The Lmo2 Oncogene Initiates Leukemia in Mice by Inducing Thymocyte Self-Renewal

MP McCormack, LF Young, S Vasudevan, CA de Graaf… - Science, 2010 - science.org
MP McCormack, LF Young, S Vasudevan, CA de Graaf, R Codrington, TH Rabbitts, SM Jane
Science, 2010science.org
The LMO2 oncogene causes a subset of human T cell acute lymphoblastic leukemias (T-
ALL), including four cases that arose as adverse events in gene therapy trials. To investigate
the cellular origin of LMO2-induced leukemia, we used cell fate mapping to study mice in
which the Lmo2 gene was constitutively expressed in the thymus. Lmo2 induced self-
renewal of committed T cells in the mice more than 8 months before the development of
overt T-ALL. These self-renewing cells retained the capacity for T cell differentiation but …
The LMO2 oncogene causes a subset of human T cell acute lymphoblastic leukemias (T-ALL), including four cases that arose as adverse events in gene therapy trials. To investigate the cellular origin of LMO2-induced leukemia, we used cell fate mapping to study mice in which the Lmo2 gene was constitutively expressed in the thymus. Lmo2 induced self-renewal of committed T cells in the mice more than 8 months before the development of overt T-ALL. These self-renewing cells retained the capacity for T cell differentiation but expressed several genes typical of hematopoietic stem cells (HSCs), suggesting that Lmo2 might reactivate an HSC-specific transcriptional program. Forced expression of one such gene, Hhex, was sufficient to initiate self-renewal of thymocytes in vivo. Thus, Lmo2 promotes the self-renewal of preleukemic thymocytes, providing a mechanism by which committed T cells can then accumulate additional genetic mutations required for leukemic transformation.
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