4 results on '"Borgatti, Monica"'
Search Results
2. Trimethylangelicin reduces IL-8 transcription and potentiates CFTR function.
- Author
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Tamanini, Anna, Borgatti, Monica, Finotti, Alessia, Piccagli, Laura, Bezzerri, Valentino, Favia, Maria, Guerra, Lorenzo, Lampronti, Ilaria, Bianchi, Nicoletta, Dall'Acqua, Francesco, Vedaldi, Daniela, Salvador, Alessia, Fabbri, Enrica, Mancini, Irene, Nicolis, Elena, Casavola, Valeria, Cabrini, Giulio, and Gambari, Roberto
- Subjects
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CYSTIC fibrosis , *INTERLEUKIN-8 , *INFLAMMATION , *TRANSCRIPTION factors , *NEUTROPHILS , *EPITHELIAL cells , *CHEMOKINES - Abstract
Chronic inflammatory response in the airway tract of patients affected by cystic fibrosis is characterized by an excessive recruitment of neutrophils to the bronchial lumina, driven by the chemokine interleukin (IL)-8. We previously found that 5-methoxypsoralen reduces Pseudomonas aeruginosa-dependent IL-8 transcription in bronchial epithelial cell lines, with an IC50 of 10 μM (Nicolis E, Lampronti I, Dechecchi MC, Borgatti M, Tamanini A, Bezzerri V, Bianchi N, Mazzon M, Mancini I, Giri MG, Rizzotti P, Gambari R, Cabrini G. Int Immunopharmacol 9: 1411-1422, 2009). Here, we extended the investigation to analogs of 5-methoxypsoralen, and we found that the most potent effect is obtained with 4,6,4′-trimethylangelicin (TMA), which inhibits P. aeruginosa-dependent IL-8 transcription at nanomolar concentration in IB3-1, CuFi-1, CFBE41o-, and Calu-3 bronchial epithelial cell lines. Analysis of phosphoproteins involved in proinflammatory transmembrane signaling evidenced that TMA reduces the phosphorylation of ribosomal S6 kinase-1 and AKT2/3, which we found indeed involved in P. aeruginosa-dependent activation of IL-8 gene transcription by testing the effect of pharmacological inhibitors. In addition, we found a docking site of TMA into NF-κB by in silico analysis, whereas inhibition of the NF-κB/DNA interactions in vitro by EMSA was observed at high concentrations (10 mM TMA). To further understand whether NF-κB pathway should be considered a target of TMA, chromatin immunoprecipitation was performed, and we observed that TMA (100 nM) preincubated in whole living cells reduced the interaction of NF-κB with the promoter of IL-8 gene. These results suggest that TMA could inhibit IL-8 gene transcription mainly by intervening on driving the recruitment of activated transcription factors on IL-8 gene promoter, as demonstrated here for NF-κB. Although the complete understanding of the mechanism of action of TMA deserves further investigation, an activity of TMA on phosphorylating pathways was already demonstrated by our study. Finally, since psoralens have been shown to potentiate cystic fibrosis transmembrane conductance regulator (CFTR)-mediated chloride transport, TMA was tested and found to potentiate CFTR-dependent chloride efflux. In conclusion, TMA is a dual-acting compound reducing excessive IL-8 expression and potentiating CFTR function. [ABSTRACT FROM AUTHOR]
- Published
- 2011
- Full Text
- View/download PDF
3. Increase in gamma-globin mRNA content in human erythroid cells treated with angelicin analogs.
- Author
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Lampronti, Ilaria, Bianchi, Nicoletta, Zuccato, Cristina, Dall’Acqua, Francesco, Vedaldi, Daniela, Viola, Giampietro, Potenza, Rocco, Chiavilli, Francesco, Breveglieri, Giulia, Borgatti, Monica, Finotti, Alessia, Feriotto, Giordana, Salvatori, Francesca, Gambari, Roberto, and Dall'acqua, Francesco
- Abstract
The aim of the present study was to identify molecular analogs of angelicin (ANG) able to increase erythroid differentiation of K562 cells and expression of gamma-globin genes in human erythroid precursor cells, with low effects on apoptosis. ANG-like molecules are well-known photosensitizers largely used for their antiproliferative activity in the treatment of different skin diseases (i.e., psoriasis, vitiligo, eczema, and mycosis fungoides). To verify the activity of these derivatives, we employed three experimental cell systems: (1) the human leukemic K562 cell line, (2) K562 cell clones stably transfected with a pCCL construct carrying green-EGFP under the gamma-globin gene promoter, and (3) the two-phase liquid culture of human erythroid progenitors isolated from normal donors and beta-thalassemia patients. The results of our study suggest that trimethyl ANG is a powerful inducer of erythroid differentiation, compared with known inducers, such as ANG, cytosine arabinoside, mithramycin, and cisplatin. These data could have practical relevance, because pharmacologically mediated regulation of human gamma-globin gene expression, with the consequent induction of fetal hemoglobin, is considered a potential therapeutic approach in hematological disorders including beta-thalassemia and sickle cell anemia. [ABSTRACT FROM AUTHOR]
- Published
- 2009
- Full Text
- View/download PDF
4. Accumulation of γ-globin mRNA in human erythroid cells treated with angelicin.
- Author
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Lampronti, Ilaria, Bianchi, Nicoletta, Borgatti, Monica, Fibach, Eitan, Prus, Eupenia, and Gambari, Roberto
- Subjects
PSORALENS ,LEUKEMIA ,MESSENGER RNA - Abstract
Abstract: The aim of the present study was to determine whether angelicin is able to increase the expression of γ -globin genes in human erythroid cells. Angelicin is structurally related to psoralens, a well-known chemical class of photosensitizers used for their antiproliferative activity in treatment of different skin diseases (i.e., psoriasis and vitiligo). To verify the activity of angelicin, we employed two experimental cell systems, the human leukemic K562 cell line and the two-phase liquid culture of human erythroid progenitors isolated from normal donors. The results of our investigation suggest that angelicin, compared with cytosine arabinoside, mithramycin and cisplatin, is a powerful inducer of erythroid differentiation and γ -globin mRNA accumulation of human leukemia K562 cells. In addition, when normal human erythroid precursors were cultured in the presence of angelicin, increases of γ -globin mRNA accumulation and fetal hemoglobin (HbF) production, even higher than those obtained using hydroxyurea, were detected. These results could have practical relevance, as pharmacologically-mediated regulation of the expression of human γ -globin genes, leading to HbF induction, is considered a potential therapeutic approach in hematological disorders, including β -thalassemia and sickle cell anemia. [ABSTRACT FROM AUTHOR]
- Published
- 2003
- Full Text
- View/download PDF
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