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  <title><![CDATA[PhD Defense by Xinling Li]]></title>
  <body><![CDATA[<p>In partial fulfillment of the requirements for the degree of</p><p>Doctor of Philosophy in Bioinformatics</p><p>in the Department of for&nbsp;Biomedical Engineering</p><p>&nbsp;</p><p><strong>Xinling Li</strong></p><p>&nbsp;</p><p>Will defend her thesis:</p><p>&nbsp;</p><p><strong>Quantitative Approaches for Identifying the Limitation of Single-cell Sequencing Technologies and Applying Sequencing Technologies in the Study of Infectious Diseases and Cancer</strong></p><p>&nbsp;</p><p>May 7, 2026</p><p>10:00 AM – 12:00 PM (EST)</p><p>EBB 4029</p><p><a href="https://teams.microsoft.com/meet/23036548151103?p=UplOBRjEVYTj2NYCAm" target="_blank" title="https://teams.microsoft.com/meet/23036548151103?p=UplOBRjEVYTj2NYCAm">https://teams.microsoft.com/meet/23036548151103?p=UplOBRjEVYTj2NYCAm</a></p><p>&nbsp;</p><p><strong>Thesis Advisor:</strong></p><p>Dr. Qiu Peng</p><p>Department of for&nbsp;Biomedical Engineering</p><p>Georgia Institute of Technology</p><p>&nbsp;</p><p><strong>Committee Members:</strong></p><p>Dr. Gabe Kwong</p><p>Department of for&nbsp;Biomedical Engineering</p><p>Georgia Institute of Technology</p><p>&nbsp;</p><p>Dr. Greg Gibson</p><p>School of Biological Sciences</p><p>Georgia Institute of Technology</p><p>&nbsp;</p><p>Dr. May Wang</p><p>Department of for&nbsp;Biomedical Engineering</p><p>Georgia Institute of Technology</p><p>&nbsp;</p><p>Dr. M.G. Finn</p><p>School of Chemistry and Biochemistry</p><p>Georgia Institute of Technology&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;</p><p>&nbsp;</p><p><strong>Abstract:</strong></p><p>This thesis focuses on identification of the limitation of single-cell sequencing technologies, and development of pipeline and models for analyzing sequencing data. The aim of this work is to contribute to a deeper understanding of sequencing technologies and a better utilization of the technologies in solving challenges in infectious diseases and cancer research. We first identified systematic under-detection of genes in scRNA-seq and Visium data through analyses of paired bulk RNA-seq&nbsp;and single-cell genomics&nbsp;datasets. These genes were enriched for poly(T) motifs near their 3′ ends, leading to the hypothesis that such motifs may form hairpin structures with poly(A) tails of mRNA transcripts, reducing capture efficiency during library preparation and explaining their lower detection compared to bulk RNA-seq.&nbsp;We also proposed a framework integrating graphical models and conventional machine learning to leverage scRNA-seq data for predicting COVID-19 severity and identifying biomarkers. Graphical models effectively distinguished healthy individuals from infected patients (F1-score &gt; 0.9), while traditional machine learning accurately classified disease severity (F1-score &gt; 0.99), revealing meaningful molecular signatures.&nbsp;In addition, we developed a bioinformatics pipeline to predict&nbsp;existence of&nbsp;proteases across bacterial species by leveraging known bacteria–protease relationships. Through large-scale protein–genome alignments, we identified previously unreported proteases across bacterial genomes that cause severe infectious diseases, with validation from bulk RNA-seq data.&nbsp;Finally, we constructed mathematical models based on mass action kinetics to evaluate multi-arm protease sensors, demonstrating their potential advantages in cancer detection. Overall, this work highlights limitations of current sequencing technologies and provides computational solutions to enhance their utility&nbsp;in early cancer detection and&nbsp;infectious disease&nbsp;treatment and diagnostics.</p><p>&nbsp;</p>]]></body>
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