Abstract

BackgroundA systems biology interpretation of genome-scale RNA interference (RNAi) experiments is complicated by scope, experimental variability and network signaling robustness. Over representation approaches (ORA), such as the Hypergeometric or z-score, are an established statistical framework used to associate RNA interference effectors to biologically annotated gene sets or pathways. These methods, however, do not directly take advantage of our growing understanding of the interactome. Furthermore, these methods can miss partial pathway activation and may be biased by protein complexes. Here we present a novel ORA, protein interaction permutation analysis (PIPA), that takes advantage of canonical pathways and established protein interactions to identify pathways enriched for protein interactions connecting RNAi hits.ResultsWe use PIPA to analyze genome-scale siRNA cell growth screens performed in HeLa and TOV cell lines. First we show that interacting gene pair siRNA hits are more reproducible than single gene hits. Using protein interactions, PIPA identifies enriched pathways not found using the standard Hypergeometric analysis including the FAK cytoskeletal remodeling pathway. Different branches of the FAK pathway are distinctly essential in HeLa versus TOV cell lines while other portions are uneffected by siRNA perturbations. Enriched hits belong to protein interactions associated with cell cycle regulation, anti-apoptosis, and signal transduction.ConclusionPIPA provides an analytical framework to interpret siRNA screen data by merging biologically annotated gene sets with the human interactome. As a result we identify pathways and signaling hypotheses that are statistically enriched to effect cell growth in human cell lines. This method provides a complementary approach to standard gene set enrichment that utilizes the additional knowledge of specific interactions within biological gene sets.

Highlights

  • A systems biology interpretation of genome-scale RNA interference (RNAi) experiments is complicated by scope, experimental variability and network signaling robustness

  • An Over representation approaches (ORA) that takes advantage of known connectivity between gene set members provides a complementary view to the results provided by conventional enrichment methods and identify signaling events that are enriched for small interfering RNA (siRNA) hits

  • Protein Interaction Permutation Analysis (PIPA) Algorithm For a given gene set, protein interaction permutation analysis (PIPA) identifies the probability of seeing an observed number of protein interactions between siRNA hits by chance

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Summary

Introduction

A systems biology interpretation of genome-scale RNA interference (RNAi) experiments is complicated by scope, experimental variability and network signaling robustness. Over representation approaches (ORA), such as the Hypergeometric or z-score, are an established statistical framework used to associate RNA interference effectors to biologically annotated gene sets or pathways. These methods, do not directly take advantage of our growing understanding of the interactome. Genome-scale siRNA phenotype screens consist of thousands of targeted perturbation experiments to identify significant effectors on a phenotype of interest, such as cell growth As these high-throughput screens become more automated and less expensive, there is a growing demand to associate siRNA hits with the interactome. Knockdowns that cause an impaired growth phenotype provide a glimpse to uncommonly sensitive areas of cell signaling

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