A comparison of machine learning algorithms for chemical toxicity classification using a simulated multi-scale data model

A Statnikov; AB Okey; AF Fliri; AF Fliri; AM Molinaro; C Helma; C Sima; CP Austin; D Krewski; DJ Dix; E Walum; EE Ntzani; Fathi Elloumi; GM Williams; GV Paolini; H Almuallim; H Toivonen; H Wang; Imran Shah; J Inglese; J Klekota; J Lamb; J Zhang; JPVanden Heuvel; JS Melnick; K Tietjen; LB Moore; LH Li; M Bredel; M McMillian; MT Martin; N Ancona; N Bhogal; N Japkowicz; P Baldi; P Pudil; PJ O'Brien; R Benigni; R Burbridge; R Kikkawa; R Kohavi; R Woodrow Setzer; Richard Judson; RL Strausberg; SC Smith; SG Baker; U Scherf; Y Sun; Z Lepp; Zhen Li

A comparison of machine learning algorithms for chemical toxicity classification using a simulated multi-scale data model

Authors: A Statnikov
AB Okey
AF Fliri
AF Fliri
AM Molinaro
C Helma
C Sima
CP Austin
D Krewski
DJ Dix
E Walum
EE Ntzani
Fathi Elloumi
GM Williams
GV Paolini
H Almuallim
H Toivonen
H Wang
Imran Shah
J Inglese
J Klekota
J Lamb
J Zhang
JPVanden Heuvel
JS Melnick
K Tietjen
LB Moore
LH Li
M Bredel
M McMillian
MT Martin
N Ancona
N Bhogal
N Japkowicz
P Baldi
P Pudil
PJ O'Brien
R Benigni
R Burbridge
R Kikkawa
R Kohavi
R Woodrow Setzer
Richard Judson
RL Strausberg
SC Smith
SG Baker
U Scherf
Y Sun
Z Lepp
Zhen Li
Publication date: 1 May 2008
Publisher: BioMed Central
Doi

Abstract

Abstract Background Bioactivity profiling using high-throughput <it>in vitro </it>assays can reduce the cost and time required for toxicological screening of environmental chemicals and can also reduce the need for animal testing. Several public efforts are aimed at discovering patterns or classifiers in high-dimensional bioactivity space that predict tissue, organ or whole animal toxicological endpoints. Supervised machine learning is a powerful approach to discover combinatorial relationships in complex <it>in vitro/in vivo </it>datasets. We present a novel model to simulate complex chemical-toxicology data sets and use this model to evaluate the relative performance of different machine learning (ML) methods. Results The classification performance of Artificial Neural Networks (ANN), K-Nearest Neighbors (KNN), Linear Discriminant Analysis (LDA), Naïve Bayes (NB), Recursive Partitioning and Regression Trees (RPART), and Support Vector Machines (SVM) in the presence and absence of filter-based feature selection was analyzed using K-way cross-validation testing and independent validation on simulated <it>in vitro </it>assay data sets with varying levels of model complexity, number of irrelevant features and measurement noise. While the prediction accuracy of all ML methods decreased as non-causal (irrelevant) features were added, some ML methods performed better than others. In the limit of using a large number of features, ANN and SVM were always in the top performing set of methods while RPART and KNN (k = 5) were always in the poorest performing set. The addition of measurement noise and irrelevant features decreased the classification accuracy of all ML methods, with LDA suffering the greatest performance degradation. LDA performance is especially sensitive to the use of feature selection. Filter-based feature selection generally improved performance, most strikingly for LDA. Conclusion We have developed a novel simulation model to evaluate machine learning methods for the analysis of data sets in which in vitro bioassay data is being used to predict in vivo chemical toxicology. From our analysis, we can recommend that several ML methods, most notably SVM and ANN, are good candidates for use in real world applications in this area.</p