Cancer cell redirection biomarker discovery using a mutual information approach.

PLoS One

Institute for Biological Interfaces of Engineering, Clemson University, Clemson, South Carolina, United States of America.

Published: September 2017

AI Article Synopsis

  • Introducing tumor-derived cells into normal mammary stem cell environments can lead these tumor cells to change and produce normal mammary cells, a process known as cancer cell redirection.
  • An in vitro model was created to simulate how the normal mammary microenvironment redirects cancer cells, allowing researchers to analyze the differences in gene expression between normal, redirected, and tumor cells using RNA profiling.
  • Through analyzing mutual information relationships, researchers identified 20 key molecular signatures from over 35,000 gene expressions, refining it down to 120 core biomarker genes that can differentiate between normal/redirection and tumor states.

Article Abstract

Introducing tumor-derived cells into normal mammary stem cell niches at a sufficiently high ratio of normal to tumorous cells causes those tumor cells to undergo a change to normal mammary phenotype and yield normal mammary progeny. This phenomenon has been termed cancer cell redirection. We have developed an in vitro model that mimics in vivo redirection of cancer cells by the normal mammary microenvironment. Using the RNA profiling data from this cellular model, we examined high-level characteristics of the normal, redirected, and tumor transcriptomes and found the global expression profiles clearly distinguish the three expression states. To identify potential redirection biomarkers that cause the redirected state to shift toward the normal expression pattern, we used mutual information relationships between normal, redirected, and tumor cell groups. Mutual information relationship analysis reduced a dataset of over 35,000 gene expression measurements spread over 13,000 curated gene sets to a set of 20 significant molecular signatures totaling 906 unique loci. Several of these molecular signatures are hallmark drivers of the tumor state. Using differential expression as a guide, we further refined the gene set to 120 core redirection biomarker genes. The expression levels of these core biomarkers are sufficient to make the normal and redirected gene expression states indistinguishable from each other but radically different from the tumor state.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5464651PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0179265PLOS

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