Biomedical engineers have developed a way to deliver drugs to specific types of neurons in the brain, providing extraordinary ability to study neurological diseases and also a promising pathway to treat them.
Drugs are the tool of choice for studying the connections between neurons and continue to be the mainstream treatment for neurological disease. But a major drawback in both endeavors is that the drugs affect all types of neurons, complicating the study of how cell receptors in the synapse the gap between neurons work in an intact brain, and how their manipulation can lead to clinical benefits and side effects
DART: Drugs acutely restricted by tethering DART may overcome these limitations. DART offers researchers the first opportunity to test what happens when a drug is targeted exclusively to one cell type. Parkinson’s Disease are controlled by the AMPA receptor (AMPAR)—a synaptic protein that enables neurons to receive fast incoming signals from other neurons in the brain. The results reveal why a recent clinical trial of an AMPAR-blocking drug failed and offer a new approach to using the pharmaceutical.
The paper appeared online on April 7, 2017 in the journal Science.
“This study marks a major milestone in behavioral neuropharmacology,” said Michael Tadross, assistant professor of biomedical engineering, who is in the process of moving his laboratory from the HHMI Janelia Research Campus to Duke. “The insights we gained in studying Parkinson’s mice were unexpected and could not have been obtained with any previous method.”
Mechanisms behind:
DART works by genetically programming a specific cell type to express a sort of GPS beacon. The “beacon” is an enzyme borrowed from bacteria that is inert—it does nothing more than sit on the cell surface. Nothing, that is, until researchers deliver drugs loaded with a special homing device.
Researchers administer these drugs at such low doses that they do not affect other cells. Because the homing system is so efficient, however, the drug is captured by the tagged cells’ surface, accumulating within minutes to concentrations that are 100 to 1,000 times higher than anywhere else.
The experiment:
Using a mouse model of Parkinson’s disease, Tadross and colleagues attached the homing signal beacon to two types of neurons found in the basal ganglia—the region of the brain responsible for motor control.
D1 neurons are believed to give a ‘go’ command. D2 neurons are thought to do the opposite, providing commands to stop movements.
Using DART, Tadross delivered an AMPAR-blocking pharmaceutical to only D1-neurons, only D2-neurons, or both. When delivered to both cell types simultaneously, the drugs improved only one of several components of motor dysfunction—mirroring the lackluster results of recent human clinical trials. The team then found that delivering the drug to only the D1/” go” neurons did absolutely nothing. Surprisingly, however, by targeting the same drug to D2/” stop” neurons, the mice’s movements became more frequent, faster, fluid and linear—in other words, much closer to normal.
While the drug stops neurons from receiving certain incoming signals, it does not completely shut them down. This nuance is particularly important for a subset of the D2 neurons that have two prominent forms of firing. With DART, these components could be separately manipulated, providing the first evidence that Parkinson’s motor deficits are attributable to the AMPAR-based component of firing in these cells. Tadross said this level of nuance could not have been obtained with prior cell type-specific methods that completely shut neurons down.
These experiments have led to the understanding about the synaptic basis of circuit dysfunction in Parkinson’s disease. Tadross is already looking into the possibility of converting this into a new therapy for delivering drugs.
“All too often in basic science, approaches are developed that may ‘one day’ make a difference to human health,” he said. “At Duke, there’s a palpable emphasis on providing new treatments to people as quickly as possible. I’m very excited that in this environment, my lab can work collaboratively with scientists, physicians, and biotech to solve the real-world challenges involved.”
This research was funded by the Howard Hughes Medical Institute.