Islet-1 Controls the Differentiation of Retinal Bipolar and Cholinergic Amacrine Cells

doi:10.1523/JNEUROSCI.3951-07.2007

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The Journal of Neuroscience, November 14, 2007, 27(46):12707-12720; doi:10.1523/JNEUROSCI.3951-07.2007

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Development/Plasticity/Repair
Islet-1 Controls the Differentiation of Retinal Bipolar and Cholinergic Amacrine Cells
Yasser Elshatory,¹ Drew Everhart,² Min Deng,¹ Xiaoling Xie,¹ Robert B. Barlow,² and Lin Gan¹
¹Department of Ophthalmology, University of Rochester, Rochester, New York 14642, and ²Department of Ophthalmology, State University of New York Upstate Medical Center, Syracuse, New York 13210
Correspondence should be addressed to Dr. Lin Gan, 601 Elmwood Avenue, Box 645, Rochester, NY 14642. Email: lin_gan{at}urmc.rochester.edu
Whereas the mammalian retina possesses a repertoire of factorsknown to establish general retinal cell types, these factorsalone cannot explain the vast diversity of neuronal subtypes.In other CNS regions, the differentiation of diverse neuronalpools is governed by coordinately acting LIM-homeodomain proteinsincluding the Islet-class factor Islet-1 (Isl1). We report thatdeletion of Isl1 profoundly disrupts retinal function as assessedby electroretinograms and vision as assessed by optomotor behavior.These deficits are coupled with marked reductions in matureON- and OFF-bipolar (>76%), cholinergic amacrine (93%), andganglion (71%) cells. Mosaic deletion of Isl1 permitted a chimericanalysis of "wild-type" cells in a predominantly Isl1-null environment,demonstrating a cell-autonomous role for Isl1 in rod bipolarand cholinergic amacrine development. Furthermore, the effectson bipolar cell development appear to be dissociable from thepreceding retinal ganglion cell loss, because Pou4f2-null miceare devoid of similar defects in bipolar cell marker expression.Expression of the ON- and OFF-bipolar cell differentiation factorsBhlhb4 and Vsx1, respectively, requires the presence of Isl1,whereas the early bipolar cell marker Prox1 initially did not.Thus, Isl1 is required for engaging bipolar differentiationpathways but not for general bipolar cell specification. Spatiotemporalexpression analysis of additional LIM-homeobox genes identifiesa LIM-homeobox gene network during bipolar cell developmentthat includes Lhx3 and Lhx4. We conclude that Isl1 has an indispensablerole in retinal neuron differentiation within restricted cellpopulations and this function may reflect a broader role forother LIM-homeobox genes in retinal development, and perhapsin establishing neuronal subtypes.

Key words: retina; retinal bipolar cell; transcription factor; differentiation; ERG (electroretinogram); optomotor behavior; amacrine; retinal ganglion cell

Received March 18, 2007; revised Oct. 3, 2007; accepted Oct. 6, 2007.

Correspondence should be addressed to Dr. Lin Gan, 601 Elmwood Avenue, Box 645, Rochester, NY 14642. Email: lin_gan{at}urmc.rochester.edu

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