Your search keyword '"Irene Graziani"' showing total 10 results

1. Thrombin induces rapid PAR1-mediated non-classical FGF1 release

Author

Vihren Kolev, Igor Prudovsky, Robert Friesel, Maria F. Duarte, Thomas Maciag, Silvia Marta Oliveira, Irene Graziani, Doreen Kacer, Alexander Kirov, and Raffaella Soldi

Subjects

Biophysics, Biology, Thrombomodulin, Fibroblast growth factor, Biochemistry, Article, Mice, Thrombin, medicine, Animals, Receptor, PAR-1, Receptor, Molecular Biology, Oligopeptide, Dose-Response Relationship, Drug, Cell growth, Cell Biology, FGF1, Cell biology, NIH 3T3 Cells, cardiovascular system, Fibroblast Growth Factor 1, Signal transduction, Signal Transduction, circulatory and respiratory physiology, medicine.drug

Abstract

Thrombin induces cell proliferation and migration during vascular injury. We report that thrombin rapidly stimulated expression and release of the pro-angiogenic polypeptide fibroblast growth factor 1 (FGF1). Thrombin failed to induce FGF1 release from protease-activated receptor 1 (PAR1) null fibroblasts, indicating that this effect was dependent on PAR1. Similarly to thrombin, FGF1 expression and release were induced by TRAP, a specific oligopeptide agonist of PAR1. These results identify a novel aspect of the crosstalk between FGF and thrombin signaling pathways which both play important roles in tissue repair and angiogenesis.

Published

2006

2. The intracellular domain of Notch ligand Delta1 induces cell growth arrest

Author

Thomas Maciag, Vihren Kolev, Olga Sideleva, Igor Prudovsky, Irene Graziani, Barry W. Larman, Doreen Kacer, Radianna Trifonova, Maria F. Duarte, Raffaella Soldi, and Deena Small

Subjects

Notch, Biophysics, Notch signaling pathway, Senescence, Ligands, Cleavage (embryo), Biochemistry, Mice, Structural Biology, Cyclin-dependent kinase, Genetics, Animals, Humans, Molecular Biology, Cellular Senescence, Cell Proliferation, p21, DNA synthesis, biology, Cell growth, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Cell Biology, Transmembrane protein, Protein Structure, Tertiary, Cell biology, Notch proteins, NIH 3T3 Cells, biology.protein, Notch binding, Delta intracellular domain, Intracellular

Abstract

Notch signaling involves proteolytic cleavage of the transmembrane Notch receptor after binding to its transmembrane ligands, Delta or Jagged; and the resultant soluble intracellular domain of Notch stimulates a cascade of transcriptional events. The Delta1 ligand also undergoes proteolytic cleavage upon Notch binding, resulting in the production of a free intracellular domain. We demonstrate that the expression of the intracellular domain of Delta1 results in a non-proliferating senescent-like cell phenotype which is dependent on the expression of the cell cycle inhibitor, p21, and is abolished by co-expression of constitutively active Notch1. These data suggest a new intracellular role for Delta1.

Published

2005

3. The non-classical export routes: FGF1 and IL-1α point the way

Author

Igor Prudovsky, Francesca Tarantini, Cinzia Bagalà, Thomas Maciag, Irene Graziani, Anna Mandinova, Raffaella Soldi, Stephen Bellum, Maria F. Duarte, Matteo Landriscina, and Holly Doherty

Subjects

Signal peptide, Neovascularization, Pathologic, Membrane Fluidity, Copper metabolism, Cell Membrane, S100 Proteins, Chromosomal translocation, Cell Biology, Protein Sorting Signals, FGF1, Biology, Endoplasmic Reticulum, Cell Hypoxia, Molten globule, Tumor formation, Transport protein, Models, Structural, Protein Transport, Biochemistry, Animals, Fibroblast Growth Factor 1, Humans, Copper, Interleukin-1

Abstract

Non-classical protein release independent of the ER-Golgi pathway has been reported for an increasing number of proteins lacking an N-terminal signal sequence. The export of FGF1 and IL-1α, two pro-angiogenic polypeptides, provides two such examples. In both cases, export is based on the Cu2+-dependent formation of multiprotein complexes containing the S100A13 protein and might involve translocation of the protein across the membrane as a `molten globule'. FGF1 and IL-1α are involved in pathological processes such as restenosis and tumor formation. Inhibition of their export by Cu2+ chelators is thus an effective strategy for treatment of several diseases.

