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1 lymphocyte reductions to support a reactive granulocytosis.
2 iated by the concomitant induction of marked granulocytosis.
3 ce characterized by massive splenomegaly and granulocytosis.
4 d myelopoiesis leading to thrombocytosis and granulocytosis.
5 rapid development of hepatosplenomegaly and granulocytosis.
6 tor (G-CSF), a principal cytokine-regulating granulocytosis.
7 2 deficient mice succumbed from overwhelming granulocytosis.
9 of Sema3E in mice results in increased lung granulocytosis, airway hyperresponsiveness, mucus overpr
15 splenomegaly, extramedullary erythropoiesis, granulocytosis and thrombocytopaenia secondary to a bloc
17 f human PV, characterized by erythrocytosis, granulocytosis, extramedullary hematopoiesis, and bone m
20 mulating factor (G-CSF) as a means to induce granulocytosis in donors has rekindled interest in this
21 These data suggest that erythrocytosis and granulocytosis in JAK2(V617F) mice are the net result of
24 testinal tissues, characterized by pulmonary granulocytosis, increased Th2/Th1 T cell ratios in trach
25 a strongly argue against the clinical use of granulocytosis-inducing hematopoietic stem cell mobiliza
26 r the intestinal microbiota in regulation of granulocytosis, neutrophil homeostasis and host resistan
27 eated with G-CSF showed less than 50% of the granulocytosis observed in identically treated WT mice.
29 ytic dysplasia, and a propensity for chronic granulocytosis; phenotypes that closely resemble those o
30 CD97 deficiency did not appear to stimulate granulocytosis secondary to peripheral inflammation and
32 mia, and Icsbp(-/-) mice exhibit progressive granulocytosis with evolution to blast crisis, similar t