Maintenance of Neuroepithelial Progenitor Cells by Delta-Notch Signalling in the Embryonic Chick Retina

Overview

Journal Curr Biol

Publisher Cell Press

Specialty Biology

Date 1997 Sep 1

PMID 9285721

Citations 101

Authors

D Henrique

E Hirsinger

J Adam

I le Roux

O Pourquie

D Ish-Horowicz

J Lewis

Affiliations

Soon will be listed here.

Abstract

Background: Neurons of the vertebrate central nervous system (CNS) are generated sequentially over a prolonged period from dividing neuroepithelial progenitor cells. Some cells in the progenitor cell population continue to proliferate while others stop dividing and differentiate as neurons. The mechanism that maintains the balance between these two behaviours is not known, although previous work has implicated Delta-Notch signalling in the process.

Results: In normal development, the proliferative layer of the neuroepithelium includes both nascent neurons that transiently express Delta-1 (Dl1), and progenitor cells that do not. Using retrovirus-mediated gene misexpression in the embryonic chick retina, we show that where progenitor cells are exposed to Dl1 signalling, they are prevented from embarking on neuronal differentiation. A converse effect is seen in cells expressing a dominant-negative form of Dl1, Dl1(dn), which we show renders expressing cells deaf to inhibitory signals from their neighbours. In a multicellular patch of neuroepithelium expressing Dl1(dn), essentially all progenitors stop dividing and differentiate prematurely as neurons, which can be of diverse types. Thus, Delta-Notch signalling controls a cell's choice between remaining as a progenitor and differentiating as a neuron.

Conclusions: Nascent retinal neurons, by expressing Dl1, deliver lateral inhibition to neighbouring progenitors; this signal is essential to prevent progenitors from entering the neuronal differentiation pathway. Lateral inhibition serves the key function of maintaining a balanced mixture of dividing progenitors and differentiating progeny. We propose that the same mechanism operates throughout the vertebrate CNS, enabling large numbers of neurons to be produced sequentially and adopt different characters in response to a variety of signals. A similar mechanism of lateral inhibition, mediated by Delta and Notch proteins, may regulate stem-cell function in other tissues.

Citing Articles

Identification and Characterization of ATOH7-Regulated Target Genes and Pathways in Human Neuroretinal Development.

Atac D, Maggi K, Feil S, Maggi J, Cuevas E, Sowden J Cells. 2024; 13(13.

PMID: 38994994 PMC: 11240604. DOI: 10.3390/cells13131142.

Phototactic preference and its genetic basis in the planulae of the colonial Hydrozoan .

Birch S, McGee L, Provencher C, DeMio C, Plachetzki D bioRxiv. 2024; .

PMID: 38617216 PMC: 11014542. DOI: 10.1101/2024.03.28.585045.

Notch pathway mutants do not equivalently perturb mouse embryonic retinal development.

Bosze B, Suarez-Navarro J, Cajias I, Brzezinski Iv J, Brown N PLoS Genet. 2023; 19(9):e1010928.

PMID: 37751417 PMC: 10522021. DOI: 10.1371/journal.pgen.1010928.

Key transcription factors influence the epigenetic landscape to regulate retinal cell differentiation.

Ge Y, Chen X, Nan N, Bard J, Wu F, Yergeau D Nucleic Acids Res. 2023; 51(5):2151-2176.

PMID: 36715342 PMC: 10018358. DOI: 10.1093/nar/gkad026.

Müller Glia in Retinal Development: From Specification to Circuit Integration.

Tworig J, Feller M Front Neural Circuits. 2022; 15:815923.

PMID: 35185477 PMC: 8856507. DOI: 10.3389/fncir.2021.815923.