The current state of preclinical prostate cancer animal models

Kenneth J. Pienta, Cory Abate-Shen, David B. Agus, Ricardo M. Attar, Leland W.K. Chung, Norman M. Greenberg, William C. Hahn, John T. Isaacs, Nora M. Navone, Donna M. Peehl, Jonathon W. Simons, David B. Solit, Howard R. Soule, Terry A. VanDyke, Michael J. Weber, Lily Wu, Robert L. Vessella

Research output: Contribution to journalReview articlepeer-review

96 Scopus citations


Prostate cancer continues to be a major cause of morbidity and mortality in men around the world. The field of prostate cancer research continues to be hindered by the lack of relevant preclinical models to study tumorigenesis and to further development of effective prevention and therapeutic strategies. The Prostate Cancer Foundation held a Prostate Cancer Models Working Group (PCMWG) Summit on August 6th and 7th, 2007 to address these issues. The PCMWG reviewed the state of prostate cancer preclinical models and identified the current limitations of cell line, xenograft and genetically engineered mouse models that have hampered the transition of scientific findings from these models to human clinical trials. In addition the PCMWG identified administrative issues that inhibit the exchange of models and impede greater interactions between academic centers and these centers with industry. The PCMWG identified potential solutions for discovery bottlenecks that include: (1) insufficient number of models with insufficient molecular and biologic diversity to reflect human cancer, (2) a lack of understanding of the molecular events that define tumorigenesis, (3) a lack of tools for studying tumor-host interactions, (4) difficulty in accessing model systems across institutions, and (5) addressing why preclinical studies appear not to be predictive of human clinical trials. It should be possible to apply the knowledge gained molecular and epigenetic studies to develop new cell lines and models that mimic progressive and fatal prostate cancer and ultimately improve interventions.

Original languageEnglish (US)
Pages (from-to)629-639
Number of pages11
Issue number6
StatePublished - May 1 2008


  • Cell lines
  • Genetically engineered
  • Mouse

ASJC Scopus subject areas

  • Oncology
  • Urology


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