A Cell Profiling Framework for Modeling Drug Responses from HCS Imaging
Author(s) -
Alvin Yu Jin Ng,
Jagath C. Rajapakse,
Roy E. Welsch,
Paul Matsudaira,
Victor Horodincu,
James G. Evans
Publication year - 2010
Publication title -
slas discovery
Language(s) - English
Resource type - Journals
eISSN - 2472-5560
pISSN - 2472-5552
DOI - 10.1177/1087057110372256
Subject(s) - cluster analysis , profiling (computer programming) , drug , computational biology , hierarchical clustering , drug action , cell , cytoskeleton , high content screening , microtubule , cluster (spacecraft) , drug discovery , computer science , bioinformatics , chemistry , biological system , biology , artificial intelligence , pharmacology , genetics , programming language , operating system
The authors present an unsupervised, scalable, and interpretable cell profiling framework that is compatible with data gathered from high-content screening. They demonstrate the effectiveness of their framework by modeling drug differential effects of IC-21 macrophages treated with microtubule and actin disrupting drugs. They identify significant features of cell phenotypes for unsupervised learning based on maximum relevancy and minimum redundancy criteria. A 2-stage clustering approach annotates, clusters cells, and then merges them together to form super-clusters. An interpretable cell profile consisting of super-cluster proportions profiled at each drug treatment, concentration, or duration is obtained. Differential changes in super-cluster profiles are the basis for understanding the drug's differential effect and biology. The authors' method is validated by significant chi-squared statistics obtained from similar drug-treated super-cluster profiles from a 5-fold cross-validation. In addition, drug profiles of 2 microtubule drugs with equivalent mechanisms of action are statistically similar. Several distinct trends are identified for the 5 cytoskeletal drugs profiled under different conditions.
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