Complex biology of hyperinsulinism may offer clues to better treatment
The Children's Hospital of Philadelphia May 22, 2017
Analyzing insulin–producing pancreatic cells from children with congenital hyperinsulinism (HI), CHOP endocrinology experts have discovered patterns of metabolic function and gene expression that may lay the groundwork for potential new treatments for this rare disease.
ÂThis study shows that the pathophysiology of hyperinsulinism is far more complex than commonly understood, said co–study leader Diva D. De Leon, MD, an Endocrinologist and Director of CHOPÂs Congenital Hyperinsulinism Center. ÂWe expect that this improved understanding of events at the cellular level will allow us to identify opportunities for improved treatments.Â
De Leon and co–study leader Changhong Li, MD, PhD, also a CHOP scientist, published the study online April 25 in the journal Diabetes. Both study leaders, along with multiple co–authors, are also members of the Institute for Diabetes, Obesity and Metabolism in the Perelman School of Medicine at the University of Pennsylvania.
In congenital HI, gene mutations disrupt the insulin–secreting beta cells in the pancreas and cause insulin levels to become excessive, leading to dangerously low concentrations of glucose. The most severe form of congenital HI results from mutations that inactivate potassium channels in the beta cells. This type of HI does not respond to current drugs, and may result in brain damage or death. When the defective cells are concentrated in a small area of the pancreas (focal HI), surgery can produce a cure, but when all the beta cells are defective (diffuse HI), surgery improves but does not cure the hyperinsulinism and can leave a patient vulnerable to diabetes.
The conventional understanding is that the defective potassium channels in this type of HI simply allow uncontrolled insulin secretion. The current study offers a more comprehensive view, revealing secondary changes in gene expression and metabolic patterns that lead to broader biological effects. ÂOur goal is to use this knowledge to identify new targets for more effective treatments for this devastating condition, said De Leon.
The article, ÂFunctional and metabolic consequences of ATP–dependent potassium channel inactivation in human islets, was published in the journal Diabetes.
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ÂThis study shows that the pathophysiology of hyperinsulinism is far more complex than commonly understood, said co–study leader Diva D. De Leon, MD, an Endocrinologist and Director of CHOPÂs Congenital Hyperinsulinism Center. ÂWe expect that this improved understanding of events at the cellular level will allow us to identify opportunities for improved treatments.Â
De Leon and co–study leader Changhong Li, MD, PhD, also a CHOP scientist, published the study online April 25 in the journal Diabetes. Both study leaders, along with multiple co–authors, are also members of the Institute for Diabetes, Obesity and Metabolism in the Perelman School of Medicine at the University of Pennsylvania.
In congenital HI, gene mutations disrupt the insulin–secreting beta cells in the pancreas and cause insulin levels to become excessive, leading to dangerously low concentrations of glucose. The most severe form of congenital HI results from mutations that inactivate potassium channels in the beta cells. This type of HI does not respond to current drugs, and may result in brain damage or death. When the defective cells are concentrated in a small area of the pancreas (focal HI), surgery can produce a cure, but when all the beta cells are defective (diffuse HI), surgery improves but does not cure the hyperinsulinism and can leave a patient vulnerable to diabetes.
The conventional understanding is that the defective potassium channels in this type of HI simply allow uncontrolled insulin secretion. The current study offers a more comprehensive view, revealing secondary changes in gene expression and metabolic patterns that lead to broader biological effects. ÂOur goal is to use this knowledge to identify new targets for more effective treatments for this devastating condition, said De Leon.
The article, ÂFunctional and metabolic consequences of ATP–dependent potassium channel inactivation in human islets, was published in the journal Diabetes.
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