Abstract

Breast cancer is a biologically and clinically heterogeneous disease that makes clinical management challenging. Cancer genomics can identify candidate genetic lesions, but functional studies are required to dissect which changes impact disease progression, treatment efficacy, and development of resistance. Core B was conceived to facilitate functional studies in breast cancer by introducing state-of-the-art RNA interference technology to the Program Project. It will incorporate and implement new technology developed by Dr. Scott Lowe (the core leader) and Dr. Gregory Hannon (CSHL) based on RNA interference mediated by short hairpin RNAs (shRNAs). The core concentrates its efforts on providing shRNAs expressed from the miR-30 scaffold ? which Drs. Lowe and Hannon have optimized over the last 7 years ? as a tool to potently and reversibly repress gene expression in cultured cells and in animals. This team has also developed powerful strategies for regulated RNAi to inducibly suppress gene expression, as well as phenotype-based screens using multiplexed RNAi formats; they also have developed rapid methods for producing inducible shRNA transgenic mice for spatial, temporal, and reversible control of the expression of any gene, in vivo. Core B will provide such advanced RNAi tools to program investigators, and continue to develop and optimize RNAi methodology for controlling gene function in breast cancer models. These services will be broadly divided into two components, the first, involving vector production and screening services and, the second, support for production of inducible shRNA transgenic mice. Among these services include the implementation of an RNAi ?sensor? assay that enables the identification of highly potent shRNAs against genes of interest. The Core will benefit from existing infrastructure at MSKCC and interact with each of the proposed Projects, thus providing cost effective services and a source of interaction for the Program. Implementation of the RNAi tools provided by this core is expected to advance the ability to functional studies throughout the Program, and will stimulate the development of new technologies (shRNA libraries, and mouse models) that will be useful for the breast cancer research community

Public Health Relevance

Core B will provide innovative RNAi tools to Project members for performing function studies in cultured cells and in mice, thereby adding new technology to facilitate both the discovery and mechanistic efforts of in the Program. Studies using shRNA transgenic mice have the ability to revolutionize breast cancer animal modeling by enabling the spatial, temporal, and reversible control of endogenous gene expression to study breast cancer initiation and maintenance

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA094060-13
Application #
9099739
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2016-07-01
Budget End
2017-06-30
Support Year
13
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
Sloan-Kettering Institute for Cancer Research
Department
Type
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Er, Ekrem Emrah; Valiente, Manuel; Ganesh, Karuna et al. (2018) Pericyte-like spreading by disseminated cancer cells activates YAP and MRTF for metastatic colonization. Nat Cell Biol 20:966-978
Chen, Chun-Chin; Kass, Elizabeth M; Yen, Wei-Feng et al. (2017) ATM loss leads to synthetic lethality in BRCA1 BRCT mutant mice associated with exacerbated defects in homology-directed repair. Proc Natl Acad Sci U S A 114:7665-7670
Gao, Hua; Chakraborty, Goutam; Zhang, Zhanguo et al. (2016) Multi-organ Site Metastatic Reactivation Mediated by Non-canonical Discoidin Domain Receptor 1 Signaling. Cell 166:47-62
Ebbesen, Saya H; Scaltriti, Maurizio; Bialucha, Carl U et al. (2016) Pten loss promotes MAPK pathway dependency in HER2/neu breast carcinomas. Proc Natl Acad Sci U S A 113:3030-5
Malladi, Srinivas; Macalinao, Danilo G; Jin, Xin et al. (2016) Metastatic Latency and Immune Evasion through Autocrine Inhibition of WNT. Cell 165:45-60
Rodrik-Outmezguine, Vanessa S; Okaniwa, Masanori; Yao, Zhan et al. (2016) Overcoming mTOR resistance mutations with a new-generation mTOR inhibitor. Nature 534:272-6
Chen, Qing; Boire, Adrienne; Jin, Xin et al. (2016) Carcinoma-astrocyte gap junctions promote brain metastasis by cGAMP transfer. Nature 533:493-498
Kass, Elizabeth M; Lim, Pei Xin; Helgadottir, Hildur R et al. (2016) Robust homology-directed repair within mouse mammary tissue is not specifically affected by Brca2 mutation. Nat Commun 7:13241
She, Qing-Bai; Gruvberger-Saal, Sofia K; Maurer, Matthew et al. (2016) Integrated molecular pathway analysis informs a synergistic combination therapy targeting PTEN/PI3K and EGFR pathways for basal-like breast cancer. BMC Cancer 16:587
Yang, C; Li, Z; Bhatt, T et al. (2016) Acquired CDK6 amplification promotes breast cancer resistance to CDK4/6 inhibitors and loss of ER signaling and dependence. Oncogene :

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