The Trim family of genes and the retina: Expression and functional characterization.

To better understand the mechanisms that govern the development of retinal neurons, it is critical to gain additional insight into the specific intrinsic factors that control cell fate decisions and neuronal maturation. In the developing mouse retina, Atoh7, a highly conserved transcription factor,...

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Main Authors: Rebecca Chowdhury, Lauren A Laboissonniere, Andrea K Wester, Madison Muller, Jeffrey M Trimarchi
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC6135365?pdf=render
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spelling doaj-09887f4e75414cb6883602253da9e1a02020-11-25T00:07:59ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-01139e020286710.1371/journal.pone.0202867The Trim family of genes and the retina: Expression and functional characterization.Rebecca ChowdhuryLauren A LaboissonniereAndrea K WesterMadison MullerJeffrey M TrimarchiTo better understand the mechanisms that govern the development of retinal neurons, it is critical to gain additional insight into the specific intrinsic factors that control cell fate decisions and neuronal maturation. In the developing mouse retina, Atoh7, a highly conserved transcription factor, is essential for retinal ganglion cell development. Moreover, Atoh7 expression in the developing retina occurs during a critical time period when progenitor cells are in the process of making cell fate decisions. We performed transcriptome profiling of Atoh7+ individual cells isolated from mouse retina. One of the genes that we found significantly correlated with Atoh7 in our transcriptomic data was the E3 ubiquitin ligase, Trim9. The correlation between Trim9 and Atoh7 coupled with the expression of Trim9 in the early mouse retina led us to hypothesize that this gene may play a role in the process of cell fate determination. To address the role of Trim9 in retinal development, we performed a functional analysis of Trim9 in the mouse and did not detect any morphological changes in the retina in the absence of Trim9. Thus, Trim9 alone does not appear to be involved in cell fate determination or early ganglion cell development in the mouse retina. We further hypothesize that the reason for this lack of phenotype may be compensation by one of the many additional TRIM family members we find expressed in the developing retina.http://europepmc.org/articles/PMC6135365?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Rebecca Chowdhury
Lauren A Laboissonniere
Andrea K Wester
Madison Muller
Jeffrey M Trimarchi
spellingShingle Rebecca Chowdhury
Lauren A Laboissonniere
Andrea K Wester
Madison Muller
Jeffrey M Trimarchi
The Trim family of genes and the retina: Expression and functional characterization.
PLoS ONE
author_facet Rebecca Chowdhury
Lauren A Laboissonniere
Andrea K Wester
Madison Muller
Jeffrey M Trimarchi
author_sort Rebecca Chowdhury
title The Trim family of genes and the retina: Expression and functional characterization.
title_short The Trim family of genes and the retina: Expression and functional characterization.
title_full The Trim family of genes and the retina: Expression and functional characterization.
title_fullStr The Trim family of genes and the retina: Expression and functional characterization.
title_full_unstemmed The Trim family of genes and the retina: Expression and functional characterization.
title_sort trim family of genes and the retina: expression and functional characterization.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description To better understand the mechanisms that govern the development of retinal neurons, it is critical to gain additional insight into the specific intrinsic factors that control cell fate decisions and neuronal maturation. In the developing mouse retina, Atoh7, a highly conserved transcription factor, is essential for retinal ganglion cell development. Moreover, Atoh7 expression in the developing retina occurs during a critical time period when progenitor cells are in the process of making cell fate decisions. We performed transcriptome profiling of Atoh7+ individual cells isolated from mouse retina. One of the genes that we found significantly correlated with Atoh7 in our transcriptomic data was the E3 ubiquitin ligase, Trim9. The correlation between Trim9 and Atoh7 coupled with the expression of Trim9 in the early mouse retina led us to hypothesize that this gene may play a role in the process of cell fate determination. To address the role of Trim9 in retinal development, we performed a functional analysis of Trim9 in the mouse and did not detect any morphological changes in the retina in the absence of Trim9. Thus, Trim9 alone does not appear to be involved in cell fate determination or early ganglion cell development in the mouse retina. We further hypothesize that the reason for this lack of phenotype may be compensation by one of the many additional TRIM family members we find expressed in the developing retina.
url http://europepmc.org/articles/PMC6135365?pdf=render
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