Figure 1
Comparison of hematopoiesis and survival of JAK2-V617F–transgenic mice activated by 3 different Cre transgenes. (A) Blood counts and survival after induction with pIpC or tamoxifen. (B) Ratio between human JAK2-V617F and mouse Jak2 in the BM of JAK2-V617F–transgenic mice at 10 and 34 weeks. (C) Blood counts and survival after transplantation of 2 × 106 BM cells collected from JAK2-V617F mouse donors into lethally irradiated recipients. (D) Ratio between human JAK2-V617F and mouse Jak2 in the BM of hosts transplanted with JAK2-V617F BM cells. The BM samples were collected 35 weeks after transplantation. Mx indicates MxCre;FF1 mice (red symbols); Scl, SclCre;FF1 mice (green symbols); Vav, VavCre;FF1 mice (blue symbols); and WT, wild-type controls (black symbols). Note that all SclCre;FF1 mice died within 30 weeks after tamoxifen induction and therefore no blood counts were available beyond this time point. Survival is shown as Kaplan-Meier curves. (E-F) Numbers of hematopoietic progenitors assessed by colony assays in methylcellulose or collagen-based medium. BFU-E indicates burst forming unit erythroid; and Tpo, thrombopoietin. BM from 3 mice per group were analyzed on duplicate plates. (G-H) Percentages of LSK cells within the lineage− BM cell population of nontransplanted mice induced by pIpC or tamoxifen (G) and in the lethally irradiated hosts transplanted with the BM cells from JAK2-V617F mice (H). (I) Blood counts and survival of SclCre;FF1 mice with Jak2fl/+ or Jak2fl/fl genotypes after induction with tamoxifen. (J) Ratio between human JAK2-V617F and mouse Jak2 in the BM of SclCre;FF1 mice with the Jak2+/+, Jak2fl/+, or Jak2fl/fl genotypes. Error bars represent SEM. One-way ANOVA is shown for comparisons between wild-type and transgenic mice. ns indicates not significant. *P ≤ .05; **P ≤ .01; ***P ≤ .001.

Comparison of hematopoiesis and survival of JAK2-V617F–transgenic mice activated by 3 different Cre transgenes. (A) Blood counts and survival after induction with pIpC or tamoxifen. (B) Ratio between human JAK2-V617F and mouse Jak2 in the BM of JAK2-V617F–transgenic mice at 10 and 34 weeks. (C) Blood counts and survival after transplantation of 2 × 106 BM cells collected from JAK2-V617F mouse donors into lethally irradiated recipients. (D) Ratio between human JAK2-V617F and mouse Jak2 in the BM of hosts transplanted with JAK2-V617F BM cells. The BM samples were collected 35 weeks after transplantation. Mx indicates MxCre;FF1 mice (red symbols); Scl, SclCre;FF1 mice (green symbols); Vav, VavCre;FF1 mice (blue symbols); and WT, wild-type controls (black symbols). Note that all SclCre;FF1 mice died within 30 weeks after tamoxifen induction and therefore no blood counts were available beyond this time point. Survival is shown as Kaplan-Meier curves. (E-F) Numbers of hematopoietic progenitors assessed by colony assays in methylcellulose or collagen-based medium. BFU-E indicates burst forming unit erythroid; and Tpo, thrombopoietin. BM from 3 mice per group were analyzed on duplicate plates. (G-H) Percentages of LSK cells within the lineage BM cell population of nontransplanted mice induced by pIpC or tamoxifen (G) and in the lethally irradiated hosts transplanted with the BM cells from JAK2-V617F mice (H). (I) Blood counts and survival of SclCre;FF1 mice with Jak2fl/+ or Jak2fl/fl genotypes after induction with tamoxifen. (J) Ratio between human JAK2-V617F and mouse Jak2 in the BM of SclCre;FF1 mice with the Jak2+/+, Jak2fl/+, or Jak2fl/fl genotypes. Error bars represent SEM. One-way ANOVA is shown for comparisons between wild-type and transgenic mice. ns indicates not significant. *P ≤ .05; **P ≤ .01; ***P ≤ .001.

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