A genetic ensemble approach for gene-gene interaction identification

A Beygelzimer; A Tsymbal; AA Motsinger; AG Heidema; Albert Y Zomaya; B McKinney; Bing B Zhou; C Greene; D Arking; D Nielsen; D Quigley; D Ruta; D Ruta; D Thomas; D Velez; E Rogaeva; G Bontempi; G Brown; H Cordell; H Cordell; H Zhang; J Cleary; J Hoh; J Kittler; J Moore; JC Barrett; JH Moore; JH Moore; JL Haines; Joshua WK Ho; L Breiman; L Briollais; L Lam; LE Mechanic; LI Kuncheva; LW Hahn; M Kudo; M Ritchie; MR Nelson; P Lucek; Pengyi Yang; R Duerr; R Klein; R Somorjai; S Cantor; S Fisher; S Schmidt; SK Musani; TG Dietterich; X Chen; Y Freund; Y Tomita; Z Zhang

A genetic ensemble approach for gene-gene interaction identification

Authors: A Beygelzimer
A Tsymbal
AA Motsinger
AG Heidema
Albert Y Zomaya
B McKinney
Bing B Zhou
C Greene
D Arking
D Nielsen
D Quigley
D Ruta
D Ruta
D Thomas
D Velez
E Rogaeva
G Bontempi
G Brown
H Cordell
H Cordell
H Zhang
J Cleary
J Hoh
J Kittler
J Moore
JC Barrett
JH Moore
JH Moore
JL Haines
Joshua WK Ho
L Breiman
L Briollais
L Lam
LE Mechanic
LI Kuncheva
LW Hahn
M Kudo
M Ritchie
MR Nelson
P Lucek
Pengyi Yang
R Duerr
R Klein
R Somorjai
S Cantor
S Fisher
S Schmidt
SK Musani
TG Dietterich
X Chen
Y Freund
Y Tomita
Z Zhang
Publication date: 1 January 2010
Publisher: BioMed Central
Doi

Abstract

Abstract Background It has now become clear that gene-gene interactions and gene-environment interactions are ubiquitous and fundamental mechanisms for the development of complex diseases. Though a considerable effort has been put into developing statistical models and algorithmic strategies for identifying such interactions, the accurate identification of those genetic interactions has been proven to be very challenging. Methods In this paper, we propose a new approach for identifying such gene-gene and gene-environment interactions underlying complex diseases. This is a hybrid algorithm and it combines genetic algorithm (GA) and an ensemble of classifiers (called genetic ensemble). Using this approach, the original problem of SNP interaction identification is converted into a data mining problem of combinatorial feature selection. By collecting various single nucleotide polymorphisms (SNP) subsets as well as environmental factors generated in multiple GA runs, patterns of gene-gene and gene-environment interactions can be extracted using a simple combinatorial ranking method. Also considered in this study is the idea of combining identification results obtained from multiple algorithms. A novel formula based on pairwise <it>double fault </it>is designed to quantify the degree of complementarity. Conclusions Our simulation study demonstrates that the proposed genetic ensemble algorithm has comparable identification power to Multifactor Dimensionality Reduction (MDR) and is slightly better than Polymorphism Interaction Analysis (PIA), which are the two most popular methods for gene-gene interaction identification. More importantly, the identification results generated by using our genetic ensemble algorithm are highly complementary to those obtained by PIA and MDR. Experimental results from our simulation studies and real world data application also confirm the effectiveness of the proposed genetic ensemble algorithm, as well as the potential benefits of combining identification results from different algorithms.</p