ZFIN ID: ZDB-PUB-051207-18
Essential and overlapping roles for laminin alpha chains in notochord and blood vessel formation
Pollard, S.M., Parsons, M.J., Kamei, M., Kettleborough, R.N., Thomas, K.A., Pham, V.N., Bae, M.K., Scott, A., Weinstein, B.M., and Stemple, D.L.
Date: 2006
Source: Developmental Biology 289(1): 64-76 (Journal)
Registered Authors: Kamei, Makoto, Kettleborough, Ross, Parsons, Michael, Pham, Van, Scott, Annabelle, Stemple, Derek L., Thomas, Kevin, Weinstein, Brant M.
Keywords: Laminin, Notochord, Blood vessels, Basement membrane, Cell differentiation
MeSH Terms: Animals; Blood Vessels/chemistry; Blood Vessels/embryology; Cell Movement; Endothelial Cells/cytology (all 18) expand
PubMed: 16321372 Full text @ Dev. Biol.
FIGURES   (current status)
ABSTRACT
Laminins are major constituents of basement membranes and have wide ranging functions during development and in the adult. They are a family of heterotrimeric molecules created through association of an alpha, beta and gamma chain. We previously reported that two zebrafish loci, grumpy (gup) and sleepy (sly), encode laminin beta1 and gamma1, which are important both for notochord differentiation and for proper intersegmental blood vessel (ISV) formation. In this study we show that bashful (bal) encodes laminin alpha1 (lama1). Although the strongest allele, bal(m190), is fully penetrant, when compared to gup or sly mutant embryos, bal mutants are not as severely affected, as only anterior notochord fails to differentiate and ISVs are unaffected. This suggests that other alpha chains, and hence other isoforms, act redundantly to laminin 1 in posterior notochord and ISV development. We identified cDNA sequences for lama2, lama4 and lama5 and disrupted the expression of each alone or in mutant embryos also lacking laminin alpha1. When expression of laminin alpha4 and laminin alpha1 are simultaneously disrupted, notochord differentiation and ISVs are as severely affected as sly or gup mutants. Moreover, live imaging of transgenic embryos expressing enhanced green fluorescent protein in forming ISVs reveals that the vascular defects in these embryos are due to an inability of ISV sprouts to migrate correctly along the intersegmental, normally laminin-rich regions.
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