Published

2003

4. Protein folding does not prevent the nonclassical export of FGF1 and S100A13

Author

Sarah M. Sterling, Irene Graziani, Igor Prudovsky, Thallapuranam Krishnaswamy Suresh Kumar, David J. Neivandt, Matteo Landriscina, Francesca Tarantini, Andrew W. Doyle, and Alek Kirov

Subjects

Signal peptide, Protein Folding, Biophysics, Protein Sorting Signals, Aminopterin, Endoplasmic Reticulum, Transfection, Biochemistry, Article, Mice, Protein structure, Dihydrofolate reductase, medicine, Animals, Molecular Biology, biology, Endoplasmic reticulum, S100 Proteins, Cell Biology, Transport protein, Protein Structure, Tertiary, Protein Transport, Secretory protein, biology.protein, NIH 3T3 Cells, Fibroblast Growth Factor 1, Protein folding, medicine.drug

Abstract

Newly synthesized proteins are usually exported through the endoplasmic reticulum (ER) and Golgi due to the presence in their primary sequence of a hydrophobic signal peptide that is recognized by the ER translocation system. However, some secreted proteins lack a signal peptide and are exported independently of ER-Golgi. Fibroblast growth factor (FGF)1 is included in this group of polypeptides, as well as S100A13 that is a small calcium-binding protein critical for FGF1 export. Classically secreted proteins are transported into ER in their unfolded states. To determine the role of protein tertiary structure in FGF1 export through the cell membrane, we produced the chimeras of FGF1 and S100A13 with dihydrofolate reductase (DHFR). The specific DHFR inhibitor, aminopterin, prevents its unfolding. We found that aminopterin did not inhibit the release of FGF1:DHFR and S100A13:DHFR. Thus, FGF1 and S100A13 can be exported in folded conformation.

Published

2009

5. Opposite effects of Notch-1 and Notch-2 on mesothelioma cell survival under hypoxia are exerted through the Akt pathway

Author

Peter Strack, Yuanbin Chen, Lucio Miele, Harvey I. Pass, Melissa A. De Marco, Maurizio Bocchetta, Irene Graziani, Richard D. May, and Sandra Eliasz

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Mesothelioma, Cancer Research, Cell Survival, Notch signaling pathway, Cell Growth Processes, Tumor Cells, Cultured, PTEN, Tensin, Humans, RNA, Messenger, Receptor, Notch2, Phosphorylation, Receptor, Notch1, Notch 2, Protein kinase B, Notch 1, PI3K/AKT/mTOR pathway, biology, PTEN Phosphohydrolase, DNA, Neoplasm, Cell Hypoxia, Cell biology, Oncology, Cancer cell, biology.protein, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

Malignant mesothelioma (MM) is a cancer of the lining of the lungs, heart, and intestine and is known to respond poorly to chemotherapy. Here we show that malignant mesothelial cells have an elevated Notch signaling pathway compared with normal human mesothelial cells. We studied the role of Notch in MM under normoxic and hypoxic conditions, the latter condition best recapitulating the MM microenvironment. Genetic and chemical modulation of the Notch pathway indicated that MM cells are dependent on Notch signaling. More specifically, this signaling was Notch-1 dependent as the result of its negative transcriptional regulation on phosphatase and tensin homologue (PTEN), which led to activation of the prosurvival phosphatidylinositol 3-kinase (PI3K)/Akt/mammalian target of rapamycin (mTOR) signaling pathway. Our study also provides evidence that whereas Notch-1 is elevated in the malignant setting, Notch-2 is diminished. This differential expression of the two Notch isoforms benefits cancer cell survival because reexpression of Notch-2 was toxic to MM cells. The mechanism of Notch-2 toxicity to MM cells countered that of Notch-1, as it was the result of positive transcriptional regulation of PTEN and inhibition of the PI3K/Akt/mTOR signaling pathway. These results provide new insight into the role of Notch in MM and suggest that Notch pathway inhibitors may be useful in the treatment of this deadly disease. [Cancer Res 2008;68(23):9678–85]

