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THE ROLE OF NADPH OXIDASE 2 IN AXON GUIDANCE DURING ZEBRAFISH VISUAL SYSTEM DEVELOPMENTAslihan Terzi (9188978) 04 August 2020 (has links)
<p>Reactive oxygen species (ROS) are critical for maintaining cellular homeostasis and function when produced in physiological ranges. Important sources of cellular ROS include NADPH oxidases (Nox), which are evolutionarily conserved multi-subunit transmembrane proteins. Nox-mediated ROS regulate a variety of biological processes including stem cell proliferation and differentiation, calcium signaling, cell migration, and immunity. ROS participate in intracellular signaling by introducing post-translational modifications to proteins and thereby altering their functions. The central nervous system (CNS) expresses different Nox isoforms during both development and adulthood. There is now emerging evidence that Nox-derived ROS also control neuronal development and pathfinding. Our lab has recently shown that retinal ganglion cells (RGCs) from <i>nox2</i> mutant zebrafish exhibit pathfinding errors. However, whether Nox could act downstream of receptors for axonal growth and guidance cues is presently unknown. To investigate this question, we conducted a detailed characterization of the zebrafish <i>nox2</i> mutants that were previously established in our group. Abnormal axon projections were found throughout the CNS of the <i>nox2 </i>mutant zebrafish. Anterior commissural axons failed proper fasciculation, and aberrant axon projections were detected in the dorsal longitudinal fascicle of the spinal cord. We showed that the major brain regions are intact and that the early development of CNS is not significantly altered in <i>nox2 </i>mutants. Hence, the axonal deficits in <i>nox2</i> mutants are not due to general developmental problems, and Nox2 plays a role in axonal pathfinding and targeting. Next, we investigated whether Nox2 could act downstream of slit2/Robo2-mediated guidance during RGC pathfinding. We found that slit2-mediated RGC growth cone collapse was abolished in <i>nox2 </i>mutants <i>in vitro</i>. Further, ROS biosensor imaging showed that slit2 treatment increased growth cone hydrogen peroxide levels via mechanisms through Nox2 activation. Finally, we investigated the possible relationship between slit2/Robo2 and Nox2 signaling <i>in vivo</i>. <i>Astray/nox2</i> double heterozygous mutant larvae exhibited decreased tectal area as opposed to individual heterozygous mutants, suggesting both Nox2 and Robo2 are required for the establishment of retinotectal connections. Our results suggest that Nox2 is part of a signal transduction pathway downstream of slit2/Robo2 interaction regulating axonal guidance cell-autonomously in developing zebrafish retinal neurons.</p>
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COLLECTIVE CELL MIRATION DURING HEART MORPHOGENESIS IN DROSOPHILA REQUIRES GUIDANCE SIGNALING AND EXTRACELLULAR MATRIX REMODELLING / COLLECTIVE CELL MIGRATION OF CARDIOBLASTS DURING HEART MORPHOGENESISRaza, Qanber 11 1900 (has links)
Collective cell migration is a defining feature of many morphogenetic processes.
Diseases such as congenital heart diseases and cancer arise due to mis-regulation of
collective migratory behaviour and animal models have played a pivotal role in dissecting
the molecular mechanisms which underlie this process. During embryonic heart
development, cardiac precursors undergo a stage of collective migration in both
vertebrates and invertebrates. We developed a paradigm to quantitatively assess collective
cell migration of cardiac precursors in live embryos of Drosophila, which is the simplest
genetic model organism with a heart. Therefore, we studied processes which are
commonly observed in most collective cell migration models such as guidance signalling
and extracellular matrix remodelling. Our results demonstrate that leading edge of
migrating cardioblasts is highly active and that this behaviour is regulated by guidance
cues, Slit and Netrin and their respective receptors Robo/Robo2 and Frazzled/Uncoordinated5.
These molecules cooperatively promote leading edge motility and epithelial
characteristics of the cardioblasts. Next, we determined that matrix restructuring around
the cardioblasts requires proteases Mmp1 and Mmp2, which are members of the highly
conserved Matrix Metalloproteinase family. We demonstrate that Mmp1 and Mmp2 have
distinct roles during lumen formation, however, both Mmp1 and Mmp2 are required for
collective motility of the cardioblast leading edge. Hence, we propose that embryonic
heart development in Drosophila is an effective and amenable model of collective cell
migration which can be applied to discover unique mechanisms which coordinate cell
movement in groups. / Thesis / Doctor of Philosophy (PhD)
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