Appetite control depends on signaling at the 'primary cilium,' mouse study shows

January 8, 2018, University of California, San Francisco
Credit: CC0 Public Domain

UC San Francisco researchers have discovered that the brain's ability to regulate body weight depends on a novel form of signaling in the brain's "hunger circuit" via antenna-like structures on neurons called primary cilia.

Primary are distinct from , the finger-like projections that act as a sort of cellular conveyer belt, with functions such as removing debris from the lungs and windpipe. Immotile were once thought to be vestigial, like a cellular appendix, but in the past decade, research at UCSF and elsewhere has revealed that these structures play a key role in many forms of hormonal signaling in the body.

Now the new UCSF study—published January 8, 2018 in Nature Genetics—shows that primary cilia also play a crucial role in signaling within the brain. Neuroscientists are accustomed to thinking of brain signaling in terms of direct chemical or electrical communication among neurons at sites called synapses, but the new findings reveal that chemical signaling at primary cilia may also play an important, and previously overlooked role. In addition, the findings suggest potential new therapeutic approaches to the growing global obesity epidemic, the researchers say.

"We're building a unified understanding of the human genetics of obesity," said senior author Christian Vaisse, MD, PhD, a professor in the Diabetes Center at UCSF and a member of the UCSF Institute for Human Genetics. "Until recently, many obesity researchers had barely heard of primary cilia, but that's going to change."

Key signaling proteins in brain's hunger circuit meet in primary cilia

The modern epidemic of obesity is driven largely by environmental factors, including access to essentially unlimited sources of ready calories paired with increasingly sedentary lifestyles. But not everyone exposed to the same unhealthy conditions becomes overweight. Studies have estimated that genetics contribute between 40 and 70 percent to people's inclination towards unhealthy weight gain.

Since the 1990s, geneticists have shown that most of the genetic alterations that contribute to severe obesity in humans appear to disrupt a network of neurons within the brain's hypothalamus. This "hunger circuit" monitors levels of leptin, a hormone secreted by fat cells, and uses this information to adjust appetite and energy expenditure to maintain a stable weight. People (and mice) with mutations in the leptin gene itself, or in neural genes involved in detecting and responding to leptin, cannot detect when their body has already got plenty of fat, and constantly eat as if they were starving.

The system works like this: fat cells throughout your body secrete leptin, which travels to your brain and is detected by neurons in a part of the hypothalamus called the arcuate nucleus. These neurons then relay information about leptin levels to a group of neurons in another part of the hypothalamus, called the paraventricular nucleus (PVN), which determine if leptin levels are too high (indicating excess body fat) or too low (indicating dangerously depleted energy reserves). The PVN neurons then send out instructions to the rest of the brain to adjust your appetite and energy level appropriately.

In recent years, Vaisse and his team have demonstrated that mutations in a particular gene involved in the hunger circuit—called MC4R—are the most common single-gene driver of obesity in humans, accounting for 3 to 5 percent of all cases of (defined as having a body mass index greater than 40). Vaisse's team have shown that the MC4R protein—a receptor molecule that detects chemical signals produced by the cells in the arcuate nucleus—is present in a subset of PVN cells and appears to be critical to these neurons' ability to respond to high leptin levels by reducing appetite. However, the researchers still knew very little about these neurons or how they work.

At the same time, cilia researchers such as Jeremy Reiter, MD, PhD, professor and chair of the Department of Biochemistry at UCSF, had been exploring how rare genetic defects in primary cilia cause diseases such as Bardet-Biedl and Alström syndromes, which are nearly always accompanied by extreme obesity. A burst of research by Reiter and others in the past few years has explained how cilia defects lead to the other symptoms of these syndromes, such as extra fingers or toes, retinal defects, and kidney disease, but the link to obesity remained unclear.

In the new study, Vaisse's team collaborated with Reiter as well as neuroscientist Mark von Zastrow, MD, PhD, a professor of psychiatry at UCSF, to study whether there might be a link between how MC4R mutations and cilia defects drive obesity.

They began by fluorescently tagging the MC4R protein in the brains of laboratory mice. When the researchers examined the newly visible MC4R-expressing neurons, they found that the MC4R protein was uniquely concentrated in the cells' primary cilia, suggesting that its key appetite-regulating function may occur there. Indeed, when the researchers caused mice to express the mutated versions of the human MC4R gene seen in patients with extreme obesity, they found that the MC4R protein failed to reach the cilia.

These imaging studies also examined a protein called adenylyl cyclase 3 (ADCY3), which, like MC4R, localizes to primary cilia and has been recently associated with obesity. This protein is known to mediate signaling through proteins like MC4R, so to test whether these two proteins interact in the primary cilia of MC4R-expressing neurons in the PVN, the researchers blocked ADCY3 function in these cells in mice, and found that the animals significantly increased their food consumption and began to exhibit signs of obesity.

The researchers conclude that ADCY3 and MC4R must come together in the primary cilia of PVN neurons to allow these cells to detect signals from the arcuate nucleus indicating high body-fat levels and to respond appropriately by reducing appetite. This suggests that if genetic mutations prevent MC4R from getting to the cilia, or if other genetic defects damage the primary cilium itself, the brain has no way to pull the emergency brake on weight gain.

