Literature DB >> 33135183

Identification of retinal ganglion cell types and brain nuclei expressing the transcription factor Brn3c/Pou4f3 using a Cre recombinase knock-in allele.

Nadia Parmhans1, Anne Drury Fuller1, Eileen Nguyen1, Katherine Chuang1, David Swygart2, Sophia Rose Wienbar2, Tyger Lin1, Zbynek Kozmik3, Lijin Dong4, Gregory William Schwartz2, Tudor Constantin Badea1.   

Abstract

Members of the POU4F/Brn3 transcription factor family have an established role in the development of retinal ganglion cell (RGCs) types, the main transducers of visual information from the mammalian eye to the brain. Our previous work using sparse random recombination of a conditional knock-in reporter allele expressing alkaline phosphatase (AP) and intersectional genetics had identified three types of Brn3c positive (Brn3c+ ) RGCs. Here, we describe a novel Brn3cCre mouse allele generated by serial Dre to Cre recombination and use it to explore the expression overlap of Brn3c with Brn3a and Brn3b and the dendritic arbor morphologies and visual stimulus response properties of Brn3c+ RGC types. Furthermore, we explore brain nuclei that express Brn3c or receive input from Brn3c+ neurons. Our analysis reveals a much larger number of Brn3c+ RGCs and more diverse set of RGC types than previously reported. Most RGCs expressing Brn3c during development are still Brn3c positive in the adult, and all express Brn3a while only about half express Brn3b. Genetic Brn3c-Brn3b intersection reveals an area of increased RGC density, extending from dorsotemporal to ventrolateral across the retina and overlapping with the mouse binocular field of view. In addition, we report a Brn3c+ RGC projection to the thalamic reticular nucleus, a visual nucleus that was not previously shown to receive retinal input. Furthermore, Brn3c+ neurons highlight a previously unknown subdivision of the deep mesencephalic nucleus. Thus, our newly generated allele provides novel biological insights into RGC type classification, brain connectivity, and cytoarchitectonic.
© 2021 Wiley Periodicals LLC.

Entities:  

Keywords:  Brn3c; Cre recombinase; Pou4f3; deep mesencephalic nucleus; periaqueductal gray; retinal ganglion cells; superior colliculus; thalamic reticular nucleus; transcription factor

Mesh:

Substances:

Year:  2020        PMID: 33135183      PMCID: PMC8009822          DOI: 10.1002/cne.25065

Source DB:  PubMed          Journal:  J Comp Neurol        ISSN: 0021-9967            Impact factor:   3.028


  121 in total

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  2 in total

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