Figure 2
Figure 2. hMRP8-NPMc+ transgenic mice develop a nonreactive myeloproliferation with expansion of mature granulocytes/monocytes. (A) Table showing the total number of mice analyzed from different transgenic lines, their age range, and myeloproliferation (MP) penetrance involving either BM or spleen. (B) Composite data from age-matched littermates of indicated genotypes demonstrating splenomegaly in NPMc+ transgenic mice (mean ± SEM; NT, n = 5; NPMc+ 28, n = 5). **P < .01. Spleen masses are 160 ± 60.8 mg for NT (n = 5) versus 567 ± 284 mg for NPMc+ 28 (n = 5; P = .014). (C) Histopathologic sections of BM and spleen from representative NT and NPMc+ transgenic mice. (i) NT BM (hematoxylin and eosin, original magnification, ×1000). (ii) NT BM cytospin (original magnification, ×1000). represents an erythroblast; , granulocytes. (iii) NPMc+ BM (hematoxylin and eosin, original magnification, ×1000). (iv) NPMc+ BM cytospin (original magnification, ×1000). represent granulocytes. (v) NT spleen (hematoxylin and eosin, original magnification, ×40). (vi) NT spleen (hematoxylin and eosin, original magnification, ×400). (vii) NPMc+ spleen (hematoxylin and eosin, original magnification, ×40). represents areas of expanded red pulp with extramedullary hematopoiesis. (viii) NPMc+ spleen (hematoxylin and eosin, original magnification, ×400). represents extramedullary hematopoiesis. (D) Flow cytometric analysis of single-cell suspensions of BM and spleen from representative NT and NPMc+ transgenic mice demonstrates an increase in granulocytic/monocytic (Mac-1+;Gr-1+) and mature myeloid (Mac-1+;cKit−) cells with a corresponding decrease in the amount of B (B220+) and T (CD3+) lymphoid cell populations. (E) Quantification of granulocytic/monocytic (Mac-1+;Gr-1+), mature myeloid (Mac-1+/cKit+), B cells (B2200+), and T cells (CD3+) in BM and spleen of age-matched NT and NPMc+ transgenic mice analyzed as in panel D (mean ± SEM; NT, n = 6; NPMc+ 28, n = 6). *P < .05. **P < .01. ***P < .001. n.s. indicates not statistically significant.

hMRP8-NPMc+ transgenic mice develop a nonreactive myeloproliferation with expansion of mature granulocytes/monocytes. (A) Table showing the total number of mice analyzed from different transgenic lines, their age range, and myeloproliferation (MP) penetrance involving either BM or spleen. (B) Composite data from age-matched littermates of indicated genotypes demonstrating splenomegaly in NPMc+ transgenic mice (mean ± SEM; NT, n = 5; NPMc+ 28, n = 5). **P < .01. Spleen masses are 160 ± 60.8 mg for NT (n = 5) versus 567 ± 284 mg for NPMc+ 28 (n = 5; P = .014). (C) Histopathologic sections of BM and spleen from representative NT and NPMc+ transgenic mice. (i) NT BM (hematoxylin and eosin, original magnification, ×1000). (ii) NT BM cytospin (original magnification, ×1000). represents an erythroblast; , granulocytes. (iii) NPMc+ BM (hematoxylin and eosin, original magnification, ×1000). (iv) NPMc+ BM cytospin (original magnification, ×1000). represent granulocytes. (v) NT spleen (hematoxylin and eosin, original magnification, ×40). (vi) NT spleen (hematoxylin and eosin, original magnification, ×400). (vii) NPMc+ spleen (hematoxylin and eosin, original magnification, ×40). represents areas of expanded red pulp with extramedullary hematopoiesis. (viii) NPMc+ spleen (hematoxylin and eosin, original magnification, ×400). represents extramedullary hematopoiesis. (D) Flow cytometric analysis of single-cell suspensions of BM and spleen from representative NT and NPMc+ transgenic mice demonstrates an increase in granulocytic/monocytic (Mac-1+;Gr-1+) and mature myeloid (Mac-1+;cKit) cells with a corresponding decrease in the amount of B (B220+) and T (CD3+) lymphoid cell populations. (E) Quantification of granulocytic/monocytic (Mac-1+;Gr-1+), mature myeloid (Mac-1+/cKit+), B cells (B2200+), and T cells (CD3+) in BM and spleen of age-matched NT and NPMc+ transgenic mice analyzed as in panel D (mean ± SEM; NT, n = 6; NPMc+ 28, n = 6). *P < .05. **P < .01. ***P < .001. n.s. indicates not statistically significant.

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