Associations and prognostic interactions between circulating levels of hepcidin, ferritin and inflammatory cytokines in primary myelofibrosis

Pardanani, Animesh; Finke, Christy; Abdelrahman, Ramy A.; Lasho, Terra L.; Tefferi, Ayalew

doi:10.1002/ajh.23406

Cited by 68 publications

(61 citation statements)

References 22 publications

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“…34 These changes in iron metabolism were more pronounced in JAK2;Ex12 mice than in our JAK2-V617F mice, and may contribute to the more prominent erythrocytosis observed in JAK2;Ex12 mice compared with JAK2-V617F mice. In line with a previous report, 38 serum hepcidin levels were significantly elevated in PMF patients with JAK2-V617F ( Figure 7H). Consistently, a trend toward increased TFR1 and ERFE mRNA expression was also noted in BFU-E Hepcidin protein concentration in the serum of PV patients with JAK2 exon 12 mutations (n 5 6) and in MPN patients with the JAK2-V617F mutation (PV, n 5 10; ET, n 5 12; and PMF, n 5 10 patients per group).…”

Section: 32supporting

confidence: 93%

JAK2 exon 12 mutant mice display isolated erythrocytosis and changes in iron metabolism favoring increased erythropoiesis

Grisouard

Kubovčáková

et al. 2016

Blood

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Key Points• Mice expressing a JAK2 exon 12 mutation display isolated erythrocytosis similar to the majority of patients with JAK2 exon 12 mutations.• JAK2 exon 12 mutation induces changes in iron metabolism that increase iron availability to allow maximal production of red cells.Mutations in JAK2 exon 12 are frequently found in patients with polycythemia vera (PV) that do not carry a JAK2-V617F mutation. The majority of these patients display isolated erythrocytosis. We generated a mouse model that expresses JAK2-N542-E543del, the most frequent JAK2 exon 12 mutation found in PV patients. Mice expressing the human JAK2-N542-E543del (Ex12) showed a strong increase in red blood cell parameters but normal neutrophil and platelet counts, and reduced overall survival. Erythropoiesis was increased in the bone marrow and spleen, with normal megakaryopoiesis and absence of myelofibrosis in histopathology. Erythroid progenitors and precursors were increased in hematopoietic tissues, but the numbers of megakaryocytic precursors were unchanged. Phosphorylation Stat3 and Erk1/2 proteins were increased, and a trend toward increased phospho-Stat5 and phospho-Stat1 was noted. However, Stat1 knock out in Ex12 mice induced no changes in platelet or red cell parameters, indicating that Stat1 does not play a central role in mediating the effects of Ex12 signaling on megakaryopoiesis or erythropoiesis. Ex12 mice showed decreased expression of hepcidin and increased expression of transferrin receptor-1 and erythroferrone, suggesting that the strong erythroid phenotype in Ex12 mutant mice is favored by changes in iron metabolism that optimize iron availability to allow maximal production of red cells. (Blood. 2016;128(6):839-851)

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Section: 32supporting

confidence: 93%

JAK2 exon 12 mutant mice display isolated erythrocytosis and changes in iron metabolism favoring increased erythropoiesis

Grisouard

Kubovčáková

et al. 2016

Blood

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“…It is still unclear how the determination of serum hepcidin would fit into diagnostic algorithms for iron deficient states outside of IRIDA 88 . With the exception of hereditary hemochromatosis, in which elevated serum ferritin is accompanied by inappropriately low serum hepcidin, in most other cases serum ferritin and hepcidin levels correlate with each other.…”

