Cell types like astrocytes regulate metabolic processes – Discovery of a brain sugar switch

Researchers at the Technical University of Munich (TUM) discovered that our brain actively takes sugar from the blood.
Prior to this, researchers around the world had assumed that this was a purely passive process.
An international team led by diabetes expert Matthias Tschöp reported in the journal ‘Cell’ that transportation of sugar into the brain is regulated by so-called glia cells that react to hormones such as insulin or leptin; previously it was thought that this was only possible for neurons.
Insulin signaling in astrocytes is required for proper glucose entry to the brain. Above panel: a model of intact insulin signaling in astrocytes and below panel a disrupted model. (Source: Garcia-Caceres)
Insulin signaling in astrocytes is required for proper glucose entry to the brain. Above panel: a model of intact insulin signaling in astrocytes and below panel a disrupted model. (Source: Garcia-Caceres Click for larger image size

The rapid rise in obesity and the associated spread of type 2 diabetes represent
an enormous challenge for our society. No efficient and safe medicines to prevent or stop this development are available. The failure to develop adequate treatments is thought to be primarily due to the fact that the molecular machinery controlling systemic metabolism still remains mostly unknown.


Matthias Tschöp of the Chair for Metabolic Diseases at TUM and Director of the Division of Metabolic Diseases and also of the Helmholtz Diabetes Center (HDC) at Helmholtz Zentrum München, is investigating how control centers in the brain remotely control our metabolism in order to adjust optimally to our environment. The brain has the highest sugar consumption of all organs and also controls, for example, hunger feelings.

“We therefore suspected that a process as important as providing the brain with sufficient sugar was unlikely to be completely random,” so Dr. Cristina García-Cáceres, neurobiologist at the HDC and the study’s lead author.
“We were misled by the fact that nerve cells apparently did not control this process and therefore first thought it to occur passively.
Then we had the idea that glia cells such as astrocytes*, which had long been misunderstood as less important ‘support cells’, might have something to do with transporting sugar into the brain.”

The scientists therefore first examined the activity of insulin receptors on the surface of astrocytes, molecular structures which respond to insulin to influence cell metabolism.
Here they found that if this receptor was missing on certain astrocytes the result was less activity in neurons that curb food uptake (proopiomelanocortin neurons).

At the same time, adaption of metabolism to challenges like sugar intake became impaired.
With the help of advanced imaging technologies such as positron emission tomography, the scientists were able to show that hormones such as insulin and leptin act specifically on ‘support’ glia cells to regulate sugar intake into the brain, like a ‘sugar switch’.
Without insulin receptors, astrocytes became less efficient in transporting glucose into the brain, particularly in the area of the satiety centers, which are located in the hypothalamus.


“Our results showed for the first time that essential metabolic and behavioral processes are not regulated via neuronal cells alone and that other cell types in the brain, such as astrocytes, play a crucial role,” explains study leader Matthias Tschöp, who also heads the drug discovery division at the German Center for Diabetes Research (DZD).
“This represents a paradigm shift and could help explain why it has been so difficult to find sufficiently efficient and save medicines for diabetes and obesity until now.”

According to the scientists, numerous new studies will now be necessary to adjust the old model of purely neural control of food intake and metabolism with a concept where astrocytes and possibly even immune cells in the brain also play a crucial role. Once there is a better understanding of the interaction between these various cells, the idea is to find ways and substances that modulate pathways on multiple cell types to curb sugar addiction and ultimately provide better treatment to the growing number of obese and diabetic individuals.
“We have a lot of work ahead of us,” states García-Cáceres, “but at least now we have a better idea where to look.”


* Astrocytes are the most common cells in the brain. One of their jobs is to form the blood-brain barrier by enclosing the blood vessels that run in the brain and selectively allowing only certain substances through to the nerve cells.

Just recently the scientists had already shown that astrocytes react to leptin, a metabolic hormone (Kim et al., 2014). This is an important factor for satiety.
Because now both leptin and insulin have been shown to influence astrocytes, the researchers propose to develop a new model which, in addition to the neurons, also takes into account the astrocytes as the adjustors of the metabolism and the feeling of hunger.
They hope that the more detailed view this produces will provide new perspectives for drug development.


Caceres, C. et al. (2016): Astrocytic insulin signalling couples brain glucose uptake with nutrient availability, Cell, 08/2016. DOI: 10.1016/j.cell.2016.07.028


Prof. Dr. Matthias Tschöp
Technical University og Munich
Chair for Metabolic Deseases
Mail: matthias.tschoep@tum.de



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