Abstract

Nkx2.9 is a member of the NK homeobox family and resembles Nkx2.2 both in homology and expression pattern. However, while Nkx2.2 is required for development of serotonergic neurons, the role of Nkx2.9 in the mid-hindbrain region is still ill-defined. We have previously shown that Nkx2.9 expression is downregulated upon loss of En1 during development. Here, we determined whether mdDA neurons require Nkx2.9 during their development. We show that Nkx2.9 is strongly expressed in the IsO and in the VZ and SVZ of the embryonic midbrain, and the majority of mdDA neurons expressed Nkx2.9 during their development. Although the expression of Dat and Cck are slightly affected during development, the overall development and cytoarchitecture of TH-expressing neurons is not affected in the adult Nkx2.9-depleted midbrain. Transcriptome analysis at E14.5 indicated that genes involved in mid- and hindbrain development are affected by Nkx2.9-ablation, such as Wnt8b and Tph2. Although the expression of Tph2 extends more rostral into the isthmic area in the Nkx2.9 mutants, the establishment of the IsO is not affected. Taken together, these data point to a minor role for Nkx2.9 in mid-hindbrain patterning by repressing a hindbrain-specific cell-fate in the IsO and by subtle regulation of mdDA neuronal subset specification.

Highlights

  • NK homeobox genes, first described in drosophila, program organogenesis during embryonic development [1]

  • In the absence of En1 the expression in medial sections is lost in the isthmic organizer (IsO)-region, but expression is retained in the zona limitans intrathalamica (ZLI)

  • We showed that Nkx2.9 is lost in En1 mutant embryos and that expression of Nkx2.9 overlaps with the expression of known IsO markers, such as Fgf8

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Summary

Introduction

NK homeobox genes, first described in drosophila, program organogenesis during embryonic development [1]. The murine NK2 family consists of seven genes: Nkx2.1–Nkx2.6 and Nkx2.9, which is named Nkx2.8 in most other species [2,3,4]. These seven genes can be subdivided based on their homology to the drosophila NK genes and their dependence on sonic hedgehog (SHH) signaling. Nkx2.1, Nkx2.2 and Nkx2.9 resemble NK2 drosophila genes and are dependent on SHH-signaling for their expression, whilst Nkx2.3, Nkx2.5 and. Nkx2.6 resemble NK3 and are SHH-independent [4,5]. Nkx2.1, Nkx2.2 and Nkx2.9 are expressed in the central nervous system.

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