Loss of laminin alpha 1 results in multiple structural defects and divergent effects on adhesion during vertebrate optic cup morphogenesis
Retinal Ganglion Cells
Organogenesis
Retinal Pigment Epithelium
Time-Lapse Imaging
Retina
Eye morphogenesis
Lens
03 medical and health sciences
Cell Movement
Lens, Crystalline
Animals
Eye Proteins
Molecular Biology
Zebrafish
Focal Adhesions
0303 health sciences
Microscopy, Confocal
Cell Polarity
Cell Biology
Zebrafish Proteins
Extracellular Matrix
Luminescent Proteins
Cell polarity
Adhesion
Laminin
Developmental Biology
DOI:
10.1016/j.ydbio.2016.06.025
Publication Date:
2016-06-22T21:15:44Z
AUTHORS (3)
ABSTRACT
The vertebrate eye forms via a complex set of morphogenetic events. The optic vesicle evaginates and undergoes transformative shape changes to form the optic cup, in which neural retina and retinal pigmented epithelium enwrap the lens. It has long been known that a complex, glycoprotein-rich extracellular matrix layer surrounds the developing optic cup throughout the process, yet the functions of the matrix and its specific molecular components have remained unclear. Previous work established a role for laminin extracellular matrix in particular steps of eye development, including optic vesicle evagination, lens differentiation, and retinal ganglion cell polarization, yet it is unknown what role laminin might play in the early process of optic cup formation subsequent to the initial step of optic vesicle evagination. Here, we use the zebrafish lama1 mutant (lama1(UW1)) to determine the function of laminin during optic cup morphogenesis. Using live imaging, we find, surprisingly, that loss of laminin leads to divergent effects on focal adhesion assembly in a spatiotemporally-specific manner, and that laminin is required for multiple steps of optic cup morphogenesis, including optic stalk constriction, invagination, and formation of a spherical lens. Laminin is not required for single cell behaviors and changes in cell shape. Rather, in lama1(UW1) mutants, loss of epithelial polarity and altered adhesion lead to defective tissue architecture and formation of a disorganized retina. These results demonstrate that the laminin extracellular matrix plays multiple critical roles regulating adhesion and polarity to establish and maintain tissue structure during optic cup morphogenesis.
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