AI Article Synopsis
- Neuronal subtypes have different synaptic structures and functions, but the gene expression differences behind these variations are not well understood.
- Researchers used Patch-seq RNA profiling on two types of Drosophila motoneurons to explore these molecular pathways.
- They found that tonic motoneurons have weaker synapses on single muscles, while phasic motoneurons have stronger synapses on multiple muscles, with distinct genetic signatures influencing their unique functions and structures.
Article Abstract
Although neuronal subtypes display unique synaptic organization and function, the underlying transcriptional differences that establish these features are poorly understood. To identify molecular pathways that contribute to synaptic diversity, single-neuron Patch-seq RNA profiling was performed on Drosophila tonic and phasic glutamatergic motoneurons. Tonic motoneurons form weaker facilitating synapses onto single muscles, while phasic motoneurons form stronger depressing synapses onto multiple muscles. Super-resolution microscopy and in vivo imaging demonstrated that synaptic active zones in phasic motoneurons are more compact and display enhanced Ca influx compared with their tonic counterparts. Genetic analysis identified unique synaptic properties that mapped onto gene expression differences for several cellular pathways, including distinct signaling ligands, post-translational modifications, and intracellular Ca buffers. These findings provide insights into how unique transcriptomes drive functional and morphological differences between neuronal subtypes.
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| http://dx.doi.org/10.1016/j.neuron.2023.07.019 | DOI Listing |
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