<html><head><meta http-equiv="content-type" content="text/html; charset=utf-8"></head><body dir="auto">Colloquium Speaker<div><div class="event-value" style="box-sizing: border-box;"><font color="#000000"><span style="background-color: rgba(255, 255, 255, 0);"><a href="https://systemsbiology.columbia.edu/people/smita-krishnaswamy" target="_blank" style="box-sizing: border-box; text-decoration: none;">Smita Krishnaswamy</a>, from <a href="http://www.columbia.edu/" target="_blank" style="box-sizing: border-box; text-decoration: none;">Columbia University</a></span></font></div></div><div>Thursday, March 5, 12:30pm</div><div>Computer Science 105</div><div><br></div><div><h1 class="page-header" style="box-sizing: border-box; margin: 0px 0px 20px; font-weight: 500; padding-bottom: 9px; border-bottom-width: 1px; border-bottom-style: solid; border-bottom-color: rgb(238, 238, 238);"><span style="font-size: 21px; background-color: rgba(255, 255, 255, 0);">Unlocking Cellular Computation and Information Processing through Multidimensional Single-Cell Data</span></h1></div><div><span style="font-size: 21px; background-color: rgba(255, 255, 255, 0);"><br></span></div><div><span style="background-color: rgba(255, 255, 255, 0);">Cells are computational entities that process external signals through networks of interacting proteins and reconfigure their state via biochemical modifications of proteins and changes in gene expression. Despite progress in the understanding of signaling biology, graph diagrams typically used as depictions of signaling relationships only offer qualitative abstractions. New single-cell measurement technologies provide quantitatively precise measurements of dozens of cellular components representing important biochemical functions. However, a major challenge in deciphering single-cell signaling data is developing computational methods that can handle the complexity, noise and bias in the measurements. I will describe algorithms that quantify the flow of information through signaling interactions and mathematically characterize relationships between signaling molecules, using statistical techniques to detect dependencies while mitigating the effect of noise. I will show how these algorithms can be utilized to characterize signaling relationships in immune cells, detect subtle differences between cell types, and predict differential responses to perturbation. Next, I will analyze T cells from non-obese diabetic (NOD) mice and show that previously recognized defects in extracellular-signal-regulated kinase <b style="box-sizing: border-box;">(</b>ERK) signaling can be traced back to a small receptor-proximal defect that is amplified through reconvergence in the network. Then, I will show how multidimensional extensions of these techniques can be used to track dynamic changes in the relatively unknown network driving the epithelial-to-mesenchymal (EMT) transition that occurs during cancer metastasis, with the goal of predicting drugs to halt the process. Finally, I will discuss future directions involving integration of gene expression and other data types in order to gain a more complete picture of cellular computation. </span></div></body></html>