Programmable Genotoxins Targeted Against Prostate

Abstract

The purpose of our research is to develop better chemotherapeutic drugs for the treatment of prostate cancers. We have used chemical synthetic methods to create bifunctional compounds consisting of a ligand for the androgen receptor linked to a reactive alkylating group that can produce covalent damage in cellular DNA. It is proposed that such damage would persist in tumor cells that express the androgen receptor (AR) because the DNA lesions would be masked by their association with the AR. Initial work prepared chemically modified non-steroid and steroid derivatives that were tested for their affinity for the AR. This work led to the identification of structures that when attached to a linker molecule still retained good affinity for the AR. Subsequently, a number of bifunctional compounds were constructed and tested in biochemical assays and in prostate cancer cells in culture. We have identified a lead compound containing an 11beta-substituted steroid linked to an aniline mustard. This compound damaged DNA and retained good affinity for the AR. We discovered, however, that when added to prostate cancer cells in culture its AR binding activity is lost. We have prepared radiolabled compounds to study their metabolic fate both in cell culture and in animal models.

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Document Details

Document Type
Technical Report
Publication Date
Mar 01, 2001
Accession Number
ADA391961

Entities

People

  • John M. Essigmann

Organizations

  • Massachusetts Institute of Technology

Tags

DTIC Thesaurus Topics

  • Androgen Receptors
  • Androgens
  • Biomedical Research
  • Cancer
  • Chemical Compounds
  • Chemical Synthesis
  • Chemistry
  • Culture Techniques
  • Health Services
  • Lead Compounds
  • Metabolism
  • Molecules
  • Neoplasms
  • Organic Compounds
  • Prostate
  • Prostate Cancer

Fields of Study

  • Biology

Readers

  • Molecular and Cellular Biochemistry
  • Organic Chemistry
  • Prostate Cancer Biology.