Structural and Functional Analyses of the Six1 Transcriptional Complex for Anti-Breast Cancer Drug Design

Abstract

Cancer and normal development share many properties. During normal development, genes are activated that stimulate proliferation, migration, invasion, vascularization, and that alter cell survival. These gene products are often lost once organ development is complete. In cancer, many developmental genes are re-activated, stimulating the aforementioned processes out of context. The Six1 gene encodes a transcription factor that induces the expression of a large number of genes that are involved in the proliferation, survival, migration, and invasion of cells during embryonic development. In most tissues, Six1 expression is lost once development is complete. However, Six1 is reactivated in many breast cancers, where as many as 90% of metastatic tumors overexpress the gene. Six1 plays a role in both tumor initiation and metastasis of breast cancers, and its inhibition dramatically diminishes both tumor cell proliferation and metastasis in a number of mouse cancer models. Because Six1 is expressed during embryogenesis, lost in most adult tissues, and re-expressed in tumors, we believe it is an ideal drug target whose inactivation will inhibit tumor cell proliferation and metastasis with limited side effects. Our goal in this proposal is to lay the foundation for developing novel, tumor-specific chemotherapeutic agents for breast cancer. This will be accomplished by coupling the expertise of a cancer/molecular biologist with a structural biologist/biochemist. Within the proposal, we will identify multiple avenues for targeting the Six1 transcriptional complex, and use an innovative rational drug design and complementary high throughput screeing (HTS) approach to identify small molecule inhibitors of the Six1 complex. The Six1 transcriptional complex has never before been clinically targeted- but its inhibition would be expected to inhibit both tumor cell proliferation and metastasis, while sparing normal cells. Such a target is badly needed in breast cancer, where many of

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Document Details

Document Type
Technical Report
Publication Date
Apr 01, 2011
Accession Number
ADA553105

Entities

People

  • Heide L Ford

Organizations

  • University of Colorado Boulder

Tags

DTIC Thesaurus Topics

  • Breast Cancer
  • Cell Line
  • Cell Physiological Processes
  • Cells
  • Chemistry
  • Culture Techniques
  • Data Sets
  • Department Of Defense
  • Indicator Dyes
  • Mammary Glands
  • Medical Personnel
  • Molecular Biology
  • Small Molecules
  • Statistical Analysis
  • Stem Cells
  • Students
  • Therapy

Fields of Study

  • Biology

Readers

  • Molecular Biology and Genetics
  • Oncology (Cancer Research).
  • Systems Analysis and Design