Every single cancer survivor fears relapse. While being free of the primary tumor after treatment is encouraging, it is emotionally devastating to step out of the clinic after a yearly checkup with a diagnosis of metastatic disease. Approximately 90% of cancer lethality is due to metastasis - the spreading of primary tumor cells to distant organs. Despite a dramatic increase in early screening methods and comprehensive treatment regimens for primary breast tumors, the overall mortality of patients who relapsed with metastatic cancer in the US has not changed in the past two decades. Clinical failure in treating metastatic tumors is largely due to the evolutionary nature of tumor metastasis. In order to survive and establish secondary tumors in a different tissue microenvironment at distant organs, disseminated tumor cells have to adapt (metastatic evolution) to the host environment. Clinically, metastatic tumors exhibit drastically different characteristics from their primary counterpart. Therefore, current cancer treatments, designed based on the features of primary tumors, are rarely effective. Optimal design of breakthrough anti-metastasis therapies relies on our in-depth understanding of the common and functionally important traits during the early metastatic evolution. In this proposed study, we will use breast cancer brain metastasis as model system and take state-of-the-art approaches to trace and analyze a single cancer cell within its precise metastatic microenvironment from the initial moment of metastatic colonization. This collaborative effort from a multidisciplinary team, including a cancer biologist, a computational biologist, a mathematician and a bioinformatician will allow us to: 1) depict the dynamics of gene transcription during the different stages of brain metastasis at single cell level; 2) visualize th behavior of a single colonized metastatic tumor cell and its interaction with the microenvironment through real-time intravital imaging and deep tissue imaging; 3) mathematically integrate molecular (RNA-seq), behavioral (intravital) and structural (deep tissue imaging) information to identify the common and functionally important early metastatic evolutionary traits during the breast cancer brain metastasis in its native tissue context. Shifting the current clinical treatment model relies on new in-depth mechanistic insight obtained through basic and pre-clinical innovative research. Utilizing cutting-edge sequencing and imaging modality in our proposed study, we will have the capacity to systematically dissect traits of early metastatic behavior and discover potential novel therapeutic targets for paradigm-shifting novel adjuvant therapy tailored to specific target metastatic evolution. The conceptual validation from our bold and pioneering attempt proposed in this study will serves as a blueprint for a new category of adjuvant therapies for effective anti-metastasis treatment.

Public Health Relevance

Successful anti-metastasis treatment is rooted deep in our mechanistic understanding of early metastatic evolution and our capability to stop metastatic progression before aggressive outgrowth occurs. Using single cell transcriptome sequencing and multiplexed single cell deep-tissue imaging, we aim to trace and analyze the lineage dynamics of a single cancer cell within its specific metastatic microenvironment from the initial moment of metastatic colonization. The conceptual advances validated from this study will serve as a blueprint for future adjuvant therapies targeting early metastatic evolution, providing more effective cancer treatments.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA194697-01
Application #
8876876
Study Section
Special Emphasis Panel (ZCA1)
Program Officer
Woodhouse, Elizabeth
Project Start
2015-06-01
Project End
2019-05-31
Budget Start
2015-06-01
Budget End
2016-05-31
Support Year
1
Fiscal Year
2015
Total Cost
Indirect Cost
Name
University of Notre Dame
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
824910376
City
Notre Dame
State
IN
Country
United States
Zip Code
46556
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Zhang, Lin; Zhang, Siyuan; Yao, Jun et al. (2015) Microenvironment-induced PTEN loss by exosomal microRNA primes brain metastasis outgrowth. Nature 527:100-104