AML1-ETO Rapidly Induces Acute Myeloblastic Leukemia in Cooperation with the Wilms Tumor Gene, WT1

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2005 Dec 29

PMID 16380455

Citations 55

Authors

Sumiyuki Nishida

Naoki Hosen

Toshiaki Shirakata

Keisuke Kanato

Masashi Yanagihara

Shin-ichi Nakatsuka

Yoshihiko Hoshida

Tsutomu Nakazawa

Yukie Harada

Naoya Tatsumi

Akihiro Tsuboi

Manabu Kawakami

Yoshihiro Oka

Yusuke Oji

Katsuyuki Aozasa

Ichiro Kawase

Haruo Sugiyama

Affiliations

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Abstract

AML1-ETO, a chimeric gene frequently detected in acute myelogenous leukemia (AML), inhibits the differentiation of myeloid progenitors by suppressing genes associated with myeloid differentiation and increases the replating ability of clonogenic myeloid progenitors. However, AML1-ETO alone cannot induce AML and thus additional genetic events are required for the onset of AML. The Wilms tumor gene (WT1), which has been identified as the gene responsible for Wilms tumor, is expressed at high levels in almost all human leukemias. In this study, we have generated transgenic mice (WT1-Tg) that overexpress WT1 in hematopoietic cells to investigate the effects of WT1 on AML1-ETO-associated leukemogenesis. AML1-ETO-transduced bone marrow (BM) cells from WT1-Tg mice exhibited inhibition of myeloid differentiation at more immature stages and higher in vitro colony-forming ability compared with AML1-ETO-transduced BM cells from wild-type mice. Most importantly, all of the mice that received a transplant of AML1-ETO-transduced BM cells from the WT1-Tg mice rapidly developed AML. These results demonstrate that AML1-ETO may exert its leukemogenic function in cooperation with the expression of WT1.

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