Abstract

Therapy-related myelodysplastic syndrome (t-MDS) and acute myeloid leukemia (t-AML) are distinct clinical syndromes that have been recognized as late complications of cytotoxic therapy (either radiation and/or chemotherapy) used in the treatment of both malignant and nonmalignant diseases. We reported previously that nonrandom chromosomal abnormalities are commonly observed in the malignant cells of patients with t-MDS/t-AML. In our updated series, we observed loss of an entire chromosome 5 and/or 7 or a deletion of the long arm of these chromosomes [del(5q)/del(7q)] in 97 of 129 (75%) patients whom we examined. By comparing the deletions of chromosome 5 observed in these patients, we have determined that a small region (critical region), consisting of band 5q31, is consistently deleted in all patients, suggesting that loss of a gene(s) located within this segment is involved in the pathogenesis of these myeloid disorders. Of note is the fact that this region contains the genes encoding four hematopoietic growth factors; however, no direct role for these genes in myeloid leukemogenesis has been demonstrated. We now propose to use cytogenetic and molecular approaches to map the critical region of 5q by using in situ chromosomal hybridization and radiolabeled or biotin-labeled probes, and physical mapping techniques, such as pulsed-field gel electrophoresis (performed in collaboration with Dr. Carol Westbrook). Similarly, cytogenetic analysis of patients who have t-MDS/t-AML with deletions or other rearrangements of 7q and gene mapping techniques will be used to prepare a genetic map of the critical region of chromosome 7. To determine if DNA rearrangements have occurred within the critical region of the normal 5 homologue, we will then use this map to examine DNA derived from leukemia cells of t-AML patients with a del(5q) or other rearrangements of 5q, and from t-AML patients who do not have a cytogenetic abnormality of 5q. The detection of DNA rearrangements will identify candidate """"""""suppressor"""""""" genes that may be integrally involved in leukemogenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
2P01CA040046-06A1
Application #
3795054
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
6
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Type
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Clay-Gilmour, Alyssa I; Hahn, Theresa; Preus, Leah M et al. (2017) Genetic association with B-cell acute lymphoblastic leukemia in allogeneic transplant patients differs by age and sex. Blood Adv 1:1717-1728
Churpek, Jane E; Marquez, Rafael; Neistadt, Barbara et al. (2016) Inherited mutations in cancer susceptibility genes are common among survivors of breast cancer who develop therapy-related leukemia. Cancer 122:304-11
Sasaki, Mark M; Skol, Andrew D; Hungate, Eric A et al. (2016) Whole-exome Sequence Analysis Implicates Rare Il17REL Variants in Familial and Sporadic Inflammatory Bowel Disease. Inflamm Bowel Dis 22:20-7
Stoddart, Angela; Qian, Zhijian; Fernald, Anthony A et al. (2016) Retroviral insertional mutagenesis identifies the del(5q) genes, CXXC5, TIFAB and ETF1, as well as the Wnt pathway, as potential targets in del(5q) myeloid neoplasms. Haematologica 101:e232-6
Hungate, Eric A; Vora, Sapana R; Gamazon, Eric R et al. (2016) A variant at 9p21.3 functionally implicates CDKN2B in paediatric B-cell precursor acute lymphoblastic leukaemia aetiology. Nat Commun 7:10635
Shankar, Sunita; Pitchiaya, Sethuramasundaram; Malik, Rohit et al. (2016) KRAS Engages AGO2 to Enhance Cellular Transformation. Cell Rep 14:1448-1461
Vasanthakumar, Aparna; Arnovitz, Stephen; Marquez, Rafael et al. (2016) Brca1 deficiency causes bone marrow failure and spontaneous hematologic malignancies in mice. Blood 127:310-3
Wong, Jasmine C; Weinfurtner, Kelley M; Alzamora, Maria Del Pilar et al. (2015) Functional evidence implicating chromosome 7q22 haploinsufficiency in myelodysplastic syndrome pathogenesis. Elife 4:
Sasaki, Mark M; Skol, Andrew D; Bao, Riyue et al. (2015) Integrated genomic analysis suggests MLL3 is a novel candidate susceptibility gene for familial nasopharyngeal carcinoma. Cancer Epidemiol Biomarkers Prev 24:1222-8
Sundaravel, Sriram; Duggan, Ryan; Bhagat, Tushar et al. (2015) Reduced DOCK4 expression leads to erythroid dysplasia in myelodysplastic syndromes. Proc Natl Acad Sci U S A 112:E6359-68

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