Visual Neuroscience

  • Visual Neuroscience (2006), 23 : pp 917-929
  • Copyright © 2006 Cambridge University Press
  • DOI: 10.1017/S095252380623027X (About DOI)
  • Published online: 30 January 2007

Table of Contents - 2006 - Volume 23, Issue 06  


The transcription factor Nr2e3 functions in retinal progenitors to suppress cone cell generation

NEENA B.  HAIDER  a1 a2 c1 , PAUL  DEMARCO  a3 a4 , ARNE M.  NYSTUEN  a1 , XIAONA  HUANG  a1 , RICHARD S.  SMITH  a2 , MAUREEN A.  MCCALL  a3 , JÜRGEN K.  NAGGERT  a2 and PATSY M.  NISHINA  a2
a1 Departments of Genetics, Cell Biology, Anatomy and Ophthalmology and Visual Sciences, University of Nebraska Medical Center, Omaha, Nebraska
a2 The Jackson Laboratory, Bar Harbor, Maine
a3 Departments of Psychological & Brain Sciences and Ophthalmology & Visual Sciences, University of Louisville, Louisville, Kentucky
a4 Louisville VA Medical Center, Louisville, Kentucky

Article author query
haider nb   [Google Scholar] 
demarco p   [Google Scholar] 
nystuen am   [Google Scholar] 
huang x   [Google Scholar] 
smith rs   [Google Scholar] 
mccall ma   [Google Scholar] 
naggert jk   [Google Scholar] 
nishina pm   [Google Scholar] 
 

Abstract

The transcription factor Nr2e3 is an essential component for development and specification of rod and cone photoreceptors; however, the mechanism through which it acts is not well understood. In this study, we use Nr2e3rd7/rd7 mice that harbor a mutation in Nr2e3, to serve as a model for the human retinal disease Enhanced S Cone Syndrome. Our studies reveal that NR2E3 is expressed in late retinal progenitors and differentiating photoreceptors of the developing retina and localized to the cell bodies of mature rods and cones. In particular, we demonstrate that the abnormal increase in cone photoreceptors observed in Nr2e3rd7/rd7 mice arise from ectopic mitotic progenitor cells that are present in the outer nuclear layer of the mature Nr2e3rd7/rd7 retina. A prolonged phase of proliferation is observed followed by abnormal retinal lamination with fragmented and disorganized photoreceptor synapses that result in a progressive loss of rod and cone function. An extended and pronounced wave of apoptosis is also detected at P30 and temporally correlates with the phase of prolonged proliferation. Approximately twice as many apoptotic cells were detected compared to proliferating cells. This wave of apoptosis appears to affect both rod and cone cells and thus may account for the concurrent loss of rod and cone function. We further show that Nr2e3rd7/rd7 cones do not express rod specific genes and Nr2e3rd7/rd7 rods do not express cone specific genes. Our studies suggest that, based on its temporal and spatial expression, NR2E3 acts simultaneously in different cell types: in late mitotic progenitors, newly differentiating post mitotic cells, and mature rods and cones. In particular, this study reveals the function of NR2E3 in mitotic progenitors is to repress the cone generation program. NR2E3 is thus one of the few genes known to influence the competency of retinal progenitors while simultaneously directing the rod and cone differentiation.

(Received March 31 2006)
(Accepted October 20 2006)


Key Words: Nr2e3; Cell proliferation; Photoreceptors; Retinal development; Retinal progenitors.

Correspondence:
c1 Address Correspondence and reprint requests to: Neena B. Haider, Department of Genetics, Cell Biology, and Anatomy and Ophthalmology and Visual Sciences, 985805 Nebraska Medical Center, Omaha, NE 68198. E-mail: nhaidern@unmc.edu

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