Published

2008

6. Novel cross-talk between three cardiovascular regulators: thrombin cleavage fragment of Jagged1 induces fibroblast growth factor 1 expression and release

Author

Deena Small, Robert Friesel, Joseph M. Verdi, Aleksandr Kirov, Raffaella Soldi, Igor Prudovsky, Doreen Kacer, Carla Mouta-Bellum, Maria F. Duarte, Lucy Liaw, Irene Graziani, Vihren Kolev, and Thomas Maciag

Subjects

Transcription, Genetic, Notch signaling pathway, Biology, Fibroblast growth factor, Cell Line, Mice, Thrombin, Thrombin receptor, medicine, Animals, Humans, Receptor, PAR-1, Serrate-Jagged Proteins, Molecular Biology, Receptors, Notch, Multipotent Stem Cells, Calcium-Binding Proteins, Endothelial Cells, Membrane Proteins, Cardiovascular Agents, Cell Biology, Articles, Receptors, Fibroblast Growth Factor, Peptide Fragments, Cell biology, Hairless, Protein Structure, Tertiary, Molecular Weight, Protein Transport, Neural Crest, Cardiovascular agent, Jagged-1 Protein, Fibroblast Growth Factor 1, Intercellular Signaling Peptides and Proteins, Receptors, Thrombin, Signal transduction, medicine.drug, Signal Transduction

Abstract

Angiogenesis is controlled by several regulatory mechanisms, including the Notch and fibroblast growth factor (FGF) signaling pathways. FGF1, a prototype member of FGF family, lacks a signal peptide and is released through an endoplasmic reticulum–Golgi-independent mechanism. A soluble extracellular domain of the Notch ligand Jagged1 (sJ1) inhibits Notch signaling and induces FGF1 release. Thrombin, a key protease of the blood coagulation cascade and a potent inducer of angiogenesis, stimulates rapid FGF1 release through a mechanism dependent on the major thrombin receptor protease-activated receptor (PAR) 1. This study demonstrates that thrombin cleaves Jagged1 in its extracellular domain. The sJ1 form produced as a result of thrombin cleavage inhibits Notch-mediated CBF1/Suppressor of Hairless [(Su(H)]/Lag-1–dependent transcription and induces FGF1 expression and release. The overexpression of Jagged1 in PAR1 null cells results in a rapid thrombin-induced export of FGF1. These data demonstrate the existence of novel cross-talk between thrombin, FGF, and Notch signaling pathways, which play important roles in vascular formation and remodeling.

Published

2008

7. Sphingosine kinase 1 is a critical component of the copper-dependent FGF1 export pathway

Author

Timoty Hla, Anna Mandinova, Aleksandr Kirov, Thomas Maciag, Maria F. Duarte, Irene Graziani, Stuart M. Pitson, Igor Prudovsky, Raffaella Soldi, Krishnan Venkataraman, Mathew A. Vadas, Doreen Kacer, Vihren Kolev, and Universidade do Minho

Subjects

Medicina Básica [Ciências Médicas], Mitogen-activated protein kinase kinase, Article, MAP2K7, 03 medical and health sciences, Mice, 0302 clinical medicine, Non-classical release, Animals, ASK1, Sphingosine kinase 1, Cloning, Molecular, Cells, Cultured, 030304 developmental biology, Chelating Agents, Mice, Knockout, Molybdenum, 0303 health sciences, Science & Technology, MAP kinase kinase kinase, biology, Cyclin-dependent kinase 2, Temperature, Fibroblast growth factor 1, Cell Biology, Lipid signaling, Fibroblasts, 3. Good health, Cell biology, Phosphotransferases (Alcohol Group Acceptor), Protein Transport, Biochemistry, 030220 oncology & carcinogenesis, Sphingosine kinase 1 Fibroblast growth factor 1 Non-classical release Angiogenesis, Ciências Médicas::Medicina Básica, biology.protein, NIH 3T3 Cells, Cyclin-dependent kinase 9, Angiogenesis, Copper

