Abstract

The focus of this program project is the study of MLL associated leukemogenesis. The long-term goal is to understand the process of leukemogenesis associated with MLL-fusion genes resulting from translocations involving chromosome 11 band q23. These leukemia's include several subsets: de novo adult and pediatric leukemia, therapy-related leukemia subsequent to treatment of other cancers with topoisomerase-II inhibitors, and infant leukemia that apparently arise in utero. Projects 1 and 2 will address aspects of the initiation and progression of the leukemogenic process: Project I will explore the hypothesis that apoptotic nucleases play a significant role in the generation of the chromosome 11 translocations that initiate the leukemic process both in treatment related leukemia and in infant leukemia. It will also search for mutations that allow cells to survive apoptosis after undergoing rearrangements, and will search for MLL rearrangements in human patients subjected to cytotoxic therapy. Project 2 will try to identify secondary mutations that push the initiated clones into clinically detectable leukemia using animal models. The fusion proteins of MLL conserve the N-terminal part of MLL, and replace its C-terminal part with one from the partner proteins. Project 2 will also try to dissect these different domains of MLL to determine which ones are ? Essential for, and which ones are inhibitory of transformation. Project 3 will ask a related question testing the hypothesis that Cyp33, a protein that binds the third PHD finger of MLL, inhibits the Tran activating activity of MLL by controlling the function of its repression domain and its effect on target gene chromatin structure. The role of Cyp33 as a sensor for non-coding RNAs generated in the intergenic regions of the MLL target genes will also be studied in Project 3. Project 4 will test the hypothesis that MLL regulates its target genes through modifications in the histones and chromatin structure of their promoters and enhancers. It also will look at the possibility that modifications (i.e: acetylation) of the MLL protein itself modulate its function as a trans-activator of the target genes. A DNA-Microarray Core and a Retroviral Core will provide help to these projects. These studies will provide a better understanding of the leukemogenic process and its relationship to hematopoiesis regulation by epigenetic processes and its disruption by genetic mutation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
3P01CA105049-01A2S1
Application #
7127116
Study Section
Subcommittee G - Education (NCI)
Program Officer
Ogunbiyi, Peter
Project Start
2005-09-23
Project End
2010-06-30
Budget Start
2005-09-29
Budget End
2006-06-30
Support Year
1
Fiscal Year
2005
Total Cost
$124,041
Indirect Cost

  Institution

Name
Loyola University Chicago
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
791277940
City
Maywood
State
IL
Country
United States
Zip Code
60153

  Publications

Wang, Q F; Li, Y J; Dong, J F et al. (2014) Regulation of MEIS1 by distal enhancer elements in acute leukemia. Leukemia 28:138-46
Chen, Allen M; Zahra, Talia; Daly, Megan E et al. (2013) Definitive radiation therapy without chemotherapy for human papillomavirus-positive head and neck cancer. Head Neck 35:1652-6
Risner, Laurie E; Kuntimaddi, Aravinda; Lokken, Alyson A et al. (2013) Functional specificity of CpG DNA-binding CXXC domains in mixed lineage leukemia. J Biol Chem 288:29901-10
Chauhan, Chhavi; Zraly, Claudia B; Parilla, Megan et al. (2012) Histone recognition and nuclear receptor co-activator functions of Drosophila cara mitad, a homolog of the N-terminal portion of mammalian MLL2 and MLL3. Development 139:1997-2008
Do, To Uyen; Ho, Bay; Shih, Shyh-Jen et al. (2012) Zinc Finger Nuclease induced DNA double stranded breaks and rearrangements in MLL. Mutat Res 740:34-42
Shih, Shyh-Jen; Fass, Joseph; Buffalo, Vincent et al. (2012) Multiple clonal MLL fusions in a patient receiving CHOP-based chemotherapy. Br J Haematol 159:50-7
Wang, Qian-Fei; Wu, George; Mi, Shuangli et al. (2011) MLL fusion proteins preferentially regulate a subset of wild-type MLL target genes in the leukemic genome. Blood 117:6895-905
Beaudette-Zlatanova, Britte C; Knight, Katherine L; Zhang, Shubin et al. (2011) A human thymic epithelial cell culture system for the promotion of lymphopoiesis from hematopoietic stem cells. Exp Hematol 39:570-9
Chang, Ming-Jin; Wu, Hongyu; Achille, Nicholas J et al. (2010) Histone H3 lysine 79 methyltransferase Dot1 is required for immortalization by MLL oncogenes. Cancer Res 70:10234-42
Du, Nga; Baker, Pamela M; Do, To Uyen et al. (2010) 11q21.1-11q23.3 Is a site of intrinsic genomic instability triggered by irradiation. Genes Chromosomes Cancer 49:831-43

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