AI Article Synopsis
- Behavior is influenced by molecular, cellular, and circuit factors, making it challenging to manipulate proteins in specific cell types due to their widespread expression.
- The DART technique uses targeted pharmacology to deliver drugs specifically to defined cells while preserving the native targets, enabling faster and more precise studies.
- In experiments with parkinsonian mice, the DART AMPAR antagonist revealed that motor deficits are linked to specific neuronal activity, demonstrating the effectiveness of DART for studying different cellular targets.
Article Abstract
Behavior has molecular, cellular, and circuit determinants. However, because many proteins are broadly expressed, their acute manipulation within defined cells has been difficult. Here, we combined the speed and molecular specificity of pharmacology with the cell type specificity of genetic tools. DART (drugs acutely restricted by tethering) is a technique that rapidly localizes drugs to the surface of defined cells, without prior modification of the native target. We first developed an AMPAR antagonist DART, with validation in cultured neuronal assays, in slices of mouse dorsal striatum, and in behaving mice. In parkinsonian animals, motor deficits were causally attributed to AMPARs in indirect spiny projection neurons (iSPNs) and to excess phasic firing of tonically active interneurons (TANs). Together, iSPNs and TANs (i.e., D2 cells) drove akinesia, whereas movement execution deficits reflected the ratio of AMPARs in D2 versus D1 cells. Finally, we designed a muscarinic antagonist DART in one iteration, demonstrating applicability of the method to diverse targets.
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| http://dx.doi.org/10.1126/science.aaj2161 | DOI Listing |
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