Therapeutic Mechanism of BET Bromodomain Inhibitor in Breast

Abstract

Genomic profiling of the MCF7 breast cancer cell line using BRD4 ChIP-seq and DNase-seq revealed BRD4 ChIP-seq and DNase-seq to be highly similar. We discovered that the BET inhibitor JQ1 tends to be more effective in slowing the growth of basal rather than luminal breast cancer cell lines. The initial gene expression response of a basal breast cancer cell line, SUM159, on treatment with JQ1, is predominated by the down-regulation of gene expression and this down-regulation is highly associated with BRD4 occupied genomic loci. By 24h of JQ1 treatment secondary effects dominate the gene expression pattern and BRD4 binding no longer predicts gene expression changes. Long-term treatment of SUM159 with JQ1 results in this cell line becoming insensitive to JQ1 and adopting a gene expression pattern that is more luminal-like. Long-term exposure of SUM159 cells to JQ1 leads to drug resistance that is acquired through a mechanism that allows BRD4 to bind to chromatin in a bromodomain independent manner.

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Document Details

Document Type
Technical Report
Publication Date
Dec 01, 2015
Accession Number
AD1008455

Entities

People

  • Xiaole Shirley Liu

Organizations

  • Dana–Farber Cancer Institute

Tags

DTIC Thesaurus Topics

  • Androgen Receptors
  • Breast Cancer
  • Cell Line
  • Cell Physiological Processes
  • Cells
  • Chemistry
  • Computational Biology
  • Confocal Microscopy
  • Cultured Cells
  • Data Analysis
  • Diseases And Disorders
  • Drug Resistance
  • Gene Expression
  • Genetics
  • Health Services
  • Medical Personnel
  • Neoplasms

Fields of Study

  • Biology

Readers

  • Breast cancer cell signaling and growth regulation.
  • Military History
  • Molecular Genetics