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시냅스뇌질환연구단
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Transcriptional diversity in specific synaptic gene sets discriminates cortical neuronal identity

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Title
Transcriptional diversity in specific synaptic gene sets discriminates cortical neuronal identity
Author(s)
Roig Adam, Amparo; Martínez-López, José A.; van der Spek, Sophie J. F.; Achsel, Tilmann; Andres-Alonso, Maria; Bagni, Claudia; Bayés, Àlex; Biederer, Thomas; Brose, Nils; Chua, John Jia En; Coba, Marcelo P.; Cornelisse, L. Niels; de Juan-Sanz, Jaime; Goldschmidt, Hana L.; Gundelfinger, Eckart D.; Huganir, Richard L.; Imig, Cordelia; Jahn, Reinhard; Hwajin Jung; Kaeser, Pascal S.; Eunjoon Kim; Koopmans, Frank; Kreutz, Michael R.; Lipstein, Noa; MacGillavry, Harold D.; McPherson, Peter S.; O’Connor, Vincent; Pielot, Rainer; Ryan, Timothy A.; Sala, Carlo; Sheng, Morgan; Smalla, Karl-Heinz; Thomas, Paul D.; Toonen, Ruud F.; van Weering, Jan R. T.; Verpelli, Chiara; Sullivan, Patrick F.; Smit, August B.; Verhage, Matthijs; Hjerling-Leffler, Jens
Publication Date
2023-05
Journal
Biology Direct, v.18, no.1
Publisher
BioMed Central Ltd
Abstract
Synapse diversity has been described from different perspectives, ranging from the specific neurotransmitters released, to their diverse biophysical properties and proteome profiles. However, synapse diversity at the transcriptional level has not been systematically identified across all synapse populations in the brain. To quantify and identify specific synaptic features of neuronal cell types we combined the SynGO (Synaptic Gene Ontology) database with single-cell RNA sequencing data of the mouse neocortex. We show that cell types can be discriminated by synaptic genes alone with the same power as all genes. The cell type discriminatory power is not equally distributed across synaptic genes as we could identify functional categories and synaptic compartments with greater cell type specific expression. Synaptic genes, and specific SynGO categories, belonged to three different types of gene modules: gradient expression over all cell types, gradient expression in selected cell types and cell class- or type-specific profiles. This data provides a deeper understanding of synapse diversity in the neocortex and identifies potential markers to selectively identify synapses from specific neuronal populations. © 2023, The Author(s).
URI
https://pr.ibs.re.kr/handle/8788114/13440
DOI
10.1186/s13062-023-00372-y
ISSN
1745-6150
Appears in Collections:
Center for Synaptic Brain Dysfunctions(시냅스 뇌질환 연구단) > 1. Journal Papers (저널논문)
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