Intermediary Neuron Acts as Synaptic Cloaking Device, Says Carnegie Mellon Study
Researchers Find That Somatostatin Neurons Regulate Synaptic Activity in the Neocortex
By Jocelyn Duffy
PITTSBURGH—Neuroscientists believe that the connectome, a map of each and every connection between the millions of neurons in the brain, will provide a blueprint that will allow them to link brain anatomy to brain function. But a new study from Carnegie Mellon University has found that a specific type of neuron might be thwarting their efforts at mapping the connectome by temporarily cloaking the synapses that link a wide field of neurons.
If you’re a Star Trek fan, think of it as a Romulan or Klingon cloaking device, which hides a warship. The cloaked ship is invisible until it fires at an enemy. In the study published in the March 16 issue of Current Biology, the researchers found that a class of inhibitory neurons, called somatostatin cells, send out a signal – much like a cloaking device – that silences neighboring excitatory neurons. Synapses, like a cloaked warship, can’t be seen if they aren’t firing; activating the somatostatin cells makes the synapses and local network of neurons invisible to researchers.
Furthermore, by silencing certain parts of the neuronal network, the activity of the somatostatin neurons also can change the way the brain functions, heightening some perceptual pathways and silencing others.
“It was totally unexpected that these cells would work this way,” said Alison Barth, professor of biological sciences and a member of BrainHubSM, Carnegie Mellon’s neuroscience research initiative. “Changing the activity of just this one cell type can let you change the brain’s circuit structure at will. This could dramatically change how we look at – and use – the connectome.”
The Carnegie Mellon researchers discovered this synaptic cloaking device, much in the same way Starfleet would detect a cloaked Klingon warship – they were conducting their normal research and noticed that something just didn’t look quite right.
Joanna Urban-Ciecko, a research scientist in Barth’s lab, noticed that the synapses in her experiments were not behaving the way that previous experimenters had reported. Prior studies reported that the synapses should be strong and reliable, and that they should always grow and strengthen in response to a stimulus. But the neurons Urban-Ciecko looked at were weak and unreliable.
The difference between Urban-Ciecko’s research and the previously completed work was that her research was being done under real-life conditions. Prior research on synapse function was done under conditions optimized for observing synapses. However, such experimental conditions don’t reflect the noisy brain environment in which synapses normally exist.
“There’s this big black box in neuroscience. We know how to make synapses stronger in a dish. But what’s going on in the brain to initiate synaptic strengthening in real life?” Barth asked.
To find out, Urban-Ciecko looked at neurons in the brain’s neocortex that were functioning under normal, noisy conditions. She took paired-cell recordings from pyramidal cells, a type of excitatory neuron, and found that many of the synapses between the neurons were not functioning, or functioning at an unexpectedly low level. Urban-Ciecko then recorded the activity of somatostatin cells, a type of inhibitory neuron, and found that those neurons were much more active than expected.
“The somatostatin cells were so active, I wondered if they could possibly be driving the inhibition of synapses,” Urban-Ciecko said.
To test her hypothesis, Urban-Ciecko turned to optogenetics, a technique that controls neurons with light. She used light to trigger an enzyme that activated and deactivated the somatostatin neuron. When the somatostatin cells were turned off, synapses grew big and strong. When the cells were turned on, the synapses became weaker and in some cases, disappeared entirely.
“You have inputs coming at you all the time, why do you remember one thing and not the other?” “We think that somatostatin neurons may be gating whether synapses are used, and whether they can be changed during some important event, to enable learning,” said Barth, who is also a member of the joint CMU/University of Pittsburgh Center for the Neural Basis of Cognition (CNBC).
The researchers found that when the somatostatin neurons were turned on, this triggered the cloaking device. The neuron activated the GABAb receptors on hundreds of excitatory neurons in the immediate area. Activating this receptor suppressed the excitatory neurons, which prevented them from creating and strengthening synapses – and made them invisible to researchers.
The researchers next plan to see if the somatostatin cells behave similarly in other areas of the brain. If they do, it could represent a novel target for studying and improving learning and memory.
Erika E. Fanselow, a research biologist formerly with Carnegie Mellon and the CNBC, also contributed to this paper.
As the birthplace of artificial intelligence and cognitive psychology, Carnegie Mellon has been a leader in the study of brain and behavior for more than 50 years. The university has created some of the first cognitive tutors, helped to develop the Jeopardy-winning Watson, founded a groundbreaking doctoral program in neural computation, and completed cutting-edge work in understanding the genetics of autism. Building on its strengths in biology, computer science, psychology, statistics and engineering, CMU recently launched BrainHubSM, a global initiative that focuses on how the structure and activity of the brain give rise to complex behaviors.
About Carnegie Mellon University: Carnegie Mellon (www.cmu.edu) is a private, internationally ranked research university with programs in areas ranging from science, technology and business, to public policy, the humanities and the arts. More than 13,000 students in the university’s seven schools and colleges benefit from a small student-to-faculty ratio and an education characterized by its focus on creating and implementing solutions for real problems, interdisciplinary collaboration and innovation. A global university, Carnegie Mellon has campuses in Pittsburgh, Pa., California’s Silicon Valley and Qatar, and programs in Africa, Asia, Australia, Europe and Mexico.