Abstract

The overall objective of this proposal is to understand MLL-AF4, also known as t(4;l1), leukemia. This is the most common leukemia in infants and has a poor prognosis; it is also seen in older children and adults. We have recently developed """"""""knock-in"""""""" technology to produce murine embryonic stem (ES) MLL-AF4 cells. We demonstrated that MLL-AF4 fusion protein is anti-apoptotic in ES cells and blocks hematopoietic differentiation in more mature cells. We predict that mice with leukemia derived from MLL-AF4 ES cells will have the same specific phenotype seen in human MLL-AF4 leukemia. We will evaluate the hypothesis that the poor prognosis of human MLL-AF4 leukemia results from resistance to apoptosis; in humans, apoptosis occurs in good prognosis leukemias following growth factor deprivation or chemotherapy but not in MLL-AF4 leukemia. We have three revised specific aims: (1) To evaluate the hypothesis that fusion gene is anti-apoptotic and the AF4 fusion gene is critical for this effect. Differentiation will be studied using embryoid body and hematopoietic colony culture systems. Conditional MLL-AF4 expression systems will be developed to control gene expression and permit survival of viable progenitor cells. (2) To evaluate the hypothesis that the effects of MLL-AF4 fusion gene are cell-type specific. (3) To study mice with MLL-AF4 or MLL-AF9 fusion gene leukemia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA087053-03
Application #
6633776
Study Section
Pathology B Study Section (PTHB)
Program Officer
Mufson, R Allan
Project Start
2001-07-01
Project End
2005-06-30
Budget Start
2003-07-01
Budget End
2004-06-30
Support Year
3
Fiscal Year
2003
Total Cost
$277,324
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Pathology
Type
Schools of Medicine
DUNS #
555917996
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Bindels, Eric M J; Havermans, Marije; Lugthart, Sanne et al. (2012) EVI1 is critical for the pathogenesis of a subset of MLL-AF9-rearranged AMLs. Blood 119:5838-49
Kumar, Ashish R; Yao, Qing; Li, Quanzhi et al. (2011) t(4;11) leukemias display addiction to MLL-AF4 but not to AF4-MLL. Leuk Res 35:305-9
Kumar, Ashish R; Sarver, Aaron L; Wu, Baolin et al. (2010) Meis1 maintains stemness signature in MLL-AF9 leukemia. Blood 115:3642-3
Kumar, Ashish R; Li, Quanzhi; Hudson, Wendy A et al. (2009) A role for MEIS1 in MLL-fusion gene leukemia. Blood 113:1756-8
Chen, Weili; Kumar, Ashish R; Hudson, Wendy A et al. (2008) Malignant transformation initiated by Mll-AF9: gene dosage and critical target cells. Cancer Cell 13:432-40
Yao, Qing; Weigel, Brenda; Kersey, John (2007) Synergism between etoposide and 17-AAG in leukemia cells: critical roles for Hsp90, FLT3, topoisomerase II, Chk1, and Rad51. Clin Cancer Res 13:1591-600
Chen, Weili; Li, Quanzhi; Hudson, Wendy A et al. (2006) A murine Mll-AF4 knock-in model results in lymphoid and myeloid deregulation and hematologic malignancy. Blood 108:669-77
Yao, Q; Nishiuchi, R; Kitamura, T et al. (2005) Human leukemias with mutated FLT3 kinase are synergistically sensitive to FLT3 and Hsp90 inhibitors: the key role of the STAT5 signal transduction pathway. Leukemia 19:1605-12
Yao, Qing; Nishiuchi, Ritsuo; Li, Quanzhi et al. (2003) FLT3 expressing leukemias are selectively sensitive to inhibitors of the molecular chaperone heat shock protein 90 through destabilization of signal transduction-associated kinases. Clin Cancer Res 9:4483-93
Johnson, Jennifer J; Chen, Weili; Hudson, Wendy et al. (2003) Prenatal and postnatal myeloid cells demonstrate stepwise progression in the pathogenesis of MLL fusion gene leukemia. Blood 101:3229-35