Myeloproliferative disease in transgenic mice expressing P230 Bcr/Abl: longer disease latency, thrombocytosis, and mild leukocytosis-Reference-Cited by-同舟云学术

Myeloproliferative disease in transgenic mice expressing P230 Bcr/Abl: longer disease latency, thrombocytosis, and mild leukocytosis

Published:2003-07-01 Issue:1 Volume:102 Page:320-323
ISSN:0006-4971
Container-title:Blood
language:en
Short-container-title:

Author:

Inokuchi Koiti¹,Dan Kazuo¹,Takatori Miyuki¹,Takahuji Hidemasa¹,Uchida Naoya¹,Inami Mitsuharu¹,Miyake Koichi¹,Honda Hiroaki¹,Hirai Hisamaru¹,Shimada Takashi¹

Affiliation:

1. From the Division of Hematology, Department of Internal Medicine, Department of Biochemistry and Molecular Biology, and Research Center for Life Science, Nippon Medical School, Tokyo, Japan; Department of Developmental Biology, Division of Radiation Biology and Medicine, Hiroshima University, Japan; and Department of Hematology/Oncology, Graduate School of Medicine, University of Tokyo, Japan.

Abstract

Abstract P230 Bcr/Abl has been associated with indolent myeloproliferative disease (MPD). We generated transgenic mice expressing P230Bcr/Abl driven by the promoter of the long terminal repeat of the murine stem cell virus of the MSCV neo P230 BCR/ABL vector. Two founder mice exhibited mild granulocytosis and marked thrombocytosis and developed MPD. The disease of one founder mouse, no. 13, progressed to extramedullary myeloblastic crisis in the liver at 12 months old. The other founder mouse, no. 22, was found to have chronic-phase MPD with large populations of megakaryocytes and granulocytes in an enlarged spleen. The transgenic progeny of no. 22 clearly exhibited MPD at 15 months old. These results showed that P230Bcr/Abl had leukemogenic properties and induced MPD. The phenotype of the MPD caused by P230Bcr/Abl was characterized by mild granulocytosis, a high platelet count, infiltration of megakaryocytes in some organs, and a longer disease latency compared with the MPD caused by P210Bcr/Abl. (Blood. 2003;102:320-323)

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

Link

http://ashpublications.org/blood/article-pdf/102/1/320/1688644/h81303000320.pdf

Reference22 articles.

1. Shtivelman E, Lifshitz B, Gale RP, Canaani E. Fused transcript of abl and bcr genes in chronic myelogenous leukemia. Nature.1985;315: 550-554.

2. Melo JV. The diversity of BCR-ABL fusion proteins and their relationship to leukemia type. Blood.1996;88: 2375-2384.

3. Emilia G, Luppi M, Marasca R, Torelli G. Relationship between BCR/ABL fusion proteins and leukemia phenotype [letter]. Blood.1997;89: 3889.

4. Pane F, Frigeri F, Sindona M, et al. Neutrophilic-chronic myeloid leukemia: distinct disease with a specific molecular marker (Bcr/Abl with C3/A2 junction). Blood.1996;88: 2410-2414.

5. Briz M, Vilches C, Cabrera R, Fores R, Fernandez MN. Typical chronic myelogenous leukemia with e19a2 junction BCR/ABL transcript [letter]. Blood.1997;90: 5024.

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