News Release 8-Sep-2020
A new study reveals that reduced body temperature plays a major role in initiating the extensive health benefits of calorie-restricted diets.
Scripps Research Institute
LA JOLLA, CA–Cutting calories significantly may not be an easy task for most, but it’s tied to a host of health benefits ranging from longer lifespan to a much lower chance of developing cancer, heart disease, diabetes and neurodegenerative conditions such as Alzheimer’s.
A new study from teams led by Scripps Research Professors Bruno Conti, PhD, and Gary Siuzdak, PhD, illuminates the critical role that body temperature plays in realizing these diet-induced health benefits. Through their findings, the scientists pave the way toward creating a medicinal compound that imitates the valuable effects of reduced body temperature.
The research appears in Science Signaling.
Making the cool connection
Conti has spent years studying how and why calorie restriction leads to better health, with the ultimate goal of translating the findings into medicines that can mimic what happens naturally when a person eats less.
One consistent observation is that when mammals consume less food, their body temperature drops. It’s evolution’s way of helping us conserve energy until food is available again, Conti explains. It makes sense, considering that up to half of what we eat every day is turned into energy simply to maintain our core body temperature.
Conti’s previous work showed that temperature reduction can increase lifespan independently of calorie restriction–and that these effects involve activation of certain cellular processes, most of which remain to be identified.
On the flip side, studies have shown that preventing body temperature from dropping can actually counteract positive effects of calorie restriction. Notably, in an experiment involving calorie-restricted mice, anti-cancer benefits were diminished when core body temperature remained the same.
“It’s not easy to discern what’s driving the beneficial changes of calorie restriction,” Conti says. “Is it the reduced calories on their own, or the change in body temperature that typically happens when one consumes fewer calories? Or is it a combination of both?”
Metabolites hold the answer
In the new research, Conti and his team designed an experiment that would allow them to independently evaluate the effects of reduced nutrients and those of body temperature.
They compared one group of calorie-restricted mice housed at room temperature–about 68 degrees Fahrenheit (22 degrees Celsius) to another group housed at 86 degrees (30 degrees Celsius). The warmer environment invoked “thermoneutrality,” a state at which most animals cannot easily reduce their body temperature.
The Siuzdak team, using a technology they developed called activity metabolomics, then evaluated the mice by measuring their metabolites, or chemicals released by the animals’ metabolism. Through this, they were able to look for molecules in the bloodstream and in the brain that are changed by the reduction of either nutrients or body temperature.
“The data we collected showed that temperature has an equal or greater effect than nutrients on metabolism during calorie restriction,” Conti says. Notably, the team provided the first comprehensive profiling of the metabolites that are changed by temperature reduction.
Through a computing analysis of results from both groups of mice, the scientists were able to prioritize which metabolites were most responsible for triggering changes to core body temperature. In a separate experiment, they also showed it is possible to administer certain metabolites as a drug to affect body temperature.
Conti says further work to validate the changes induced by temperature during calorie restriction should provide novel targets for future medicines he calls “temperature mimetics,” which could offer the health-promoting effects without having to reduce body temperature.
The paper, “Metabolic adaptation to calorie restriction,” was authored by Carlos Guijas, J. Rafael Montenegro-Burke, Rigo Cintron-Colon, Xavier Domingo-Almenara, Manuel Sanchez-Alavez, Carlos A. Aguirre, Kokila Shankar, Erica L.-W. Majumder, Elizabeth Billings, Bruno Conti and Gary Siuzdak.
The research was supported by the National Institutes of Health [R01 GM114368-03, P30 MH062261-17, P01 DA026146-02 and GM113894], the NIH Cloud Credits Model Pilot (a component of the NIH Big Data to Knowledge program), the Skaggs Graduate School of Chemical and Biological Sciences and ARCS Foundation.