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  <title><![CDATA[PhD Defense by Matthew Hunter Seabolt]]></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>&nbsp;</p>

<p><span><span><span><strong><span>Matthew Hunter Seabolt</span></strong></span></span></span></p>

<p><span><span><span>&nbsp;</span></span></span></p>

<p><span><span><span><span>Defends his thesis:</span></span></span></span></p>

<p><span><span><strong><span><span>Expanding the Bioinformatics Toolbox for DIVERSITY and TAXONOMIC STUDIES OF Microbial Eukaryotic Pathogens</span></span></strong></span></span></p>

<p>&nbsp;</p>

<p><span><span>Wednesday July 26, 2023</span></span></p>

<p><span><span>3:00-4:00pm </span></span></p>

<p><span><span>Krone Engineered Biosystems Building, Children’s Healthcare of Atlanta Seminar Room (EBB 1005)</span></span></p>

<p><span><span><a href="https://cdc.zoomgov.com/j/1616164156?pwd=dy9GZjc2Y05NYU9IWkhyTmZjS3YxZz09&amp;from=addon" target="_blank"><span>Join Zoom Meeting</span></a></span></span></p>

<p>&nbsp;</p>

<p><span><span><strong>Thesis Advisor:</strong></span></span></p>

<p><span><span><span><span>Dr. Kostas Konstantinidis, Advisor</span></span></span></span></p>

<p><span><span><span><span>School of Civil &amp; Environmental Engineering</span></span></span></span></p>

<p><span><span><span><span><em>Georgia Institute of Technology</em></span></span></span></span></p>

<p>&nbsp;</p>

<p><span><span><span><span><strong>Committee Members:</strong></span></span></span></span></p>

<p><span><span><span><span>Dr. Joel Kostka</span></span></span></span></p>

<p><span><span><span><span>School of Biological Sciences</span></span></span></span></p>

<p><span><span><span><span><em>Georgia Institute of Technology</em></span></span></span></span></p>

<p>&nbsp;</p>

<p><span><span><span><span>Dr. I. King Jordan</span></span></span></span></p>

<p><span><span><span><span>School of Biological Sciences</span></span></span></span></p>

<p><span><span><span><span><em>Georgia Institute of Technology</em></span></span></span></span></p>

<p>&nbsp;</p>

<p><span><span><span><span>Dr. Christine Heitsch</span></span></span></span></p>

<p><span><span><span><span>School of Mathematics</span></span></span></span></p>

<p><span><span><span><span><em>Georgia Institute of Technology</em></span></span></span></span></p>

<p>&nbsp;</p>

<p><span><span><span><span>Dr. Dawn M. Roellig</span></span></span></span></p>

<p><span><span><span><span>Waterborne Disease Prevention Branch</span></span></span></span></p>

<p><span><span><span><span>Division of Foodborne, Waterborne, and Environmental Diseases</span></span></span></span></p>

<p><span><span><span><span><em>Centers for Disease Control and Prevention</em></span></span></span></span></p>

<p>&nbsp;</p>

<p><span><span><span><strong><span>Abstract:</span></strong><br />
Cataloguing and studying microbial eukaryote diversity and speciation present unique challenges due to their evolutionary divergence from well-studied model genomes, limited culturing methods, and uncertain taxonomy. The scarcity of high-quality genomic data poses a significant obstacle to understanding genome relatedness and important traits like virulence and antimicrobial resistance, with much debate centered on how to reconcile discordant phylogenetic signals from existing molecular typing data with historical records and type specimens.&nbsp; Thus far, no major movement has occurred in almost two decades.&nbsp; Additionally, existing bioinformatics methods need advancement to handle large eukaryotic genomes effectively.</span></span></span></p>

<p><span><span>This research aims to expand the set of available bioinformatics tools for the comparative analysis of genomes of microbial eukaryotes. Case studies using the protozoan parasite <em>Giardia duodenalis</em> as a model organism are presented. These studies include (i) developing a new, automated pipeline for identifying the best gene markers in the genome for phylogenetic reconstruction purposes and strain-level resolution, (ii) the creation of a statistical framework to identify cryptic species and quantify their evolutionary relationships, and (iii) improving reference genome annotation of the <em>Giardia</em> genome.&nbsp; Lastly, we employed the genome aggregate average nucleotide identity (ANI) and graph-based methods to assess whether or not natural boundaries between eukaryotic species exist, similar to those previously observed for <em>Prokaryotes</em>, and study the relationship between shared gene content and ANI (or degree of genetic relatedness).</span></span></p>

<p><br />
<span><span>The findings suggest that sequence-discrete clusters of genomes, akin to traditional species, are prevalent among the examined genomes and our methodology is robust across eukaryote phyla and at multiple taxonomic hierarchies. Applying the conclusions from this research, such as 95% ANI as a general-purpose species boundary in eukaryotes as well as ANI’s utility for molecular typing, this research’s conclusions contribute novel biological insights and bioinformatics methods to the toolkit for eukaryote taxonomy, and genome analysis.</span></span></p>

<p>&nbsp;</p>
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