Role of the Barhl2 homeobox gene in the specification of glycinergic amacrine cells

doi:10.1242/dev.01071

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Development ePress online publication date 3 Mar 2004
doi: 10.1242/dev.01071

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Research article

Role of the Barhl2 homeobox gene in the specification of glycinergic amacrine cells

Zeqian Mo, Shengguo Li, Xuejie Yang, and Mengqing Xiang^*
^* Author for correspondence (e-mail: xiang{at}cabm.rutgers.edu)

The mammalian retina contains numerous morphological and physiologicalsubtypes of amacrine cells necessary for integrating and modulatingvisual signals presented to the output neurons. Among subtypesof amacrine cells grouped by neurotransmitter phenotypes, theglycinergic and ${gamma}$ -aminobutyric acid (GABA)ergic amacrine cellsconstitute two major subpopulations. To date, the molecularmechanisms governing the specification of subtype identity ofamacrine cells remain elusive. We report here that during mousedevelopment, the Barhl2 homeobox gene displays an expressionpattern in the nervous system that is distinct from that ofits homologue Barhl1. In the developing retina, Barhl2 expressionis found in postmitotic amacrine, horizontal and ganglion cells,while Barhl1 expression is absent. Forced expression of Barhl2in retinal progenitors promotes the differentiation of glycinergicamacrine cells, whereas a dominant-negative form of Barhl2 hasthe opposite effect. By contrast, they exert no effect on theformation of GABAergic neurons. Moreover, misexpressed Barhl2inhibits the formation of bipolar and Müller glial cells,indicating that Barhl2 is able to function both as a positiveand negative regulator, depending on different types of cells.Taken together, our data suggest that Barhl2 may function tospecify the identity of glycinergic amacrine cells from competentprogenitors during retinogenesis.

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