Abstract

Sphingosine kinase 1 catalyzes the formation of sphingosine-1-phosphate, a lipid mediator involved in the regulation of angiogenesis. Sphingosine kinase 1 is constitutively released from cells, even though it lacks a classical signal peptide sequence. Because copper-dependent non-classical stress-induced release of FGF1 also regulates angiogenesis, we questioned whether sphingosine kinase 1 is involved in the FGF1 release pathway. We report that (i) the coexpression of sphingosine kinase 1 with FGF1 inhibited the release of sphingosine kinase 1 at 37 degrees C; (ii) sphingosine kinase 1 was released at 42 degrees C in complex with FGF1; (iii) sphingosine kinase 1 null cells failed to release FGF1 at stress; (iv) sphingosine kinase 1 is a high affinity copper-binding protein which formed a complex with FGF1 in a cell-free system, and (v) sphingosine kinase 1 over expression rescued the release of FGF1 from inhibition by the copper chelator, tetrathiomolybdate. We propose that sphingosine kinase 1 is a component of the copper-dependent FGF1 release pathway., NIH grants HL67330 and HL60694 to TH and HL32348, HL 35627 and RR15555 (Project 4) to IP

Published

2007

8. Release of FGF1 and p40 synaptotagmin 1 correlates with their membrane destabilizing ability

Author

Francesca Tarantini, Andrew W. Doyle, Raffaella Soldi, Maria F. Duarte, Chin Yu, Vihren Kolev, Igor Prudovsky, David J. Neivandt, Cinzia Bagalà, Thomas Maciag, Thallapuranam Krishnaswamy Suresh Kumar, and Irene Graziani

Subjects

Lipid Bilayers, Biophysics, Phospholipid, Golgi Apparatus, SYT1, Biochemistry, Models, Biological, Synaptotagmin 1, Article, chemistry.chemical_compound, Mice, Calcium-binding protein, Animals, Lipid bilayer, Molecular Biology, Liposome, Chemistry, Cell Membrane, Cell Biology, FGF1, Recombinant Proteins, Cell biology, Membrane, Synaptotagmin I, Liposomes, NIH 3T3 Cells, Fibroblast Growth Factor 1

Abstract

Fibroblast growth factor (FGF)1 is released from cells as a constituent of a complex that contains the small calcium binding protein S100A13, and the p40 kDa form of synaptotagmin (Syt)1, through an ER-Golgi-independent stress-induced pathway. FGF1 and the other components of its secretory complex are signal peptide-less proteins. We examined their capability to interact with lipid bilayers by studying protein-induced carboxyfluorescein release from liposomes of different phospholipid (pL) compositions. FGF1, p40 Syt1, and S100A13 induced destabilization of liposomes composed of acidic but not of zwitterionic pL. We produced mutants of FGF1 and p40 Syt1, in which specific basic amino acid residues in the regions that bind acidic pL were substituted. The ability of these mutants to induce liposomes destabilization was strongly attenuated, and they exhibited drastically diminished spontaneous and stress-induced release. Apparently, the non-classical release of FGF1 and p40 Syt1 involves destabilization of membranes containing acidic pL.

