PUBLICATION

Characterization of drCol 15a1b: A Novel Component of the Stem Cell Niche in the Zebrafish Retina

Authors

Gonzalez-Nunez, V., Nocco, V., and Budd, A.

ID

ZDB-PUB-100621-18

Date

2010

Source

Stem cells (Dayton, Ohio) 28(8): 1399-1411 (Journal)

Registered Authors

González Nuñez, Veronica

Keywords

ciliary marginal zone, col 15a1, col 18a1, extracellular matrix, consensus network, phylogenetic network

MeSH Terms

Collagen/classification
Collagen/genetics
Collagen/metabolism
Zebrafish
Phylogeny
Zebrafish Proteins/classification
Zebrafish Proteins/genetics
Zebrafish Proteins/metabolism*
In Situ Hybridization
Retina/embryology
Retina/metabolism*
Stem Cell Niche/metabolism*
Polymerase Chain Reaction
Animals
Immunohistochemistry

(all 15)

PubMed

20549708 Full text @ Stem Cells

Abstract

There is a clear need to develop novel tools to help improve our understanding of stem-cell biology, and potentially also the utility of stem-cells in regenerative medicine. We report the cloning, functional, and bioinformatic characterization of a novel stem-cell marker in the zebrafish retina, drCol 15a1b. The expression pattern of drCol 15a1b is restricted to stem-cell niches located in the central nervous system, while other collagen XVs are associated with muscle and endothelial tissues. Knocking-down drCol 15a1b expression causes smaller eyes, ear defects, and brain edema. Microscopic analysis reveals enhanced proliferation in the morphant eye, with many mitotic nuclei located in the central retina, together with a delayed differentiation of the mature retinal cell types. Besides, several markers known to be expressed in the CMZ display broader expression areas in morpholino-injected embryos, suggesting an anomalous diffusion of signalling effectors from the shh and notch pathways. These results indicate that drCol 15a1b is a novel stem-cell marker in the central nervous system that has a key role in homing stem-cells into specialized niches in the adult organism. Moreover, mutations in the hCol 18a1 gene are responsible for the Knobloch syndrome, which affects brain and retinal structures, suggesting that drCol 15a1b may function similarly to mammalian Col 18a1. Thus, our results shed new light on the signalling pathways that underlie the maintenance of stem-cells in the adult organism while helping us to understand the role of extracellular matrix proteins in modulating the signals that determine stem-cell differentiation, cell-cycle exit and apoptosis.

Genes / Markers

Figures

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Expression

Phenotype

Fish	Conditions	Stage	Phenotype	Figure
TL + MO1-col15a1b	standard conditions	Protruding-mouth	apoptotic process increased occurrence, abnormal	Fig. 3
TL + MO1-col15a1b	standard conditions	Protruding-mouth	cell population proliferation increased occurrence, abnormal	Fig. 3
TL + MO1-col15a1b	standard conditions	Protruding-mouth	eye decreased size, abnormal	Fig. 2
TL + MO1-col15a1b	standard conditions	Protruding-mouth	inner ear morphology, abnormal	Fig. 2
TL + MO1-col15a1b	standard conditions	Protruding-mouth	neural tube closure arrested, abnormal	Fig. 2
mi2001Tg + MO1-col15a1b	standard conditions	Protruding-mouth	glial cell differentiation decreased occurrence, abnormal	Fig. 4

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Mutations / Transgenics

Allele	Construct	Type	Affected Genomic Region
mi2001Tg	Tg(gfap:GFP)	Transgenic Insertion
t4		Deficiency	shha

Human Disease / Model

Sequence Targeting Reagents

Target	Reagent	Reagent Type
col15a1b	MO1-col15a1b	MRPHLNO

Fish

Fish
Df(Chr07)t4
mi2001Tg
mi2001Tg + MO1-col15a1b
TL
TL + MO1-col15a1b

Antibodies

Orthology

Gene	Orthology
col15a1b

Engineered Foreign Genes

Marker	Marker Type	Name
GFP	EFG	GFP

Mapping

Gonzalez-Nunez et al., 2010 ZDB-PUB-100621-18 PMID:20549708

Characterization of drCol 15a1b: A Novel Component of the Stem Cell Niche in the Zebrafish Retina

Gonzalez-Nunez et al., 2010

ZDB-PUB-100621-18
PMID:20549708