Section: Serum Hepcidinmentioning

confidence: 99%

Diagnosis of iron-deficient states

Archer

Brugnara

2015

Critical Reviews in Clinical Laboratory Sciences

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The diagnosis of iron deficiency anemia is typically straightforward, especially when classic biochemical and hematological changes are present in a subject at risk. It can be challenging in the presence of diseases or when it is due to inherited defects of iron metabolism. The identification of iron deficiency prior to anemia development is also difficult. New hematological parameters such as reticulocyte Hb content have expanded the classic ones such as MCV, MCH and MCHC. A variety of hematology analyzers now provide novel parameters to assess cellular hypochromia and microcytosis in both reticulocytes and mature red blood cells. The repertoire of biochemical markers has also been expanded, with iron, transferrin and ferritin being supplemented by circulating transferrin receptor and hepcidin. Molecular identification of functional variants of key iron metabolism determinants has provided explanations for the heritability of some iron metabolism biomarkers. Genetic defects in some of these molecules are responsible for hereditary microcytic anemias, also called atypical microcytic anemias. In this review, we examine the most significant hematological and biochemical markers for iron metabolism, as well as relevant genetic polymorphisms and defects affecting iron handling.

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“…However, the molecular mechanisms underlying MPN-associated myelofibrosis are still not clear. JAK-STAT pathway activation is the main mechanism of myeloproliferation [3,4]; however, available evidence indicates that inflammatory/immune mechanisms play an important role in the phenotype of MPN-associated myelofibrosis by increased production of inflammatory cytokines and reduced number of regulatory T-cells [5][6][7][8][9][10]. From these considerations, it appears that understanding the mechanisms involved in the initiation and progression of MPNassociated myelofibrosis is a pivotal step for the generation of more effective therapeutic approaches.…”

Section: Introductionmentioning

confidence: 99%

Increased plasma nicotinamide phosphoribosyltransferase is associated with a hyperproliferative phenotype and restrains disease progression in MPN‐associated myelofibrosis

et al. 2016

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Myeloproliferative neoplasm (MPN)-associated myelofibrosis is a clonal, neoplastic disorder of the hematopoietic stem cells, in which inflammation and immune dysregulation play an important role. Extracellular nicotinamide phosphoribosyltransferase (eNAMPT), also known as visfatin, is a cytokine implicated in a number of inflammatory and neoplastic diseases. Here plasma levels of eNAMPT in patients with MPN-associated myelofibrosis and their effects on disease phenotype and outcomes were examined. The concordance of eNAMPT levels with the marker of general inflammation high-sensitivity C-reactive protein (hs-CRP) was also studied. A total of 333 MPN-associated myelofibrosis patients (187 males and 146 females) and 31 age-and gender-matched normal-weight healthy subjects were enrolled in the study main body. Levels of eNAMPT and hs-CRP were simultaneously assayed in 209 MPN-associated myelofibrosis patients. Twenty-four polycythemia vera or essential thrombocythemia patients were used as controls. eNAMPT was over expressed in MPN-associated myelofibrosis, and eNAMPT expression was correlated with higher white blood cell count, higher hemoglobin, and higher platelet count, suggesting that eNAMPT is an indispensable permissive agent for myeloproliferation of MPN-associated myelofibrosis. The lack of correlation between eNAMPT and hs-CRP revealed that eNAMPT in MPN-associated myelofibrosis does not behave as a canonical inflammatory cytokine. In addition, higher levels of eNAMPT predicted longer time to blast transformation, and protected against progression toward thrombocytopenia and large splenomegaly. In conclusion, in MPN-associated myelofibrosis high levels of eNAMPT mark the myeloproliferative potential and, at variance with a high number of cancers, are protective against disease progression.Am. J.

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Associations and prognostic interactions between circulating levels of hepcidin, ferritin and inflammatory cytokines in primary myelofibrosis

Cited by 68 publications

References 22 publications

JAK2 exon 12 mutant mice display isolated erythrocytosis and changes in iron metabolism favoring increased erythropoiesis

JAK2 exon 12 mutant mice display isolated erythrocytosis and changes in iron metabolism favoring increased erythropoiesis

Diagnosis of iron-deficient states

Increased plasma nicotinamide phosphoribosyltransferase is associated with a hyperproliferative phenotype and restrains disease progression in MPN‐associated myelofibrosis

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