A. M. Vannucchi scite author profile

A. M. Vannucchi

5Publications

26Citation Statements Received

0Citation Statements Given

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Azienda Ospedaliero-Universitaria Careggi, University of Florence

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Identification and conditions for selective expression of megakaryocytic markers in Friend erythroleukemia cells

Paoletti

Vannucchi

Mocali

et al. 1995

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Friend murine erythroleukemia cells (MELCs) have been reevaluated in terms of their nature and potential pathways of differentiation. MELC induced with 5 mmol/L hexamethylene bisacetamide (HMBA), in addition to expression of known markers of the erythroid phenotype, were also found to exhibit traits of the megakaryocytic lineage. Erythroid differentiation was shown by the typical synthesis and accumulation of hemoglobin (Hb); megakaryoblastoid differentiation of MELCs upon induction was shown by increased specific activity of acetylcholinesterase (AChE). Incubation of MELCs with 5 mmol/L HMBA in RPMI supplemented with 1% fetal calf serum (FCS) (instead of the usual 5%), induced cells to selectively express high levels of AChE (up to approximately 170 mU/mg protein) with little activation of Hb synthesis (less than 5% B+ cells). The increase in AChE levels was a general phenomenon affecting the whole cell population and approached its maximum within 3 days of incubation with the inducer. Subsequently, MELCs become committed to terminal division, undergoing growth arrest and expression of the megakaryocytic phenotype even after the removal of HMBA. There were no appreciable changes of basal AChE levels in MELCs that were either made resistant to HMBA or treated with 0.1 mmol/L hemin that activated differentiated erythroid function without commitment. Phorbol 12-myristate 13-acetate (PMA), known to repress induced Hb synthesis in these cells, did not prevent the full increase in AChE when incubated with MELCs 2 days before HMBA addition. HMBA-induced MELCs always underwent AChE increase that was more or less pronounced depending on the low or high serum content in culture, respectively. Conversely, Hb expression was permitted only when MELCs were transferred in the late phase or at the end of commitment from low to high serum media. Variations of FCS content in culture media proved to be a simple and reliable approach to change the MELC response to inducers and to modulate expression of either megakaryocytic or mixed erythromegakaryocytic phenotype. These findings suggested that MELC might be considered, at least, as a bipotential model of differentiation to be used for studies on regulation of either megakaryocytic or erythroid markers and on competition between the two hematopoietic lineages. In this regard, it was intriguing that AChE levels attained under selective induction (low serum) were always higher than under conditions allowing coexpression of both AChE and Hb (high serum). Moreover, MELCs were also found to bind the specific rat-antimouse platelet monoclonal antibody 4A5.(ABSTRACT TRUNCATED AT 400 WORDS)

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Effects of cyclosporin A on erythropoietin production by the human Hep3B hepatoma cell line

Vannucchi

Grossi

Bosi

et al. 1993

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There is evidence that the inadequate erythropoietin (Epo) production observed in patients undergoing allogeneic bone marrow transplantation (BMT) might be ascribed to an inhibitory effect caused by the immunosuppressive drug cyclosporin A (CsA). In this in vitro study, we have evaluated the effects of CsA on the release of Epo in the culture medium by the human Hep3B hepatoma cell line. In cultures incubated with both CsA and the nonimmunosuppressive CsA analog MeAla-6, but not with the CsA-unrelated immunosuppressive agent FK-506, the levels of Epo in the medium were significantly reduced in comparison with controls, at concentrations (0.01 to 1.6 mumol/L) not affecting total protein synthetic rate nor the constitutive secretion of alpha- fetoprotein. Hep3B cells were found to contain a CsA-binding molecule, with an M(r) of 18 Kd, as assessed by high performance liquid chromatography (HPLC) and ligand-blotting analysis. CsA did not affect the expression of the Epo gene, as judged by Northern blot analysis, but caused a significant amount of Epo to remain unsecreted within the cells; almost all (97% of total) of the intracellular Epo was associated with the plasma membrane subcellular fraction. We conclude that: (1) CsA is able to inhibit Epo release in vitro by Hep3B cells, further supporting the hypothesis that the drug might have a role in the inappropriately low Epo levels observed in BMT patients; (2) the inhibitory effect appears to be specific and not caused by a general impairment of protein synthesis and/or secretion; and (3) the reduced Epo levels found in the medium of CsA-treated Hep3B cultures are supposed to be the consequence of an inability of the cells to correctly process Epo molecules for the secretory pathway.

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P1037: Does Early Intervention in Myelofibrosis Impact Outcomes? A Pooled Analysis of the Comfort I and Ii Studies

Harrison

Kiladjian

Vannucchi

et al. 2022

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P1051: A Phase 2 Study of Img-7289 (Bomedemstat) in Patients With Advanced Myelofibrosis

Gill

Yacoub

Pettit

et al. 2022

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S195: Momentum: Phase 3 Randomized Study of Momelotinib (Mmb) Versus Danazol (Dan) in Symptomatic and Anemic Myelofibrosis (Mf) Patients Previously Treated With a Jak Inhibitor

Verstovsek

Vannucchi

Gerds

et al. 2022

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A. M. Vannucchi

Identification and conditions for selective expression of megakaryocytic markers in Friend erythroleukemia cells

Effects of cyclosporin A on erythropoietin production by the human Hep3B hepatoma cell line

P1037: Does Early Intervention in Myelofibrosis Impact Outcomes? A Pooled Analysis of the Comfort I and Ii Studies

P1051: A Phase 2 Study of Img-7289 (Bomedemstat) in Patients With Advanced Myelofibrosis

S195: Momentum: Phase 3 Randomized Study of Momelotinib (Mmb) Versus Danazol (Dan) in Symptomatic and Anemic Myelofibrosis (Mf) Patients Previously Treated With a Jak Inhibitor

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