Why testosterone reduces diabetes risk

May 6, 2016

This article is published in collaboration with Futurity.

A diabetes patient has her pulse checked by diabetes specialist Doctor Tong Xiao Lin during a medical check-up at the Guanganmen Chinese medicine Hospital in Beijing March 19, 2012. In 30 years, the Chinese people have gone from having barely enough to eat to worrying about chronic diseases like diabetes, leaving the healthcare system struggling with a condition that is rapidly outpacing its ability to keep up. Spending on diabetes reached $25 billion in China in 2010, only 6 percent of the $390 billion spent worldwide. But the rate of diabetes in China is already at the same levels as in the West, leaving doctors, drug companies and policymakers to hunt for low-cost alternatives before the disease swamps the rudimentary healthcare system. Picture taken March 19, 2012. To match Feature CHINA-DIABETES/ REUTERS/David Gray

Scientists have identified how testosterone regulates blood sugar in men, which could improve type 2 diabetes therapies. Image: REUTERS/David Gray

Keith Brannon

Associate Director, Tulane University

Doctors have long known that men with low testosterone are more likely to develop type 2 diabetes.

Now, for the first time, they have identified how the hormone helps men regulate blood sugar by triggering key signaling mechanisms in islets, clusters of cells within the pancreas that produce insulin.

The results, published in the journal Cell Metabolism, could help identify new treatments, researchers say.

“We have found the cause—and a potential treatment pathway—for type 2 diabetes in testosterone-deficient men,” says senior author Franck Mauvais-Jarvis, professor of medicine at Tulane University School of Medicine. “Our study shows that testosterone is an anti-diabetic hormone in men. If we can modulate its action without side effects, it is a therapeutic avenue for type 2 diabetes.”

Researchers used specially bred male mice with pancreatic beta cells lacking the receptor to testosterone (the androgen receptor). They fed them a diet rich in fats and sugar, and tested their response to glucose. The mice without androgen receptors all developed lower insulin secretion, leading to glucose intolerance compared with normal mice in the control group.

To better understand how testosterone interacted with insulin production within the pancreas, researchers administered the hormone and glucose directly to human islet cells treated with an androgen receptor inhibitor and islets cells harvested from mice without androgen receptors. In both cases the islet cells showed decreased insulin production compared to islet cells whose receptor to testosterone was not inhibited or missing.

Further experiments in cultured mouse and human islet cells showed the insulin-producing effect of testosterone could be abolished by inhibiting glucagon-like peptide-1 (GLP-1), a hormone the body produces after a meal. The study suggests that testosterone amplifies the islet impact of the hormone, which is currently used as a diabetes treatment.

Other researchers from Tulane and from Northwestern University, Vanderbilt University, University of Chicago, University of Illinois, and Catholic University of Leuven in Belgium are coauthors of the study.

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