Abstract

Our proposed studies will address major clinical challenges associated with differential drug treatment response, focusing on advanced prostate cancer. Our overall approach is based upon the co-clinical trial paradigm, in which genetically-engineered mouse (GEM) models are assayed for drug response to provide information that can be incorporated into patient treatment regimens. Here, we propose a novel augmented co- clinical paradigm that uses analyses of tissue-specific organoids together with GEM models to expedite investigation of differential drug response and drug synergy, as well as sophisticated computational systems biology approaches to identify molecular regulators of drug response that are conserved from mouse models to human cancer. In preliminary studies, we have established methods for novel three-dimensional culture of tumor organoids, which display drug responses characteristic of the GEM models from which they were established. Furthermore, we have used computational systems methods to generate gene regulatory networks (interactomes) for both mouse and human prostate cancer, and have demonstrated their utility for cross-species identification of candidate master regulators of tumor aggressiveness. We have expanded these systems biology approaches for prediction of drug response in preclinical studies and to extrapolate these data to human prostate cancer. Based on these preliminary studies, we hypothesize that systematic analysis of drug response in genetically-engineered mouse (GEM) models followed by cross-species systems analyses can inform human cancer treatment by enabling the systematic evaluation of optimal drug treatments in distinct tumor contexts as well as by identifying patients who are most likely to respond to treatment. Thus, our proposed research will pursue the broad objective of identifying the underlying mechanisms of differential drug response in distinct prostate tumor contexts. Our specific plans are:
Aim 1 : To identify optimal drug treatments for specific tumor contexts, we will use organoid lines derived from a series of GEM models of prostate cancer to assay response to a range of drugs, including agents currently used for treatment of advanced prostate cancer. These findings from organoid models will be experimentally validated in GEM models in vivo.
Aim 2 : To analyze molecular mechanisms of drug response and drug synergy, we will use cross-species computational systems approaches to identify genes and pathways that regulate drug response in human prostate cancer. These results will be experimentally validated in organoid, GEM, and xenograft models. Impact: Our proposed studies directly address the broad goals of the Oncology Models Forum, since they introduce new experimental paradigms for effective translation of mouse models to achieve unmet translational needs. Our newly developed organoid models and cross-species computational analyses and validation will be of broad value to members of the Oncology Forum and are sharable through the NCIP Hub.

Public Health Relevance

Despite considerable recent advances in the development of targeted therapeutics, many patients still succumb to cancer, either because their tumors do not respond to therapy or because they initially respond but ultimately acquire resistance. In this application, we propose the development of an augmented co-clinical paradigm to utilize state-of-the-art genetically-engineered mouse models, innovative organoid models grown in tissue culture, and computational systems biology approaches to perform comprehensive analyses of drug response in prostate cancer. Our proposed studies will address major clinical challenges associated with differential treatment responses, while our general approach will be broadly applicable for many types of cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA196662-03
Application #
9516951
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Forry, Suzanne L
Project Start
2016-07-01
Project End
2019-06-30
Budget Start
2018-07-01
Budget End
2019-06-30
Support Year
3
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Arriaga, Juan M; Abate-Shen, Cory (2018) Genetically Engineered Mouse Models of Prostate Cancer in the Postgenomic Era. Cold Spring Harb Perspect Med :
Chua, Chee Wai; Epsi, Nusrat J; Leung, Eva Y et al. (2018) Differential requirements of androgen receptor in luminal progenitors during prostate regeneration and tumor initiation. Elife 7:
Le Magnen, Clémentine; Shen, Michael M; Abate-Shen, Cory (2018) Lineage Plasticity in Cancer Progression and Treatment. Annu Rev Cancer Biol 2:271-289
Lee, Suk Hyung; Hu, Wenhuo; Matulay, Justin T et al. (2018) Tumor Evolution and Drug Response in Patient-Derived Organoid Models of Bladder Cancer. Cell 173:515-528.e17
Shen, Michael M; Rubin, Mark A (2018) Prostate Cancer Research at the Crossroads. Cold Spring Harb Perspect Med :
Li, Jia J; Shen, Michael M (2018) Prostate Stem Cells and Cancer Stem Cells. Cold Spring Harb Perspect Med :
Dutta, Aditya; Panja, Sukanya; Virk, Renu K et al. (2017) Co-clinical Analysis of a Genetically Engineered Mouse Model and Human Prostate Cancer Reveals Significance of NKX3.1 Expression for Response to 5?-reductase Inhibition. Eur Urol 72:499-506
Owczarek, Tomasz B; Kobayashi, Takashi; Ramirez, Ricardo et al. (2017) ARF Confers a Context-Dependent Response to Chemotherapy in Muscle-Invasive Bladder Cancer. Cancer Res 77:1035-1046
Zou, Min; Toivanen, Roxanne; Mitrofanova, Antonina et al. (2017) Transdifferentiation as a Mechanism of Treatment Resistance in a Mouse Model of Castration-Resistant Prostate Cancer. Cancer Discov 7:736-749