PUBLICATION

Zebrafish Zic2a and Zic2b regulate neural crest and craniofacial development

Authors

Teslaa, J.J., Keller, A.N., Nyholm, M.K., and Grinblat, Y.

ID

ZDB-PUB-130610-54

Date

2013

Source

Developmental Biology 380(1): 73-86 (Journal)

Registered Authors

Grinblat, Yevgenya, Nyholm, Molly Wagner, TeSlaa, Jessica Joy

Keywords

zebrafish, zic, craniofacial cartilage, forebrain, holoprosencephaly

MeSH Terms

Mutation
Recombinant Fusion Proteins/metabolism
Brain/embryology
Cartilage/metabolism
Transcription Factors/genetics
Transcription Factors/physiology*
Body Patterning
Gene Expression Regulation, Developmental*
Zebrafish/embryology*
Zebrafish Proteins/genetics
Zebrafish Proteins/physiology*
Neural Crest/cytology*
Skull/embryology*
Animals
Holoprosencephaly
Gene Expression Profiling
Chondrocytes/cytology

(all 17)

PubMed

23665173 Full text @ Dev. Biol.

Abstract

Holoprosencephaly (HPE), the most common malformation of the human forebrain, is associated with defects of the craniofacial skeleton. ZIC2, a zinc-finger transcription factor, is strongly linked to HPE and to a characteristic set of dysmorphic facial features in humans. We have previously identified important functions for zebrafish Zic2 in the developing forebrain. Here, we demonstrate that ZIC2 orthologs zic2a and zic2b also regulate the forming zebrafish craniofacial skeleton, including the jaw and neurocranial cartilages, and use the zebrafish to study Zic2-regulated processes that may contribute to the complex etiology of HPE. Using temporally controlled Zic2a overexpression, we show that the developing craniofacial cartilages are sensitive to Zic2 elevation prior to 24 hpf. This window of sensitivity overlaps the critical expansion and migration of the neural crest (NC) cells, which migrate from the developing neural tube to populate vertebrate craniofacial structures. We demonstrate that zic2b influences the induction of NC at the neural plate border, while both zic2a and zic2b regulate NC migratory onset and strongly contribute to chromatophore development. Both Zic2 depletion and early ectopic Zic2 expression cause moderate, incompletely penetrant mispatterning of the NC-derived jaw precursors at 24 hpf, yet by 2 dpf these changes in Zic2 expression result in profoundly mispatterned chondrogenic condensations. We attribute this discrepancy to an additional role for Zic2a and Zic2b in patterning the forebrain primordium, an important signaling source during craniofacial development. This hypothesis is supported by evidence that transplanted Zic2-deficient cells can contribute to craniofacial cartilages in a wild-type background. Collectively, these data suggest that zebrafish Zic2 plays a dual role during craniofacial development, contributing to two disparate aspects of craniofacial morphogenesis: (1) neural crest induction and migration, and (2) early patterning of tissues adjacent to craniofacial chondrogenic condensations.

Genes / Markers

Figures

Show all Figures

Expression

Gene	Fish	Conditions	Stage	Qualifier	Anatomy	Assay	Figure
col2a1a	uw6Tg; vu22Tg	heat shock	Long-pec	Not Detected	ethmoid cartilage	ISH	Fig. 3
col2a1a	uw6Tg; vu22Tg	heat shock	Long-pec		neurocranial trabecula	ISH	Fig. 3
col2a1a	WT	control	Long-pec		ethmoid cartilage	ISH	Fig. 3
col2a1a	WT	control	Long-pec		neurocranial trabecula	ISH	Fig. 3
col2a1a	WT + MO3-zic2a	standard conditions	Long-pec	Not Detected	ethmoid cartilage	ISH	Fig. 3
col2a1a	WT + MO3-zic2a	standard conditions	Long-pec		neurocranial trabecula	ISH	Fig. 3
dlx2a	uw6Tg; vu22Tg	heat shock	Prim-5		hypothalamus	ISH	Fig. 8
dlx2a	uw6Tg; vu22Tg	heat shock	Prim-5		pharyngeal arch 1 mandibular neural crest	ISH	Fig. 7
dlx2a	uw6Tg; vu22Tg	heat shock	Prim-5		pharyngeal arch 1 mandibular neural crest	ISH	Fig. 7
dlx2a	uw6Tg; vu22Tg	heat shock	Prim-5		pharyngeal arch 2 hyoid neural crest	ISH	Fig. 7

1 - 10 of 98

Show

Phenotype

Fish	Conditions	Stage	Phenotype	Figure
WT + MO2-zic2b	standard conditions	5-9 somites	neural crest cell cellular quality, abnormal	Fig. 4
WT + MO2-zic2b	standard conditions	5-9 somites	neural crest cell differentiation decreased process quality, abnormal	Fig. 4
WT + MO2-zic2b	standard conditions	14-19 somites	cranial neural crest mislocalised dorsally, abnormal	Fig. 5
WT + MO2-zic2b	standard conditions	14-19 somites	neural crest cell migration decreased process quality, abnormal	Fig. 5
WT + MO2-zic2b	standard conditions	Prim-5	forebrain development decreased process quality, abnormal	Fig. 8
WT + MO2-zic2b	standard conditions	Prim-5	melanoblast aggregated, abnormal	Fig. 6
WT + MO2-zic2b	standard conditions	Prim-5	melanoblast mislocalised, abnormal	Fig. 6
WT + MO2-zic2b	standard conditions	Prim-5	melanocyte differentiation decreased process quality, abnormal	Fig. 6
WT + MO2-zic2b	standard conditions	Prim-5	melanocyte migration decreased process quality, abnormal	Fig. 6
WT + MO2-zic2b	standard conditions	Prim-5	pharyngeal arch cellular quality, normal	Fig. 7

1 - 10 of 87

Show

Mutations / Transgenics

Allele	Construct	Type	Affected Genomic Region
uw6Tg	Tg(11xUAS:zic2a-YFP,myl7:mCherry)	Transgenic Insertion
vu22Tg	Tg(hsp70l:GAL4-VP16)	Transgenic Insertion

Human Disease / Model

Sequence Targeting Reagents

Target	Reagent	Reagent Type
zic2a	MO1-zic2a	MRPHLNO
zic2a	MO2-zic2a	MRPHLNO
zic2a	MO3-zic2a	MRPHLNO
zic2b	MO1-zic2b	MRPHLNO
zic2b	MO2-zic2b	MRPHLNO

Fish

Fish
uw6Tg; vu22Tg
WT
WT + MO2-zic2b
WT + MO2-zic2b + MO3-zic2a
WT + MO3-zic2a

Antibodies

Orthology

Engineered Foreign Genes

Marker	Marker Type	Name
GAL4	EFG	GAL4
mCherry	EFG	mCherry
YFP	EFG	YFP

Mapping

Teslaa et al., 2013 ZDB-PUB-130610-54 PMID:23665173

Zebrafish Zic2a and Zic2b regulate neural crest and craniofacial development

Teslaa et al., 2013

ZDB-PUB-130610-54
PMID:23665173