Abstract

APL is associated with reciprocal translocations always involving the RAR[1] locus which variably fuses to the PML, PLZF, NPM or NuMA genes (referred to as X genes), two aberrant fusion genes are thus generated which encode X-RAR[1] and RAR[1]-X fusion proteins. We hypothesize that the various X/RAR[1] fusion proteins disrupt the genetic events synergistically cooperate with X/RAR[1] leading to APL. We will test this hypothesis in vivo, by a direct genetic approach, with the following Specific Aims: 1) To define the leukemogenic potential of the fusion proteins of APL in transgenic mice (TM). Hemopoiesis, leukemogenesis, and response to RA and As2O3 treatments will be analyzed in X/RAR[1] and RAR[1]/X TM in which the expression of the transgene is restricted to the myeloid/promyelocytic hemopoietic compartment through the use of a human Cathepsin-G (hCG) minigene expression vector. hCG-X-RAR[1] and RAR[1]-X lines will be intercrossed to elucidate the possible cooperative roles of these molecules in leukemogenesis. 2) To establish the role of X and RAR[1] proteins in APL promotion and progression. We will test whether the reduction to heterozygosity of X and/or RAR[1] in APL, or their functional inactivation by the fusion products is a crucial event in APL leukemogenesis. To this end, we will interbreed hCG-X/RAR[1] and RAR[1]/X TM with PML, PLZF or RAR[1] Knock-Out mice to reproduce in vivo the genetic complexity observed in the APL blast, and study hemopoiesis and leukemogenesis in the resulting transgene combinations. 3) To define the mechanisms of leukemogenesis and transcriptional repression in APL. We will study in vivo, in TM, as well as in vitro, in transcriptional and cell culture assays, the biochemical and oncogenic activities of X/RAR[1] and RAR[1] proteins harboring mutations in ligand binding, repressive and activating domains. 4) To study leukemogenesis and the concept of dominance/interference by X-RAR[1] on X function utilizing an in vivo """"""""Knock-in"""""""" approach. We will introduce the PLZF-RAR[1] fusion gene in the PLZF locus in mouse ES cells by a Knock-in approach. We will study the resulting phenotype and leukemogenesis by the PLZF-RAR[1] fusion protein in vivo, in mice and/or chimeras generated from these ES cells, as well as in vitro, in ES cells differentiation experiments. 5) To identify target genes of the oncogenic activity the various X-RAR[1] and RAR[1]-X fusion proteins. We will utilize purified promyelocytic cell populations from our TM to identify, on a comparative basis, target genes relevant for their oncogenic functions utilizing microarray and chromatin immunoprecipitation techniques. 6) To identify additional genetic events contributing to APL pathogenesis. Retroviral insertional mutagenesis in PML-RAR[1] and PLZF-RAR[1] TM, and Spectral Karyotyping (SKY) will be utilized to identify additional genetic events in APL leukemogenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA074031-05
Application #
6376392
Study Section
Pathology B Study Section (PTHB)
Project Start
1997-06-01
Project End
2005-05-31
Budget Start
2001-06-01
Budget End
2002-05-31
Support Year
5
Fiscal Year
2001
Total Cost
$374,625
Indirect Cost

  Institution

Name
Sloan-Kettering Institute for Cancer Research
Department
Type
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Khanna-Gupta, Arati; Abayasekara, Nirmalee; Levine, Michelle et al. (2012) Up-regulation of translation eukaryotic initiation factor 4E in nucleophosmin 1 haploinsufficient cells results in changes in CCAAT enhancer-binding protein ? activity: implications in myelodysplastic syndrome and acute myeloid leukemia. J Biol Chem 287:32728-37
Carracedo, Arkaitz; Ito, Keisuke; Pandolfi, Pier Paolo (2011) The nuclear bodies inside out: PML conquers the cytoplasm. Curr Opin Cell Biol 23:360-6
Cheng, Ke; Sportoletti, Paolo; Ito, Keisuke et al. (2010) The cytoplasmic NPM mutant induces myeloproliferation in a transgenic mouse model. Blood 115:3341-5
Lin, Hui-Kuan; Wang, Guocan; Chen, Zhenbang et al. (2009) Phosphorylation-dependent regulation of cytosolic localization and oncogenic function of Skp2 by Akt/PKB. Nat Cell Biol 11:420-32
Ito, Keisuke; Bernardi, Rosa; Pandolfi, Pier Paolo (2009) A novel signaling network as a critical rheostat for the biology and maintenance of the normal stem cell and the cancer-initiating cell. Curr Opin Genet Dev 19:51-9
Rego, E M; Ruggero, D; Tribioli, C et al. (2006) Leukemia with distinct phenotypes in transgenic mice expressing PML/RAR alpha, PLZF/RAR alpha or NPM/RAR alpha. Oncogene 25:1974-9
Shen, Tian Huai; Lin, Hui-Kuan; Scaglioni, Pier Paolo et al. (2006) The mechanisms of PML-nuclear body formation. Mol Cell 24:331-9
Matsushita, Hiromichi; Scaglioni, Pier Paolo; Bhaumik, Mantu et al. (2006) In vivo analysis of the role of aberrant histone deacetylase recruitment and RAR alpha blockade in the pathogenesis of acute promyelocytic leukemia. J Exp Med 203:821-8
Gurrieri, Carmela; Capodieci, Paola; Bernardi, Rosa et al. (2004) Loss of the tumor suppressor PML in human cancers of multiple histologic origins. J Natl Cancer Inst 96:269-79
Sukhai, Mahadeo A; Wu, Xuemei; Xuan, Yali et al. (2004) Myeloid leukemia with promyelocytic features in transgenic mice expressing hCG-NuMA-RARalpha. Oncogene 23:665-78

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