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  <title><![CDATA[PhD Defense by Eunbi Park]]></title>
  <body><![CDATA[<p><span><span><span><span>In partial fulfillment of the requirements for the degree of</span></span></span></span></p>

<p><span><span><span><span>Doctor of Philosophy in Bioinformatics</span></span></span></span></p>

<p><span><span><span><span>in the School of Biological Sciences</span></span></span></span></p>

<p><span><span><strong>&nbsp;</strong></span></span></p>

<p><span><span><strong><span><span>Eunbi Park</span></span></strong></span></span></p>

<p><span><span>&nbsp;</span></span></p>

<p><span><span><span><span>Defends her thesis:</span></span></span></span></p>

<p><span><span><strong>Modeling emergent patterning within pluripotent colonies through Boolean canalizing functions</strong></span></span></p>

<p>&nbsp;</p>

<p><span><span>Wednesday, April 17th, 2024</span></span></p>

<p><span><span>11:00 AM</span></span></p>

<p><span><span><span><span>Krone Engineered Biosystems Building (EBB), Room #5029</span></span></span></span></p>

<p><span><span><span><span>Zoom Link: </span></span><a href="https://gatech.zoom.us/j/98921652004?pwd=QmxVZUNxdVgvMVhYU1BUMGs4alJ0dz09">https://gatech.zoom.us/j/98921652004?pwd=QmxVZUNxdVgvMVhYU1BUMGs4alJ0dz09</a></span></span></p>

<p><span><span>Meeting ID: 989 2165 2004</span></span></p>

<p>&nbsp;</p>

<p><span><span><strong>Thesis Advisor:</strong></span></span></p>

<p><span><span>Dr. Melissa L. Kemp</span></span></p>

<p><span><span>Wallace H. Coulter Department of Biomedical Engineering</span></span></p>

<p><span><span><em>Georgia Institute of Technology and Emory University</em></span></span></p>

<p>&nbsp;</p>

<p><span><span><strong>Committee Members:</strong></span></span></p>

<p><span><span>Dr. Ahmet F. Coskun</span></span></p>

<p><span><span>Wallace H. Coulter Department of Biomedical Engineering</span></span></p>

<p><span><span><em>Georgia Institute of Technology and Emory University</em></span></span></p>

<p>&nbsp;</p>

<p><span><span>Dr. Elena S. Dimitrova</span></span></p>

<p><span><span><span><span>Mathematics Department</span></span></span></span></p>

<p><span><span><em>California Polytechnic State University</em></span></span></p>

<p>&nbsp;</p>

<p><span><span>Dr. Jeffrey T. Streelman</span></span></p>

<p><span><span><span><span>School of Biological Sciences</span></span></span></span></p>

<p><span><span><em>Georgia Institute of Technology</em></span></span></p>

<p>&nbsp;</p>

<p><span><span>Dr. Matthew P. Torres</span></span></p>

<p><span><span>School of Biological Sciences</span></span></p>

<p><span><span><em>Georgia Institute of Technology</em></span></span></p>

<p>&nbsp;</p>

<p><span><span>Dr. Denis V. Tsygankov</span></span></p>

<p><span><span>Wallace H. Coulter Department of Biomedical Engineering</span></span></p>

<p><span><span><em>Georgia Institute of Technology and Emory University</em></span></span></p>

<p>&nbsp;</p>

<p><span><span><strong>Abstract:</strong></span></span></p>

<p>&nbsp;</p>

<p><span><span>The early events of human induced pluripotent stem cell (hiPSC) differentiation require collective intercellular communication at both local and long distances for symmetry breaking and pattern formation. It is currently unclear which mechanisms take priority in context-specific situations, and resolving these mechanisms is needed to advance hiPSC-derived tissue engineering. Prior work reported intracellular and intercellular regulation of the FGF/ERK/GATA6 pathway in the mouse blastocyst as a driver of differentiation and self-organization. Computational models capable of simulating intrinsic and/or neighbor-to-neighbor mechanisms provide a useful approach to analyze the role of signaling in multicellular organization during the initial loss of pluripotency. </span></span></p>

<p>&nbsp;</p>

<p><span><span>The objective of this research was to investigate the dynamics of emergent patterning and collective intra-/inter-cellular communication that directs early cell fate decisions in hiPSCs. To enable the interpretation of cellular interactions, a novel pipeline was developed to quantify the differences between spatial organization obtained from both <em>in vitro</em> microscopy images and <em>in silico</em> modeling outcomes using topological data analysis (TDA). Next, I performed characterization of FGF/ERK/GATA6 pathway during emergent pattern formation under multiple molecular perturbations, elucidating context-specific attributes in two-dimensional and three-dimensional culture conditions. Finally, a Python agent-based model of hiPSC colony patterning was created with Boolean networks to discriminate between putative mechanisms of cell fate decisions and compared experimentally observed patterns via TDA. Overall, this work demonstrates that the strategies of quantifying spatial organization and modeling and testing engineered hiPSCs in colonies and organoids are tractable alternative approaches to embryonic systems, allowing for the identification of modes of intercellular communication that determine cell fates.</span></span></p>

<p>&nbsp;</p>

<p>&nbsp;</p>
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