Cell-Based Fuzzy Metrics Enhance High-Content Screening (HCS) Assay Robustness

Author:

Azegrouz Hind1,Karemore Gopal1,Torres Alberto2,Alaíz Carlos M.2,Gonzalez Ana M.2,Nevado Pedro1,Salmerón Alvaro1,Pellinen Teijo3,del Pozo Miguel A.3,Dorronsoro José R.2,Montoya María C.1

Affiliation:

1. Cellomics Unit, Department of Vascular Biology and Inflammation, Centro Nacional de Investigaciones Cardiovasculares (CNIC), Madrid, Spain

2. Machine Learning Group, Escuela Politécnica Superior, Universidad Autónoma de Madrid, Madrid, Spain

3. Integrin Signalling Lab, Department of Vascular Biology and Inflammation, Centro Nacional de Investigaciones Cardiovasculares (CNIC), Madrid, Spain

Abstract

High-content screening (HCS) allows the exploration of complex cellular phenotypes by automated microscopy and is increasingly being adopted for small interfering RNA genomic screening and phenotypic drug discovery. We introduce a series of cell-based evaluation metrics that have been implemented and validated in a mono-parametric HCS for regulators of the membrane trafficking protein caveolin 1 (CAV1) and have also proved useful for the development of a multiparametric phenotypic HCS for regulators of cytoskeletal reorganization. Imaging metrics evaluate imaging quality such as staining and focus, whereas cell biology metrics are fuzzy logic–based evaluators describing complex biological parameters such as sparseness, confluency, and spreading. The evaluation metrics were implemented in a data-mining pipeline, which first filters out cells that do not pass a quality criterion based on imaging metrics and then uses cell biology metrics to stratify cell samples to allow further analysis of homogeneous cell populations. Use of these metrics significantly improved the robustness of the monoparametric assay tested, as revealed by an increase in Z′ factor, Kolmogorov-Smirnov distance, and strict standard mean difference. Cell biology evaluation metrics were also implemented in a novel supervised learning classification method that combines them with phenotypic features in a statistical model that exceeded conventional classification methods, thus improving multiparametric phenotypic assay sensitivity.

Publisher

Elsevier BV

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