Xiro homeoproteins coordinate cell cycle exit and primary neuron formation by upregulating neuronal-fate repressors and downregulating the cell-cycle inhibitor XGadd45-gamma

Calle-Mustienes, ED; Glavic A.; Modolell, J; Gomez-Skarmeta, JL

Abstract

The iroquois (iro) homeobox genes participate in many developmental processes both in vertebrates and invertebrates, among them are neural plate formation and neural patterning. In this work, we study in detail Xenopus Iro (Xiro) function in primary neurogenesis. We show that misexpression of Xiro genes promotes the activation of the proneural gene Xngnr1 but suppresses neuronal differentiation. This is probably due to upregulation of at least two neuronal-fate repressors: XHairy2A and XZic2. Accordingly, primary neurons arise at the border of the Xiro expression domains. In addition, we identify XGadd45-? as a new gene repressed by Xiro. XGadd45-? encodes a cell-cycle inhibitor and is expressed in territories where cells will exit mitosis, such as those where primary neurons arise. Indeed, XGadd45-? misexpression causes cell cycle arrest. We conclude that, during Xenopus primary neuron formation, in Xiro expressing territories neuronal differentiation is impaired, while in adjacent cells, XGadd45-? may help cells stop dividing and differentiate as neurons. © 2002 Elsevier Science Ireland Ltd. All rights reserved.

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Título según WOS: Xiro homeoproteins coordinate cell cycle exit and primary neuron formation by upregulating neuronal-fate repressors and downregulating the cell-cycle inhibitor XGadd45-gamma
Título según SCOPUS: Xiro homeoproteins coordinate cell cycle exit and primary neuron formation by upregulating neuronal-fate repressors and downregulating the cell-cycle inhibitor XGadd45-?
Título de la Revista: MECHANISMS OF DEVELOPMENT
Volumen: 119
Número: 1
Editorial: ELSEVIER SCIENCE BV
Fecha de publicación: 2002
Página de inicio: 69
Página final: 80
Idioma: English
URL: http://linkinghub.elsevier.com/retrieve/pii/S0925477302002964
DOI:

10.1016/S0925-4773(02)00296-4

Notas: ISI, SCOPUS