Published

2006

9. The alternative translation of synaptotagmin 1 mediates the non-classical release of FGF1

Author

Anna Mandinova, Raffaella Soldi, C Mouta, Thomas Maciag, Cinzia Bagalà, Irene Graziani, Igor Prudovsky, and Vihren Kolev

Subjects

Gene isoform, DNA, Complementary, Mutant, Molecular Sequence Data, Biophysics, Nerve Tissue Proteins, Biology, Biochemistry, Synaptotagmin 1, Mice, Synaptotagmins, Protein biosynthesis, Animals, Amino Acid Sequence, Molecular Biology, Peptide sequence, Membrane Glycoproteins, Base Sequence, Synaptotagmin I, Calcium-Binding Proteins, Translation (biology), Cell Biology, Molecular biology, Transmembrane protein, Cell biology, Protein Biosynthesis, Mutagenesis, Site-Directed, NIH 3T3 Cells, Fibroblast Growth Factor 1

Abstract

Although the extravesicular p40 domain of the transmembrane protein, p65 synaptotagmin (Syt) 1, is essential for the non-classical export of the signal peptide-less structure, FGF1, it was not possible to identify a specific intracellular protease responsible for the processing of p65 Syt1. Surprisingly, analysis of the p65 Syt1 coding sequence revealed the presence of two potential alternative ATG codons corresponding to Met103 and Met113 both of which were flanked by Kozak sequences. Indeed, in vitro translation of a Met103Ile but not a Met113Ile p65 Syt1 point mutant exhibited reduced expression of p40 Syt1 and the double p65 Syt1 Met103Ile and Met113Ile point mutant was unable to translate the p40 Syt1 isoform. Since the expression of the p65 Syt1 double point mutant inhibited the stress-induced release of FGF1, it is likely that the alternative translation of the p65 Syt1 transcript at Met103 may be involved in the generation of intracellular p40 Syt1, a critical component of the FGF1 release pathway.

Published

2003

10. S100A13 mediates the copper-dependent stress-induced release of IL-1alpha from both human U937 and murine NIH 3T3 cells

Author

Igor Prudovsky, Raffaella Soldi, Thomas Maciag, Cinzia Bagalà, Anna Mandinova, Francesca Tarantini, Stephen Bellum, Matteo Landriscina, and Irene Graziani

Subjects

inorganic chemicals, Transcriptional Activation, Repressor, Antineoplastic Agents, Biology, 3T3 cells, Proinflammatory cytokine, Gene product, Mice, Cytosol, Stress, Physiological, Extracellular, medicine, Animals, Humans, Chelating Agents, U937 cell, Neovascularization, Pathologic, Binding protein, S100 Proteins, Temperature, Extracellular Fluid, Cell Biology, U937 Cells, Cell biology, Repressor Proteins, medicine.anatomical_structure, Biochemistry, Mutation, NIH 3T3 Cells, Fibroblast Growth Factor 1, Intracellular, Copper, Interleukin-1

Abstract

Copper is involved in the promotion of angiogenic and inflammatory events in vivo and, although recent clinical data has demonstrated the potential of Cu2+ chelators for the treatment of cancer in man, the mechanism for this activity remains unknown. We have previously demonstrated that the signal peptide-less angiogenic polypeptide, FGF1, uses intracellular Cu2+ to facilitate the formation of a multiprotein aggregate that enables the release of FGF1 in response to stress and that the expression of the precursor form but not the mature form of IL-1alpha represses the stress-induced export of FGF1 from NIH 3T3 cells. We report here that IL-1alpha is a Cu2+-binding protein and human U937 cells, like NIH 3T3 cells, release IL-1alpha in response to temperature stress in a Cu2+-dependent manner. We also report that the stress-induced export of IL-1alpha involves the intracellular association with the Cu2+-binding protein, S100A13. In addition, the expression of a S100A13 mutant lacking a sequence novel to this gene product functions as a dominant-negative repressor of IL-1alpha release, whereas the expression of wild-type S100A13 functions to eliminate the requirement for stress-induced transcription. Lastly, we present biophysical evidence that IL-1alpha may be endowed with molten globule character, which may facilitate its release through the plasma membrane. Because Cu2+ chelation also represses the release of FGF1, the ability of Cu2+ chelators to potentially serve as effective clinical anti-cancer agents may be related to their ability to limit the export of these proinflammatory and angiogenic signal peptide-less polypeptides into the extracellular compartment.

Published

2003