Type 2 diabetes starts in liver, find University of Geneva scientists

28 Nov 2017 --- Scientists from the University of Geneva (UNIGE) in Switzerland have unraveled the factors linking obesity and insulin resistance, as well as the key role played by the liver in the onset of the disease. By deciphering how the protein PTPR- γ – which is increased in the context of obesity – inhibits insulin receptors located at the surface of liver cells, the researchers’ findings in Nature Communications open the door to potential new therapeutic strategies.

Among the detrimental effects of obesity is the risk of developing Type 2 diabetes. Even though the strong links between obesity and Type 2 diabetes are well known, the cellular and molecular mechanisms were so far poorly understood, UNIGE points out.

Affecting as many as 650 million people worldwide, obesity has become one of the most serious global health issues. Among its detrimental effects, it increases the risk of developing metabolic conditions, primarily Type 2 diabetes. If the strong links between obesity and Type 2 diabetes are well known, the cellular and molecular mechanisms by which obesity predisposes to the development of insulin resistance were so far poorly understood.

Protein provides key to insulin issues
By deciphering how the protein PTPR-γ, which is increased in the context of obesity, inhibits insulin receptors located at the surface of liver cells, the scientists have opened the door to potential new therapeutic strategies.

The expansion of fat cells, a characteristic of obesity, leads to an increase in inflammatory signals that have effects on the liver as well as on several other organs. Obesity-induced inflammation triggers the activation of a transcription factor called NF-kβ, which seems to be instrumental in the development of diabetes.

But what are the exact cellular and molecular mechanisms at stake and how could they lead to new therapeutic strategies? “To answer these questions, we focused on a protein called PTPR-γ (for Protein Tyrosine Phosphatase Receptor Gamma), which is a target of NF-kβ”, explains Professor Roberto Coppari, Coordinator of the UNIGE Faculty of Medicine Diabetes Centre.

“We first examined various human cohorts: these human studies indicated that PTPR-γ content in liver increases upon inflammation, an effect that could directly affect insulin receptors by inhibiting insulin action,” Coppari adds.

No diabetes without PTPR-γ
To test their hypothesis, the scientists modified the levels of PTPR-γ expression in mice, by either suppressing, normally expressing or overexpressing it, and observed the effect on insulin resistance.

“The mice totally lacking PTPR-γ, when put on a high-calorie diet, did develop obesity. But they did not show any sign of insulin resistance and seemed to be entirely protected from diet-induced diabetes,” explains Xavier Brenachot, a researcher at UNIGE Faculty of Medicine and first author of the study. The scientists also administered lipopolysaccharide, a toxin pertaining to certain bacteria of the gut microbiota associated with obesity and insulin resistance. Once again, the animals lacking PTPR-γ did not develop insulin resistance.

To fine-tune their analysis, Roberto Coppari and his colleagues reconstituted the expression of PTPR-γ at normal levels, but only in hepatocytes (liver cells). The mice were again prone to insulin resistance, indicating the pivotal role of the liver. Moreover, a twofold overexpression in the liver (mimicking the natural pathophysiology of obesity) was sufficient to cause insulin resistance.

Potential new therapeutic target
The metabolic functions of this protein were never characterized; this discovery therefore opens the door for potential new therapies, UNIGE reports. Previous studies had already studied PTP proteins in search for diabetes treatments to no avail.

However, contrary to some of its family members that are intracellular, the protein identified in Geneva is located on the cell membrane. It is therefore of much easier access for therapeutic molecules. Interestingly, the very form of this protein allows for potential inhibition strategies: when two independent PTPR-γ molecules are brought together by a ligand, they cannot act any more.

The researchers are now working on identifying the endogenous ligand produced by the body, or on developing molecules that could mimic its function.

Translational research shapes tomorrow’s medicine
“This study would not have been possible without the UNIGE Faculty Diabetes Centre, established in 2015 to enhance interactions between clinical and basic researchers,” indicates Roberto Coppari.

“Indeed, our research started with clinical observations made by Prof. Francesco Negro – also a member of UNIGE Faculty Diabetes Centre – at the University Hospitals of Geneva,” Coppari adds. “We now hope that our pre-clinical and clinical results will in turn be translated into clinical progress and contribute to a better management of Type 2 diabetes that, today, affects one in 11 adults globally, or 422 million people.”

To contact our editorial team please email us at editorial@cnsmedia.com