Abstract

The overall goal of this Program remains to understand how basic cellular processes are altered to promote tumor initiation and progression and how such alterations might make tumor cells vulnerable to specific, targeted interventions. Initiated by James Watson in 1968, the program focused on the action of DNA tumor viruses and in many ways powered the molecular biology revolution. Throughout its history, it revealed the underpinnings of basic biological processes central to cancer development and revealed key oncogenic mechanisms affecting their action. Taking advantage of new biological concepts and technologies emerging from its investigators, the Program has continued to innovate and evolve, with an ever greater focus on mechanisms of immediate biological and therapeutic relevance to the human disease. Over the last funding period, the Program produced fundamentally new insights into DNA replication its coordination in normal and cancer cells, and established that aberrant alternative RNA splicing is an important oncogenic mechanism. The Program has been at the forefront of non-coding RNA biology, providing some of the first evidence that microRNAs can act as oncogenes and tumor suppressors, and influence other key cancer phenotypes. Lastly, the Program has developed and implemented innovative mouse models and used them to identify new oncogenes and tumor suppressors of broad relevance to human cancer. Armed with new technologies developed by Program investigators over the last several years, we will implement a multi pronged approach towards identifying novel oncogenic mechanisms, with an eye towards revealing the vulnerabilities they create. Some elements of the Program are driven from the standpoint of particular cellular processes, such as chromosome replication and segregation or pre-mRNA splicing (Projects 1 and 2), and others implement unbiased approaches informed by changes in the cancer genome or alterations in regulatory networks to focus their studies (Projects 3-5). All Projects converge on potential anticancer targets, whose efficacy can be predicted based upon the nature or state of the cancer cell or its microenvironment. All of the Projects benefit from demonstrable interactions among themselves, taking advantage of complementary approaches and expertise. Moreover, each Project benefits from the four innovative Cores, each of wtiich is lead by outstanding and experienced researchers. Finaily, the Program benefits from, and contributes to, the collaborative environment fostered by the Coid Spring Harbor Laboratory Cancer Center and is at the heart of its activities.

Public Health Relevance

The Program is focused on key oncogenic mechanisms and understanding the vulnerabilities that these lesions create. As such the Project will contribute to our overall understanding of cancer and identify therapeutic targets whose inhibition may lead to the selective targeting of cells with certain cancer genotypes. It will also continue to develop innovative technologies and approaches that will influence cancer research beyond realization of the specific Program goals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
3P01CA013106-41S1
Application #
8519746
Study Section
Special Emphasis Panel (ZCA1-RPRB-0 (O1))
Program Officer
Spalholz, Barbara A
Project Start
1997-02-10
Project End
2016-12-31
Budget Start
2012-05-25
Budget End
2012-12-31
Support Year
41
Fiscal Year
2012
Total Cost
$188,000
Indirect Cost
$88,000

  Institution

Name
Cold Spring Harbor Laboratory
Department
Type
DUNS #
065968786
City
Cold Spring Harbor
State
NY
Country
United States
Zip Code
11724

  Publications

Banito, Ana; Li, Xiang; Laporte, Aimée N et al. (2018) The SS18-SSX Oncoprotein Hijacks KDM2B-PRC1.1 to Drive Synovial Sarcoma. Cancer Cell 34:346-348
Skucha, Anna; Ebner, Jessica; Schmöllerl, Johannes et al. (2018) MLL-fusion-driven leukemia requires SETD2 to safeguard genomic integrity. Nat Commun 9:1983
Banito, Ana; Li, Xiang; Laporte, Aimée N et al. (2018) The SS18-SSX Oncoprotein Hijacks KDM2B-PRC1.1 to Drive Synovial Sarcoma. Cancer Cell 33:527-541.e8
Lin, Kuan-Ting; Ma, Wai Kit; Scharner, Juergen et al. (2018) A human-specific switch of alternatively spliced AFMID isoforms contributes to TP53 mutations and tumor recurrence in hepatocellular carcinoma. Genome Res :
On, Kin Fan; Jaremko, Matt; Stillman, Bruce et al. (2018) A structural view of the initiators for chromosome replication. Curr Opin Struct Biol 53:131-139
Knott, Simon R V; Wagenblast, Elvin; Khan, Showkhin et al. (2018) Asparagine bioavailability governs metastasis in a model of breast cancer. Nature 554:378-381
Shamay, Yosi; Shah, Janki; I??k, Mehtap et al. (2018) Quantitative self-assembly prediction yields targeted nanomedicines. Nat Mater 17:361-368
Tramentozzi, Elisa; Ferraro, Paola; Hossain, Manzar et al. (2018) The dNTP triphosphohydrolase activity of SAMHD1 persists during S-phase when the enzyme is phosphorylated at T592. Cell Cycle 17:1102-1114
Arun, Gayatri; Diermeier, Sarah D; Spector, David L (2018) Therapeutic Targeting of Long Non-Coding RNAs in Cancer. Trends Mol Med 24:257-277
Tarumoto, Yusuke; Lu, Bin; Somerville, Tim D D et al. (2018) LKB1, Salt-Inducible Kinases, and MEF2C Are Linked Dependencies in Acute Myeloid Leukemia. Mol Cell 69:1017-1027.e6

Showing the most recent 10 out of 610 publications