"It's exciting how much progress this field has made," Vaisse said. "In the '90s, we were asking whether or not obesity is genetic; a decade ago we were discovering that most obesity risk factors primarily impact the leptin circuit in the brain; and now we are on the verge of understanding how defects in this specific subcellular structure of a particular subset of hypothalamic neurons drives weight gain and obesity."

Research highlights important role of cilia in neuronal signaling in the brain

The new study raises the possibility of developing treatments that could improve appetite control in people with by modifying signaling at the primary cilia of MC4R-expressing neurons. However, the development of treatments may still be a long way off, Vaisse cautioned. "We still know so little about the primary cilium, and particularly how it is involved in signaling within these particular neurons. We yet don't know what we might do to fix it when it is broken."

The story also highlights an intriguing distinction between how the hypothalamus controls appetite on short versus long timescales. As UCSF's Zachary Knight, PhD, has shown, the same hypothalamic neurons that reduce appetite when the body's fat stores are in good shape are also responsible for tamping down your hunger for dinner when you get your meal. The emerging picture, Vaisse says, is that fast signaling at synapses between is responsible for making sure you only eat when you're hungry, while slower signaling sensed by the primary cilia of the same cells controls your body's long-term energy balance between calorie intake and expenditure.

"I don't think anyone was thinking that MC4R, this neurotransmitter receptor associated with satiety, might not be functioning at synapses, but at cilia," Reiter said. "By studying rare diseases, we have discovered a new biological principle by which can communicate."

Explore further: Is obesity a ciliopathy, triggered by malfunctioning primary cilia?

More information: Subcellular localization of MC4R with ADCY3 at neuronal primary cilia underlies a common pathway for genetic predisposition to obesity, Nature Genetics (2018). nature.com/articles/doi:10.1038/s41588-017-0020-9

Related Stories

Is obesity a ciliopathy, triggered by malfunctioning primary cilia?

December 6, 2011
Is obesity a ciliopathy, a disorder such as polycystic kidney disease (PKD), which is triggered by a defect in the microscopic hair-like cilia that protrude from virtually every cell of humans and other vertebrates?

Obese inducing brain mechanism

September 15, 2017
Leptin is an adipocyte-derived hormone that stimulates hypothalamic neurons to strongly inhibit food intake. Leptin signaling in the hypothalamus, a part of the mid-brain, thus plays a crucial role in the regulation of body ...

How an unlikely cellular 'antenna' can impair brain development

August 7, 2017
An antenna-like structure on cells, once considered a useless vestige, appears to be important for proper brain development in mammals and when impaired can cause defects in the brain's wiring similar to what's seen in autism, ...

Bone-derived hormone suppresses appetite in mice

March 8, 2017
A hormone secreted by bone cells can suppress appetite, according to mouse studies conducted by Columbia University Medical Center (CUMC) researchers. The hormone—called lipocalin 2—turns on neurons in the brain that ...

Brain receptor identified as link between obese mothers and children's high blood pressure

October 12, 2016
Exposure of babies to high levels of the 'fullness' hormone, leptin, in the womb irreversibly activates receptors in the brain that regulate blood pressure, according to a new study by researchers from King's College London, ...

Recommended for you

A single missing gene leads to miscarriage

October 19, 2018
A single gene from the mother plays such a crucial role in the development of the placenta that its dysfunction leads to miscarriages. Researchers from the Medical Faculty of Ruhr-Universität Bochum (RUB) have observed this ...

Making gene therapy delivery safer and more efficient

October 18, 2018
Viral vectors used to deliver gene therapies undergo spontaneous changes during manufacturing which affects their structure and function, found researchers from the Perelman School of Medicine at the University of Pennsylvania ...

Student develops microfluidics device to help scientists identify early genetic markers of cancer

October 16, 2018
As anyone who has played "Where's Waldo" knows, searching for a single item in a landscape filled with a mélange of characters and objects can be a challenge. Chrissy O'Keefe, a Ph.D. student in the Department of Biomedical ...

Researchers use brain cells in a dish to study genetic origins of schizophrenia

October 16, 2018
A study in Biological Psychiatry has established a new analytical method for investigating the complex genetic origins of mental illnesses using brain cells that are grown in a dish from human embryonic stem cells. Researchers ...

Why heart contractions are weaker in those with hypertrophic cardiomyopathy

October 16, 2018
When a young athlete suddenly dies of a heart attack, chances are high that they suffer from familial hypertrophic cardiomyopathy (HCM). Itis the most common genetic heart disease in the US and affects an estimated 1 in 500 ...

Importance of cell cycle and cellular senescence in the placenta discovered

October 15, 2018
Working with researchers from Stanford University and St. Anna Children's Cancer Research, researchers from Jürgen Pollheimer's laboratory at the Medical University of Vienna's Department of Obstetrics and Gynecology have ...

0 comments

Please sign in to add a comment. Registration is free, and takes less than a minute. Read more

Click here to reset your password.
Sign in to get notified via email when new comments are made.