Abstract

The long-term objective of this proposal is to understand the molecular events that lead to fate commitment and differentiation of different cell types during mammalian retinogenesis. The amacrine and horizontal cells are two classes of important interneurons that modulate and integrate visual signals in the retinal circuitry. Despite their physiological significance, however, the molecular bases underlying their development remain poorly understood at present. In this application, experiments are proposed that will focus on Foxn4, a forkhead/winged helix transcription factor that is expressed in a subset of dividing retinal progenitor cells characteristic of the subset with a fate biased toward amacrine and horizontal cells. Based on our preliminary studies it has been speculated that Fonx4 may play a key role in competence acquisition and fate commitment of these two cell types. The studies outlined in this proposal are designed to provide an integrated approach toward a comprehensive understanding of the biological function of Foxn4 during retinogenesis.
Four specific aims will be pursued: i) to investigate the role of Foxn4 during retinal development by overexpression in progenitor cells. These studies aim to explore the function of Foxn4 during mammalian retinogenesis using a gain-of-function approach involving retrovirus-mediated overexpression of Foxn4 in the mouse retina; ii) to study the biological function of Foxn4 during retinal development by targeted gene disruption. The proposed experiments aim to uncover the role of Foxn4 during retinogenesis using a loss-of-function approach involving the production and characterization of Foxn4 knockout mice; iii) to analyze the relationship between Foxn4 and other retinogenic factors mediating amacrine and horizontal cell development. These studies aim to test the hypothesis that Foxn4 alone or in combination with a redundant factor, may control the genesis of amacrine and horizontal cells by activating the expression of retinogenic factors involved in the specification of these two cell types; and iv) to map the fate of Foxn4-expressing retinal progenitors. The goal is to use the Cre-loxP fate-mapping strategy to test the hypothesis that the subset of Foxn4-expressing retinal progenitors may represent those with a fate biased toward amacrine and horizontal cells. Taken together, these proposed studies are expected to provide important novel insights into the genetic regulatory networks that govern the development of different retinal cell types and may provide the foundation for better understanding and treatment of neuroretinal diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY015777-02
Application #
7059891
Study Section
Biology and Diseases of the Posterior Eye Study Section (BDPE)
Program Officer
Hunter, Chyren
Project Start
2005-05-01
Project End
2008-04-30
Budget Start
2006-05-01
Budget End
2007-04-30
Support Year
2
Fiscal Year
2006
Total Cost
$261,012
Indirect Cost

  Institution

Name
University of Medicine & Dentistry of NJ
Department
Pediatrics
Type
Schools of Medicine
DUNS #
617022384
City
Piscataway
State
NJ
Country
United States
Zip Code
08854

  Publications

Li, Shengguo; Xiang, Mengqing (2011) Foxn4 influences alveologenesis during lung development. Dev Dyn 240:1512-7
Pöschl, J; Lorenz, A; Hartmann, W et al. (2011) Expression of BARHL1 in medulloblastoma is associated with prolonged survival in mice and humans. Oncogene 30:4721-30
Li, Shengguo; Misra, Kamana; Xiang, Mengqing (2010) A Cre transgenic line for studying V2 neuronal lineages and functions in the spinal cord. Genesis 48:667-72
Jin, Kangxin; Jiang, Haisong; Mo, Zeqian et al. (2010) Early B-cell factors are required for specifying multiple retinal cell types and subtypes from postmitotic precursors. J Neurosci 30:11902-16
Jiang, Haisong; Xiang, Mengqing (2009) Subtype specification of GABAergic amacrine cells by the orphan nuclear receptor Nr4a2/Nurr1. J Neurosci 29:10449-59
Qiu, Feng; Jiang, Haisong; Xiang, Mengqing (2008) A comprehensive negative regulatory program controlled by Brn3b to ensure ganglion cell specification from multipotential retinal precursors. J Neurosci 28:3392-403
Collin, Rob W J; Chellappa, Ramesh; Pauw, Robert-Jan et al. (2008) Missense mutations in POU4F3 cause autosomal dominant hearing impairment DFNA15 and affect subcellular localization and DNA binding. Hum Mutat 29:545-54
Del Barrio, Marta G; Taveira-Marques, Raquel; Muroyama, Yuko et al. (2007) A regulatory network involving Foxn4, Mash1 and delta-like 4/Notch1 generates V2a and V2b spinal interneurons from a common progenitor pool. Development 134:3427-36
Fujitani, Yoshio; Fujitani, Shuko; Luo, Huijun et al. (2006) Ptf1a determines horizontal and amacrine cell fates during mouse retinal development. Development 133:4439-50
Li, Shengguo; Misra, Kamana; Matise, Michael P et al. (2005) Foxn4 acts synergistically with Mash1 to specify subtype identity of V2 interneurons in the spinal cord. Proc Natl Acad Sci U S A 102:10688-93