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XB-ART-5491
Mech Dev 2003 Apr 01;1204:415-28. doi: 10.1016/s0925-4773(03)00018-2.
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The germ cell nuclear factor is required for retinoic acid signaling during Xenopus development.

Barreto G , Borgmeyer U , Dreyer C .


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The germ cell nuclear factor (GCNF, NR6A1) is a nuclear orphan receptor that functions as a transcriptional repressor and is transiently expressed in mammalian carcinoma cells during retinoic acid (RA) induced neuronal differentiation. During Xenopus laevis development, the spatiotemporal expression pattern of embryonic GCNF (xEmGCNF) suggests a role in anteroposterior specification of the neuroectoderm. Here, we show that RA treatment of Xenopus embryos enhances xEmGCNF expression. Moreover, we present evidence for the relevance of this finding in the context of primary neurogenesis and hindbrain development. During early development of the central nervous system, RA signals promote posterior transformation of the neuroectoderm and increase the number of cells undergoing primary neurogenesis. Our loss-of-function analyses using a xEmGCNF-specific morpholino antisense oligonucleotide indicate that xEmGCNF is required for the effect of RA on primary neurogenesis. This may be caused by transcriptional regulation of the gene encoding the RA-degrading enzyme CYP26, since this gene is derepressed after depletion of xEmGCNF and an antimorph of xEmGCNF directly activates transcription of CYP26, also in absence of protein synthesis. The effect of xEmGCNF knockdown on hindbrain patterning is similar to conditions of reduced RA signaling, which may be caused by a reduction of RAR gamma expression specifically in the presumptive hindbrain.

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Species referenced: Xenopus laevis
Genes referenced: aldh1a2 cyp26a1 dll1 eef1a2 egr2 eif3a en2 gal.2 gbx2 gbx2.2 lhx1 neurog2 nr6a1 odc1 otx2 rab40b rarg sult2a1 tbx2 tubb2b
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