Template-driven gene selection procedure

N. Knowlton, I. Dozmorov, K. D. Kyker, R. Saban, C. Cadwell, M. B. Centola, Robert E. Hurst

Research output: Contribution to journalArticlepeer-review

2 Scopus citations

Abstract

The hierarchical clustering and statistical techniques usually used to analyse microarray data do not inherently represent the underlying biology. Herein, a hybrid approach involving characteristics of both supervised and unsupervised learning is presented. This approach is based on template matching in which the interaction of the variables of inherent malignancy and the ability to express the malignant phenotype are modelled. Immortalised normal urothelial cells and bladder cancer cells of different malignancy were grown in conventional two-dimensional tissue culture and in three dimensions on extracellular matrices (ECMs) that were either permissive or restrictive for expression of the malignant phenotype. The transcriptome represents the effects of two variables - inherent malignancy and the modulatory effect of ECM. By assigning values to each of the biological variables of inherent malignancy and the ability to express the malignant phenotype, a template was constructed, which encapsulated the interaction between them. Gene expression correlating both positively and negatively with the template was observed, but when iterative correlations were carried out, the different models for the template converged on the same actual template. A subset of 21 genes was identified, which correlated with two a priori models or an optimised model above the 95% confidence limits identified in a bootstrap resampling with 5000 permutations of the data set. The correlation coefficients of expression of several genes were >0.8. Analysis of upstream transcriptional regulatory elements (TREs) confirmed that these genes were not a randomly selected set of genes. Several TREs were identified as significantly over-expressed in the sample of 20 genes for which TREs were identified, and the high correlations of several genes were consistent with transcriptional co-regulation. The authors suggest that the template method can be used to identify a unique set of genes for further investigation.

Original languageEnglish (US)
Pages (from-to)4-12
Number of pages9
JournalIEE Proceedings Systems Biology
Volume153
Issue number1
DOIs
StatePublished - Jan 2006

Keywords

  • Cancer
  • Cellular biophysics
  • Genetics
  • Iterative methods
  • Medical diagnostic computing
  • Tumours
  • Unsupervised learning

ASJC Scopus subject areas

  • Genetics
  • Molecular Medicine
  • Molecular Biology
  • Biotechnology
  • Cell Biology
  • Modeling and Simulation

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