The nuclear hormone receptor gene Nr2c1 (Tr2) is a critical regulator of early retina cell patterning.
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BORIS DOI
Publisher DOI
PubMed ID
28551284
Description
Nuclear hormone receptors play a major role in the development of many tissues. This study uncovers a novel role for testicular receptor 2 (Tr2, Nr2c1) in defining the early phase of retinal development and regulating normal retinal cell patterning and topography. The mammalian retina undergoes an overlapping yet biphasic period of development to generate all seven retinal cell types. We discovered that Nr2c1 expression coincides with development of the early retinal cells. Loss of Nr2c1 causes a severe vision deficit and impacts early, but not late retina cell types. Retinal cone cell topography is disrupted with an increase in displaced amacrine cells. Additionally, genetic background significantly impacts phenotypic outcome of cone photoreceptor cells but not amacrine cells. Chromatin-IP experiments reveal NR2C1 regulates early cell transcription factors that regulate retinal progenitor cells during development, including amacrine (Satb2) and cone photoreceptor regulators thyroid and retinoic acid receptors. This study supports a role for Nr2c1 in defining the biphasic period of retinal development and specifically influencing the early phase of retinal cell fate.
Date of Publication
2017-09-01
Publication Type
Article
Keyword(s)
Cell proliferation Cone cell patterning Development Nuclear hormone receptors Retina
Language(s)
en
Contributor(s)
Olivares, Ana Maria | |
Han, Yinan | |
Soto, David | |
Flattery, Kyle | |
Marini, Joseph | |
Mollema, Nissa | |
Haider, Ali | |
DeAngelis, Margaret M | |
Haider, Neena B |
Additional Credits
Series
Developmental biology
Publisher
Elsevier
ISSN
0012-1606
Related URL(s)
https://boris.unibe.ch/id/eprint/126327
Access(Rights)
open.access