Literature DB >> 9102306

Preventing the loss of competence for neural induction: HGF/SF, L5 and Sox-2.

A Streit1, S Sockanathan, L Pérez, M Rex, P J Scotting, P T Sharpe, R Lovell-Badge, C D Stern.   

Abstract

The response to neural induction depends on the presence of inducing signals and on the state of competence of the responding tissue. The epiblast of the chick embryo loses its ability to respond to neural induction by the organizer (Hensen's node) between stages 4 and 4+. We find that the pattern of expression of the L5(220) antigen closely mirrors the changes in competence of the epiblast in time and in space. For the first time, we describe an experiment that can extend the period of neural competence: when L5(220) expression is maintained beyond its normal time by implanting HGF/SF secreting cells, the competence to respond to Hensen's node grafts is retained. The host epiblast forms a non-regionalized neural tube, which expresses the pan-neural marker SOX-2 (a Sry-related transcription factor) but not any region-specific markers for the forebrain, hindbrain or spinal cord. Although HGF/SF secreting cells can mimic signals from Hensen's node that maintain L5 expression, they cannot rescue the ability of the node to induce anterior structures (which is normally lost after stage 4). The ectoderm may acquire stable neural characteristics during neural induction by going through a hierarchy of states: competence, neuralization and regionalization. Our findings allow us to start to define these different states at a molecular level, and show that the competence to respond to neural induction is not entirely autonomous to the responding cells, but can be regulated by extracellular signalling molecules.

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Year:  1997        PMID: 9102306     DOI: 10.1242/dev.124.6.1191

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  33 in total

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8.  AP2γ regulates neural and epidermal development downstream of the BMP pathway at early stages of ectodermal patterning.

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Review 9.  Setting appropriate boundaries: fate, patterning and competence at the neural plate border.

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10.  A transition from SoxB1 to SoxE transcription factors is essential for progression from pluripotent blastula cells to neural crest cells.

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