Differential timing of a conserved transcriptional network underlies divergent cortical projection routes across mammalian brain evolution

A unique combination of transcription factor expression and projection neuron identity demarcates each layer of the cerebral cortex. During mouse and human cortical development, the transcription factor CTIP2 specifies neurons that project subcerebrally, while SATB2 specifies neuronal projections vi...

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Bibliographic Details
Published in:Proceedings of the National Academy of Sciences - PNAS 2020-05, Vol.117 (19), p.10554-10564
Main Authors: Paolino, Annalisa, Fenlon, Laura R., Kozulin, Peter, Haines, Elizabeth, Lim, Jonathan W. C., Richards, Linda J., Suárez, Rodrigo
Format: Article
Language:English
Subjects:
Animals
Anterior commissure
Axons - metabolism
Biological Evolution
Biological Sciences
Brain - metabolism
Cerebral cortex
Cerebral Cortex - metabolism
Corpus callosum
Corpus Callosum - metabolism
Corpus Callosum - physiology
Divergence
DNA-Binding Proteins - metabolism
Egg laying
Eutheria - genetics
Evolution, Molecular
Gene expression
Gene Expression Regulation, Developmental - genetics
Gene Regulatory Networks - genetics
Hemispheres
Homology
Humans
Mammals
Mammals - genetics
Marsupialia - genetics
Marsupials
Matrix Attachment Region Binding Proteins - genetics
Matrix Attachment Region Binding Proteins - metabolism
Mice
Neural Pathways - physiology
Neurons
Neurons - metabolism
Projection
Repressor Proteins - genetics
Repressor Proteins - metabolism
Routing (telecommunications)
Structure-function relationships
Transcription factors
Transcription Factors - genetics
Transcription Factors - metabolism
Tumor Suppressor Proteins - genetics
Tumor Suppressor Proteins - metabolism
Wiring
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Summary:A unique combination of transcription factor expression and projection neuron identity demarcates each layer of the cerebral cortex. During mouse and human cortical development, the transcription factor CTIP2 specifies neurons that project subcerebrally, while SATB2 specifies neuronal projections via the corpus callosum, a large axon tract connecting the two neocortical hemispheres that emerged exclusively in eutherian mammals. Marsupials comprise the sister taxon of eutherians but do not have a corpus callosum; their intercortical commissural neurons instead project via the anterior commissure, similar to egg-laying monotreme mammals. It remains unknown whether divergent transcriptional networks underlie these cortical wiring differences. Here, we combine birth-dating analysis, retrograde tracing, gene overexpression and knockdown, and axonal quantification to compare the functions of CTIP2 and SATB2 in neocortical development, between the eutherian mouse and the marsupial fat-tailed dunnart. We demonstrate a striking degree of structural and functional homology, whereby CTIP2 or SATB2 of either species is sufficient to promote a subcerebral or commissural fate, respectively. Remarkably, we reveal a substantial delay in the onset of developmental SATB2 expression in mice as compared to the equivalent stage in dunnarts, with premature SATB2 overexpression in mice to match that of dunnarts resulting in a marsupial-like projection fate via the anterior commissure. Our results suggest that small alterations in the timing of regulatory gene expression may underlie interspecies differences in neuronal projection fate specification.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.1922422117