Abstract

The vertebrate retina is a powerful model system for addressing mechanistic questions of how individual cell subtypes are specified during development. We have found that the homeodomain transcription factor Lhx2 regulates the development and function of retinal Muller glia. Loss of function of Lhx2 results in dramatic defects in Muller glial development. Furthermore, selective deletion of Lhx2 in mature Muller glia leads to altered expression of many genes known to be expressed in Muller glia. Furthermore, these cells becoming constitutively reactive following loss of Lhx2, mimicking the effect of injury. We propose to both identify the genes which are directly regulated by Lhx2 in mature Muller glia, and to examine the consequences of this constitutive reactivity in both uninjured and injured retina. We will determine whether mice that selectively lack Lhx2 expression in mature Muller glia demonstrate a gene expression profile that is fully characteristic of a reactive state, and determine whether Lhx2 directly represses expression of genes expressed in activated glia. Since glial reactivity has been proposed to regulate photoreceptor viability, we will conduct a detailed examination of cellular changes that occur throughout the lifespan of mutant animals following deletion of Lhx2 in mature Muller glia. Furthermore, we will determine the effects of mature glia- specific deletion of Lhx2 in models of photoreceptor injury. Finally, we will characterize any molecular signals released from Lhx2-deficient glia that regulate photoreceptor survival.

Public Health Relevance

The vertebrate retina is a powerful model system for addressing mechanistic questions of how individual cell subtypes are specified during development. We have found that the homeodomain transcription factor Lhx2 regulates the expression of genes in retinal Muller glia, which provide support and sustenance to neurons of the retina. Furthermore, selective deletion of Lhx2 in mature Muller glia leads to these cells becoming constitutively reactive, mimicking the effect of injury. We propose to identify the molecular targets of Lhx2 in Muller glia. We will also investigate the functional consequences of Lhx2 deletion in mature Muller glia, and determine whether constitutive glial reactivity regulates photoreceptor survival following retinal injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY020560-02
Application #
8204536
Study Section
Special Emphasis Panel (ZRG1-CB-G (90))
Program Officer
Greenwell, Thomas
Project Start
2010-12-01
Project End
2013-11-30
Budget Start
2011-12-01
Budget End
2012-11-30
Support Year
2
Fiscal Year
2012
Total Cost
$410,000
Indirect Cost
$160,000

  Institution

Name
Johns Hopkins University
Department
Neurosciences
Type
Schools of Medicine
DUNS #
001910777
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

de Melo, Jimmy; Blackshaw, Seth (2018) In Vivo Electroporation of Developing Mouse Retina. Methods Mol Biol 1715:101-111
de Melo, Jimmy; Clark, Brian S; Venkataraman, Anand et al. (2018) Ldb1- and Rnf12-dependent regulation of Lhx2 controls the relative balance between neurogenesis and gliogenesis in the retina. Development 145:
Remez, Liv Aleen; Onishi, Akishi; Menuchin-Lasowski, Yotam et al. (2017) Pax6 is essential for the generation of late-born retinal neurons and for inhibition of photoreceptor-fate during late stages of retinogenesis. Dev Biol 432:140-150
Clark, Brian S; Blackshaw, Seth (2017) Understanding the Role of lncRNAs in Nervous System Development. Adv Exp Med Biol 1008:253-282
Liu, Sheng; Zibetti, Cristina; Wan, Jun et al. (2017) Assessing the model transferability for prediction of transcription factor binding sites based on chromatin accessibility. BMC Bioinformatics 18:355
Gueta, Keren; David, Ahuvit; Cohen, Tsadok et al. (2016) The stage-dependent roles of Ldb1 and functional redundancy with Ldb2 in mammalian retinogenesis. Development 143:4182-4192
de Melo, Jimmy; Clark, Brian S; Blackshaw, Seth (2016) Multiple intrinsic factors act in concert with Lhx2 to direct retinal gliogenesis. Sci Rep 6:32757
Thein, Thuzar; de Melo, Jimmy; Zibetti, Cristina et al. (2016) Control of lens development by Lhx2-regulated neuroretinal FGFs. Development 143:3994-4002
de Melo, Jimmy; Zibetti, Cristina; Clark, Brian S et al. (2016) Lhx2 Is an Essential Factor for Retinal Gliogenesis and Notch Signaling. J Neurosci 36:2391-405
Mattar, Pierre; Ericson, Johan; Blackshaw, Seth et al. (2015) A conserved regulatory logic controls temporal identity in mouse neural progenitors. Neuron 85:497-504

Showing the most recent 10 out of 16 publications