Abstract

OVERALL ABSTRACT The common occurrence, marked debilitation and subsequent lethality of prostate cancer (PCa) skeletal metastases has made it a major health concern. In the first fourteen years of this program, we have addressed this important issue, resulting in a major impact on the field of skeletal metastasis research, including promoting concepts such as crosstalk between tumor and bone and the importance of therapeutically targeting the microenvironment, in addition to tumor. This program has resulted in over 220-grant-related publications and set groundwork for several clinical trials. In the current competitive renewal, we further attack this problem by combining leading expertise in PCa research and bone biology. The central theme of this Program is that there is crosstalk between PCa cells and the bone microenvironment that fosters the development and progression of PCa metastasis. This crosstalk promotes the ability of PCa cells to alter the bone microenvironment and render it fertile for tumor growth and chemotherapeutic resistance. To expand on this theme the Program encompasses closely interrelated hypotheses of four scientific projects supported by three cores. Project 1 explores the novel finding that chemotherapy induces fusion of PCa cells to form multinuclear polyploid giant cancer cells (PGCCs) that confer chemoresistance in the bone microenvironment; Project 2 examines the exciting idea that abscisic acid (ABA) induces PCa cells to adopt a phenotype capable of existing in a dormant and chemoresistant state, with the capacity for long-term survival and potential to develop into overt bone metastases; Project 3 explores the surprising role that osteocytes (OCys) play in promoting PCa bone metastasis through activation of a novel growth differentiation factor-15 (GDF15) receptor, GDFN family receptor alpha-like precursor (GFRAL), that subsequently promotes PCa metastatic invasion and growth; Project 4 investigates the novel hypothesis that macrophage efferocytosis (engulfment) of apoptotic PCa cells induces immunosuppressive signaling in the bone microenvironment that subsequently enhances metastatic growth. These projects will be supported by three integral cores: Core A (Administration) that will coordinate reporting, evaluation of progress, advisory board activities, facilitate interactions among the projects and provide biostatistical support; Core B (Animal) will provide mouse models and imaging and assistance with their use and Core C (Bone) will provide expertise with bone histology processing, interpretation, and procurement of human blood and bone marrow samples. This combination of investigators, projects and cores provides a highly synergistic Program that is greater than the sum of its parts and will continue to provide cutting-edge research and leadership in the field of PCa skeletal metastases.

Public Health Relevance

Over 90% of men with advanced prostate cancer (PCa) develop skeletal metastases which subsequently leads to their death. This Program is composed of a multidisciplinary team focused on understanding how the cancer spreads to and thrives in the skeleton so that we can develop methods to prevent or treat the spread of PCa to the bone.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
2P01CA093900-16
Application #
9935666
Study Section
Special Emphasis Panel (ZCA1)
Program Officer
Watson, Joanna M
Project Start
2004-06-05
Project End
2025-05-31
Budget Start
2020-07-02
Budget End
2021-05-31
Support Year
16
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Urology
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Hill, Elliott E; Kim, Jin Koo; Jung, Younghun et al. (2018) Integrin alpha V beta 3 targeted dendrimer-rapamycin conjugate reduces fibroblast-mediated prostate tumor progression and metastasis. J Cell Biochem 119:8074-8083
Axelrod, Haley D; Valkenburg, Kenneth C; Amend, Sarah R et al. (2018) AXL Is a Putative Tumor Suppressor and Dormancy Regulator in Prostate Cancer. Mol Cancer Res :
de Groot, Amber E; Pienta, Kenneth J (2018) Epigenetic control of macrophage polarization: implications for targeting tumor-associated macrophages. Oncotarget 9:20908-20927
Roca, Hernan; Jones, Jacqueline D; Purica, Marta C et al. (2018) Apoptosis-induced CXCL5 accelerates inflammation and growth of prostate tumor metastases in bone. J Clin Invest 128:248-266
Wu, Amy; Liao, David; Kirilin, Vlamimir et al. (2018) Cancer dormancy and criticality from a game theory perspective. Cancer Converg 2:1
Park, Sun H; Keller, Evan T; Shiozawa, Yusuke (2018) Bone Marrow Microenvironment as a Regulator and Therapeutic Target for Prostate Cancer Bone Metastasis. Calcif Tissue Int 102:152-162
Singhal, Udit; Wang, Yugang; Henderson, James et al. (2018) Multigene Profiling of CTCs in mCRPC Identifies a Clinically Relevant Prognostic Signature. Mol Cancer Res 16:643-654
Lee, Eunsohl; Wang, Jingcheng; Jung, Younghun et al. (2018) Reduction of two histone marks, H3k9me3 and H3k27me3 by epidrug induces neuroendocrine differentiation in prostate cancer. J Cell Biochem 119:3697-3705
van der Toom, Emma E; Axelrod, Haley D; de la Rosette, Jean J et al. (2018) Prostate-specific markers to identify rare prostate cancer cells in liquid biopsies. Nat Rev Urol :
Roca, Hernan; McCauley, Laurie K (2018) Efferocytosis and prostate cancer skeletal metastasis: implications for intervention. Oncoscience 5:174-176

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