Figure 4.
ERG variants are LOF in an in vivo leukemia model driven by ERG overexpression. (A) Enforced expression of ERG WT and WT-like variants (P116R, M219I) in mice led to the development of erythro-megakaryocytic leukemia within 220 days. (B) mCherry engraftment over time in the PB of mice. Numbering refers to 3 ERG WT mice that succumbed to disease (Figure 5A). (C) Infiltration of ERG WT/mCherry+ transplanted FLCs into recipient mouse BM, spleen, and PB as measured by fluorescence-activated cell sorter (FACS) analysis. Recipient mouse number 3 shown is representative of all ERG WT and WT-like (P116R, M219I) mice. (D) ERG WT and WT-like variant mice developed mCherry+ erythro-megakaryocytic leukemia with cKit+ and CD71+ expression. FACS plots of a representative ERG WT leukemia are shown. Nonleukemic (ie, mCherry–) BM and spleen cells are shown as comparison.

ERG variants are LOF in an in vivo leukemia model driven by ERG overexpression. (A) Enforced expression of ERG WT and WT-like variants (P116R, M219I) in mice led to the development of erythro-megakaryocytic leukemia within 220 days. (B) mCherry engraftment over time in the PB of mice. Numbering refers to 3 ERG WT mice that succumbed to disease (Figure 5A). (C) Infiltration of ERG WT/mCherry+ transplanted FLCs into recipient mouse BM, spleen, and PB as measured by fluorescence-activated cell sorter (FACS) analysis. Recipient mouse number 3 shown is representative of all ERG WT and WT-like (P116R, M219I) mice. (D) ERG WT and WT-like variant mice developed mCherry+ erythro-megakaryocytic leukemia with cKit+ and CD71+ expression. FACS plots of a representative ERG WT leukemia are shown. Nonleukemic (ie, mCherry) BM and spleen cells are shown as comparison.

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