Abstract

Cancer is a major disease burden and one hope of changing this is to develop new treatments through a? better understanding of the disease. Recent discoveries concerning the activities of short RNAs in mammals? may provide both new insights and new treatments of cancer. A common goal of this Program is to? investigate the roles of short RNAs, such as microRNAs, in regulation of genes in normal and cancer cells.? There is strong and rapidly growing evidence suggesting that changes in miRNA regulation are related to? malignant transformation and in fact could be a critical event in oncogenic transformation. The function of? the mir-17-92-1 cluster which is frequently overexpressed/amplified in a subset of human cancers will be? investigated by creation of specific mutations of these microRNAs in the context of mouse models of cancer.? Changes in microRNA populations in normal cells and tumor cells of the same developmental state will be? analyzed using both bead-array technology as well as new cloning technology. Vectors with regulated? expression of a short hairpin RNA which generates a specific siRNA for silencing a gene will be developed? for transgenic analysis of pathways. Additionally, methods will be tested for screening of small libraries of? shRNA-lentiviral vectors to identify genes which, when silenced, either inhibit or stimulate tumor? development. Furthermore, libraries of retro viral vectors expressing shRNAs will be used in screens to? identify (a) genes that modulate the proliferation and/or survival of pRB-deficient cells , (b) genes that? modulate the rate of development of a K-ras-driven lung cancer model, and (c) genes important for the? differentiation of ES cells. The potential role of short RNAs in transcriptional silencing will be investigated in? embryonic stem cells. These processes could be important for epigenetic silencing and genomic stability of? cancer cells. ES cells will also be studied for the role of miRNAs in development and proliferation. Changes? in the spectrum of microRNAs and siRNAs during T-cell development will be characterized using a cloning? technology which requires small amounts of RNAi. Activation of the Arf promoter is an early signal in? oncogenic transformation. This promoter is silenced under normal conditions by the E2F3B protein, linking? the p19Arf-mdm2-p53 pathway to the p16INK4a-cycD/cdk4-pRB-EdF pathway. The role of E2F3B complexes? and other E2F factors in regulation of the Arf promoter will be studied.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
2P01CA042063-21A1
Application #
7187894
Study Section
Special Emphasis Panel (ZCA1-GRB-S (O1))
Program Officer
Mietz, Judy
Project Start
1997-05-01
Project End
2011-08-31
Budget Start
2006-09-15
Budget End
2007-08-31
Support Year
21
Fiscal Year
2006
Total Cost
$1,388,333
Indirect Cost

  Institution

Name
Massachusetts Institute of Technology
Department
Internal Medicine/Medicine
Type
Schools of Arts and Sciences
DUNS #
001425594
City
Cambridge
State
MA
Country
United States
Zip Code
02139

  Publications

Gao, Ang; Shrinivas, Krishna; Lepeudry, Paul et al. (2018) Evolution of weak cooperative interactions for biological specificity. Proc Natl Acad Sci U S A 115:E11053-E11060
Dubbury, Sara J; Boutz, Paul L; Sharp, Phillip A (2018) CDK12 regulates DNA repair genes by suppressing intronic polyadenylation. Nature 564:141-145
Parisi, Tiziana; Balsamo, Michele; Gertler, Frank et al. (2018) The Rb tumor suppressor regulates epithelial cell migration and polarity. Mol Carcinog 57:1640-1650
Sabari, Benjamin R; Dall'Agnese, Alessandra; Boija, Ann et al. (2018) Coactivator condensation at super-enhancers links phase separation and gene control. Science 361:
Chiu, Anthony C; Suzuki, Hiroshi I; Wu, Xuebing et al. (2018) Transcriptional Pause Sites Delineate Stable Nucleosome-Associated Premature Polyadenylation Suppressed by U1 snRNP. Mol Cell 69:648-663.e7
Mori, Munemasa; Hazan, Renin; Danielian, Paul S et al. (2017) Cytoplasmic E2f4 forms organizing centres for initiation of centriole amplification during multiciliogenesis. Nat Commun 8:15857
Braun, Christian J; Stanciu, Monica; Boutz, Paul L et al. (2017) Coordinated Splicing of Regulatory Detained Introns within Oncogenic Transcripts Creates an Exploitable Vulnerability in Malignant Glioma. Cancer Cell 32:411-426.e11
Tammela, Tuomas; Sanchez-Rivera, Francisco J; Cetinbas, Naniye Malli et al. (2017) A Wnt-producing niche drives proliferative potential and progression in lung adenocarcinoma. Nature 545:355-359
Sasi, Nanda Kumar; Bhutkar, Arjun; Lanning, Nathan J et al. (2017) DDK Promotes Tumor Chemoresistance and Survival via Multiple Pathways. Neoplasia 19:439-450
JnBaptiste, Courtney K; Gurtan, Allan M; Thai, Kevin K et al. (2017) Corrigendum: Dicer loss and recovery induce an oncogenic switch driven by transcriptional activation of the oncofetal Imp1-3 family. Genes Dev 31:1066

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