Figure 2.
Effect of lenalidomide treatment on hematopoiesis in CrbnI391Vmice. (A) Peripheral blood counts of WT and CrbnI391V/I391V mice after 21 days of treatment with 50 mg/kg lenalidomide or vehicle. CD11b+ Gr1+ granulocyte and platelet data are pooled from 2 treated cohorts of mice treated for 21 to 24 days. n ≥ 3 for data shown, which are representative of 4 independent experiments. (B) Hematopoietic stem and progenitor cell compartments in WT and CrbnI391V/I391V mice after 21 days of treatment with 50 mg/kg lenalidomide or vehicle. LK cells are Lineage− c-Kit+; ST-HSC are Lineage− c-Kit+ Sca1+ CD48− CD150−; LT-HSC are Lineage− c-Kit+ Sca1+ CD48− CD150+. n ≥ 3 for data shown, which are representative of 3 independent experiments. Lineage markers are CD3, B220, CD11b, Gr1, and Ter119. (C) Hematopoietic progenitor compartments in WT and CrbnI391V/I391V mice after 28 or 35 days of treatment with 50 mg/kg lenalidomide or vehicle. MPP are Lineage− c-Kit+ Sca1+ CD48+ CD150−; CMP are Lineage− c-Kit+ Sca1− CD34+ CD16/32mid; GMP are Lineage− c-Kit+ Sca1− CD34+ CD16/32hi; MEP are Lineage− c-Kit+ Sca1− CD34+ CD16/32low. Lineage markers are CD3, B220, CD11b, Ter119, and Gr1. n ≥ 5 for data shown, which are combined from 2 independent experiments. (D) Erythroid differentiation subsets as defined by CD71 and TER119 staining in the bone marrow from WT and CrbnI391V/I391V mice after 28 days of treatment with vehicle or 50 mg/kg lenalidomide. n ≥ 4 for data shown, which are representative of 3 independent experiments. **P < .005. P values calculated using unpaired Student t test. Error bars are standard error of the mean. LSK, Lineage− c-Kit+ Sca1+; ns, not significant; PLT, platelet; WBC, white blood cell.