Efficient and Rapid Induction of a Chronic Myelogenous Leukemia-Like Myeloproliferative Disease in Mice Receiving P210 bcr/abl-Transduced Bone Marrow

Expression of the 210-kD bcr/abl fusion oncoprotein can cause achronic myelogenous leukemia (CML)-like disease in mice receiving bonemarrow cells transduced by bcr/abl-encoding retroviruses. However,previous methods failed to yield this disease at a frequency sufficientenough to allow for its use in the study of CML pathogenesis. Toovercome this limitation, we have developed an efficient and reproducible method for inducing a CML-like disease in mice receiving P210 bcr/abl-transduced bone marrow cells. All mice receiving P210bcr/abl-transduced bone marrow cells succumb to a myeloproliferative disease between 3 and 5 weeks after bone marrow transplantation. Themyeloproliferative disease recapitulates many of the hallmarks of humanCML and is characterized by high white blood cell counts and extensiveextramedullary hematopoiesis in the spleen, liver, bone marrow, andlungs. Use of a retroviral vector coexpressing P210 bcr/abl and greenfluorescent protein shows that the vast majority of bcr/abl-expressingcells are myeloid. Analysis of the proviral integration pattern showsthat, in some mice, the myeloproliferative disease is clonal. Inmultiple mice, the CML-like disease has been transplantable, inducing asimilar myeloproliferative syndrome within 1 month of transfer tosublethally irradiated syngeneic recipients. The disease in many ofthese mice has progressed to the development of acute lymphoma/leukemiaresembling blast crisis. These results demonstrate that murine CMLrecapitulates important features of human CML. As such, it should be anexcellent model for addressing specific issues relating to thepathogenesis and treatment of this disease.