda, sweets, and processed foods.

    The human digestive system relies on specific transport proteins to absorb fructose into the bloodstream. Think of these transporters as specialized doorways that line the small intestine. These doorways can only allow a limited amount of sugar to pass through at one time.

    When you ingest more fructose than your intestines can handle, the excess sugar continues to move down your digestive tract. Eventually it flows out into the large intestine. This condition is known as fructose malabsorption.

    In the large intestine, unabsorbed sugars encounter the intestinal microbiota. The microbiome is the vast collection of bacteria and other microorganisms that live in our lower gut. These microorganisms act as a secondary digestive system.

    When intestinal bacteria encounter unabsorbed fructose, they begin to ferment it. This sudden sugar feast can change the balance of bacterial species in your gut. Some bacteria will grow on the extra fructose, while others will die.

    Changes in the gut microbiome can affect other parts of the body. The gut is closely connected to the immune system and brain. Adeline Coursin, a researcher at the University of Bordeaux, and her colleagues wanted to understand this relationship.

    The research team suspected that malabsorption of fructose could disrupt the gut microbiota and cause a mild systemic inflammatory state. They hypothesized that this inflammation could be transmitted through the bloodstream. Ultimately, they believed that this series of events could activate immune cells in the brain.

    These specialized brain immune cells are called microglia. When microglia become highly active, they cause inflammation in brain tissue. This type of brain inflammation is known to be associated with mood problems such as anxiety and depression.

    To test their ideas, the researchers designed a comprehensive study with two parts. They first evaluated a group of 55 young, healthy male volunteers. They specifically selected men of average weight to avoid the metabolic effects of obesity.

    The team needed to determine which volunteers had fructose malabsorption. They asked participants to drink a solution containing a specific amount of fructose. The researchers then analyzed the participants’ breathing over several hours.

    When intestinal bacteria ferment unabsorbed fructose, gases such as hydrogen and methane are produced. These gases are absorbed into the blood and eventually expelled through the lungs. By measuring these exhaled gases, the team determined which volunteers were not fully absorbing the sugar.

    Participants also tracked their daily food intake for one week. They recorded exactly what they ate and drank. This allowed the researchers to calculate average daily fructose intake and identify dietary sources of sugar.

    To measure mental health, volunteers filled out a standardized questionnaire designed to measure anxiety traits. Finally, the researchers collected blood and stool samples from each person. These samples provided a window into their immune systems and gut bacteria.

    The results showed that 60 percent of the volunteers suffered from fructose malabsorption. Total daily fructose intake was similar between those who absorbed sugar well and those who did not. Both groups consumed an average of about 30 grams of fructose per day.

    Despite this similar intake, malabsorbers reported higher levels of anxiety traits on questionnaires. Blood tests revealed elevated levels of inflammatory proteins, which are malabsorbable substances. These proteins act as chemical messengers that signal the immune system to respond.

    The presence of these proteins indicates a mild body-wide inflammatory state with malabsorbed substances. When researchers analyzed the stool samples, they found distinct differences in the types of bacteria present. Malabsorption substances had higher abundances of certain bacterial groups and lower abundances of other bacterial groups.

    For example, malabsorbed materials contained more of a group of bacteria called bifidobacteria. Conversely, a group called Prevotella had lower levels. These changes suggest that unabsorbed sugars were directly reshaping the microscopic ecosystem of the intestine.

    The abundance of certain bacteria also correlated with where the fructose came from. Bacteria levels varied depending on whether participants ate fruit, sweet baked goods, or sugary drinks. Some of these bacterial groups were directly associated with the volunteers’ anxiety scores and blood inflammation levels.

    To better understand the biological mechanisms behind these observations, the researchers conducted experiments in mice. They used genetically engineered mice that lacked a specific protein doorway needed to absorb fructose. These mice served as a reliable model of complete fructose malabsorption.

    The engineered mice were fed a diet containing 5% fructose for 4 weeks, just like normal mice. After being fed this diet for a month, the mice were behaviorally tested. The researchers placed the animals in a raised maze shaped like a plus sign.

    This maze has two closed arms and two open, exposed arms. Rats naturally prefer dark, closed spaces, but they also like to explore. Normal mice spend a significant amount of time in open arms.

    The researchers also placed mice inside cylinders of water. They measured how long the mice spent actively swimming in an attempt to escape compared to passively floating. These standard tests help researchers assess anxiety and depressive behavior in rodents.

    Mice with impaired fructose absorption showed more anxiety-like and depressive-like behavior than normal mice. They mainly avoided the open areas of the elevated maze. They also spent more time floating motionless in the water bottle.

    The researchers then examined the mice’s intestines and brains. Similar to human volunteers, the malabsorptive mice showed clear changes in their intestinal bacterial counts. Certain bacterial families have almost completely disappeared, while others have rapidly proliferated.

    The research team took a closer look at microglia in the brain. Under normal conditions, microglia act as housekeepers, cleaning up cellular debris. When the brain is stressed, it shifts into a protective inflammatory mode.

    The researchers measured the activity of specific genes associated with this inflammatory condition. Microglia in malabsorptive mice produced higher levels of inflammatory molecules. They also showed increased activity in genes associated with distressing conditions associated with the disease.

    This evidence suggests that unabsorbed sugar in the intestine was transmitting distress signals to the brain’s immune system. The resulting brain inflammation may have caused the behavioral changes observed in the mice. This animal model perfectly mirrored the trends seen in human volunteers.

    The researchers noted that their study had several limitations. This study included only male subjects in both the human and animal parts. Biological sex can have a significant impact on both metabolic processes and mental health outcomes.

    Therefore, future studies should also include female subjects. This step will help determine whether the relationship between fructose malabsorption and anxiety applies to everyone. Enlarging the pool of subjects is necessary to fully understand the condition.

    Furthermore, the human studies were strictly observational. The researchers had no control over the volunteers’ daily diet. They were unable to see what would happen to anxiety levels if fructose was completely removed from a person’s diet.

    Future clinical trials may test whether a low-fructose diet improves anxiety symptoms in patients with malabsorption. Exploring this association may ultimately lead to new nutritional therapies. Such discoveries could provide new ways to manage mental health through personalized dietary choices.

    The study, “Fructose malabsorption induces dysbiosis and increases anxiety in humans and animal models in men,” was authored by Adeline Coursan, Delphine Polve, Anne-Marie Leroi, Magali Monnoye, Lea Roussin, Clara Benatar, Marie-Pierre Tavolacci, Muriel Quillard Muraine, Mathilde Maccarone, Olivia Guerin, and Estelle. Huivet, Charline Guerlain, Valérie Brunel, Jérôme Bélanger, Jean-Paul Pe de Barros, Guillaume Glucerol, Laurent Nordon, Sophie Ray, Charlotte Madore, Xavier Fioramonti, Chloe Mercior, Veronique Douard.



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