In a new study, researchers have described how nervous systems and immune systems talk to each other to control metabolism and inflammation. Their finding published in the journal Nature furthers scientists' understanding of why older adults fail to burn stored belly fat, which raises the risk of chronic disease. The study also points to potential therapeutic approaches to target the problem, the researchers said.
Older adults, regardless of body weight, have increased belly fat. However, when they need to expend energy, older people do not burn the energy stored in fat cells as efficiently as younger adults, leading to the accumulation of harmful belly fat. The underlying cause for this unresponsiveness in fat cells was unknown.
In the study researchers focused on specialized immune cells known as macrophages, which are typically involved in controlling infections. The lab discovered a new type of macrophage that resides on the nerves in belly fat. These nerve-associated macrophages become inflamed with age and do not allow the neurotransmitters, which are chemical messengers, to properly function.
The researchers also isolated the immune cells from fat tissue of young and old mice, and then sequenced the genome to understand the problem. "We discovered that the aged macrophages can break down the neurotransmitters called catecholamines, and thus do not allow fat cells to supply the fuel when demand arises," said the senior author.
The researchers found that when they lowered a specific receptor that controls inflammation, the NLRP3 inflammasome, in aged macrophages, the catecholamines could act to induce fat breakdown, similar to that of young mice.
"The key finding is that the immune cells talk to the nervous system to control metabolism," said the senior author.
In further experiments, the researchers blocked an enzyme that is increased in aged macrophages, restoring normal fat metabolism in older mice. Senior author noted that this enzyme, monoamine oxidase-A or MAOA, is inhibited by existing drugs in the treatment of depression. "Theoretically one could repurpose these MAOA inhibitor drugs to improve metabolism in aged individuals," senior author said. But also cautioned that more research is needed to specifically target these drugs to belly fat and to test the safety of this approach.
In future research, researchers will further examine the immune cells and their interaction with nerves, and how this neuro-immune dialogue controls health and disease. If controlling inflammation in aging immune cells can improve metabolism, it may have other positive effects on the nervous system or on the process of aging itself, said the researchers.
https://news.yale.edu/2017/09/27/battling-belly-fat-specialized-immune-cells-impair-metabolism-aging
http://www.nature.com/nature/journal/vaop/ncurrent/full/nature24022.html
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