Journal
DISEASE MODELS & MECHANISMS
Volume 15, Issue 8, Pages -Publisher
COMPANY BIOLOGISTS LTD
DOI: 10.1242/dmm.049507
Keywords
Neuronal development; Optic tectum; Synaptogenesis
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Funding
- Purdue Institute for Integrative Neuroscience, Purdue University
- Purdue University
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This study developed a genetic labeling system to study dendritic spine development in larval zebrafish, revealing the concurrent growth of PyrN dendrites and spine formation. It also found pronounced defects in dendrite growth and spine stabilization in PyrNs of fmr1 mutant zebrafish.
Dendritic spines are the principal site of excitatory synapse formation in the human brain. Several neurodevelopmental disorders cause spines to develop abnormally, resulting in altered spine number and morphology. Although spine development has been thoroughly characterized in the mammalian brain, spines are not unique to mammals. We have developed a genetic system in zebrafish to enable high-resolution in vivo imaging of spine dynamics during larval development. Although spiny neurons are rare in the larval zebrafish, pyramidal neurons (PyrNs) of the zebrafish tectum form an apical dendrite containing a dense array of dendritic spines. To characterize dendritic spine development, we performed mosaic genetic labeling of individual PyrNs labeled by an id2b:gal4 transgene. Our findings identify a developmental period during which PyrN dendrite growth is concurrent with spine formation. Throughout this period, motile, transient filopodia gradually transform into stable spines containing postsynaptic specializations. The utility of this system to study neurodevelopmental disorders was validated by examining spine development in fmr1 mutant zebrafish, a model of fragile X syndrome. PyrNs in fmr1 mutants exhibited pronounced defects in dendrite growth and spine stabilization. Taken together, these findings establish a genetic labeling system to study dendritic spine development in larval zebrafish. In the future, this system could be combined with high-throughput screening approaches to identify genes and drug targets that regulate spine formation.
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