The Multidimensional Perturbation Value

Author:

Hutz Janna E.1,Nelson Thomas1,Wu Hua1,McAllister Gregory1,Moutsatsos Ioannis1,Jaeger Savina A.1,Bandyopadhyay Somnath2,Nigsch Florian3,Cornett Ben1,Jenkins Jeremy L.1,Selinger Douglas W.1

Affiliation:

1. Novartis Institutes for Biomedical Research, Cambridge, MA, USA

2. Clinical Biomarkers, Bristol-Myers Squibb, Princeton Junction, NJ, USA

3. Novartis Institutes for Biomedical Research, Basel, Switzerland

Abstract

Screens using high-throughput, information-rich technologies such as microarrays, high-content screening (HCS), and next-generation sequencing (NGS) have become increasingly widespread. Compared with single-readout assays, these methods produce a more comprehensive picture of the effects of screened treatments. However, interpreting such multidimensional readouts is challenging. Univariate statistics such as t-tests and Z-factors cannot easily be applied to multidimensional profiles, leaving no obvious way to answer common screening questions such as “Is treatment X active in this assay?” and “Is treatment X different from (or equivalent to) treatment Y?” We have developed a simple, straightforward metric, the multidimensional perturbation value (mp-value), which can be used to answer these questions. Here, we demonstrate application of the mp-value to three data sets: a multiplexed gene expression screen of compounds and genomic reagents, a microarray-based gene expression screen of compounds, and an HCS compound screen. In all data sets, active treatments were successfully identified using the mp-value, and simulations and follow-up analyses supported the mp-value’s statistical and biological validity. We believe the mp-value represents a promising way to simplify the analysis of multidimensional data while taking full advantage of its richness.

Publisher

Elsevier BV

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