The mere sight of a meal triggers an inflammatory response in the brain
University of Basel
Even
before carbohydrates reach the bloodstream, the very sight and smell of a meal
trigger the release of insulin. 
Even before the first bite, the body starts releasing insulin.
(Photo: Carles Rabada, unsplash)
For the first time, researchers from the University of Basel and University Hospital Basel have shown that this insulin release depends on a short-term inflammatory response that takes place in these circumstances.
In overweight individuals, however, this inflammatory response
is so excessive that it can impair insulin secretion.
Even
the anticipation of a forthcoming meal triggers a series of responses in the
body, perhaps the most familiar of which is the watering of the mouth. But the
hormone insulin, which regulates blood sugar, also arrives on the scene even
before we tuck into the first mouthful of food. Experts refer to this as the
neurally mediated (or cephalic) phase of insulin secretion.
Meal stimulates immune defense
In
the past, however, it was unclear how the sensory perception of a meal
generated a signal to the pancreas to ramp up insulin production. Now,
researchers from the University of Basel and University Hospital Basel have
identified an important piece of the puzzle: an inflammatory factor known as
interleukin 1 beta (IL1B), which is also involved in the immune response to
pathogens or in tissue damage. The team have reported their findings in the
journal Cell Metabolism.
"The
fact that this inflammatory factor is responsible for a considerable proportion
of normal insulin secretion in healthy individuals is surprising, because it's
also involved in the development of type 2 diabetes," explains study
leader Professor Marc Donath from the Department of Biomedicine and the Clinic
of Endocrinology.
Also
known as "adult-onset diabetes," this form of diabetes is caused by
chronic inflammation that damages the insulin-producing cells of the pancreas,
among other things. This is another situation in which IL1B plays a key role --
in this case, it is produced and secreted in excessively large quantities. With
this in mind, clinical studies are now examining whether inhibitors against
this inflammatory factor are suitable for use as therapeutic agents for
diabetes.
Short-lived
inflammatory response
Circumstances
are different when it comes to neurally mediated insulin secretion: "The
smell and sight of a meal stimulate specific immune cells in the brain known as
the microglia," says study author Dr. Sophia Wiedemann, resident physician
for internal medicine. "These cells briefly secrete IL1B, which in turn affects
the autonomic nervous system via the vagus nerve." This system then relays
the signal to the site of insulin secretion -- that is, the pancreas.
In
the case of morbid obesity, however, this neurally mediated phase of insulin
secretion is disrupted. Specifically, by the initial excessive inflammatory
response, as explained by doctoral candidate Kelly Trimigliozzi, who carried
out the main part of the study in collaboration with Wiedemann.
"Our results indicate that IL1B plays an important role in linking up sensory information such as the sight and smell of a meal with subsequent neurally mediated insulin secretion -- and in regulating this connection," summarizes Marc Donath.
