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9 results on '"Marco De Santis Puzzonia"'

1. TGFbeta Induces Binucleation/Polyploidization in Hepatocytes through a Src-Dependent Cytokinesis Failure.

Author

Marco De Santis Puzzonia, Angela Maria Cozzolino, Germana Grassi, Francesca Bisceglia, Raffaele Strippoli, Giulia Guarguaglini, Franca Citarella, Benedetto Sacchetti, Marco Tripodi, Alessandra Marchetti, and Laura Amicone

Subjects
Medicine, Science
Abstract

In all mammals, the adult liver shows binucleated as well as mononucleated polyploid hepatocytes. The hepatic polyploidization starts after birth with an extensive hepatocyte binucleation and generates hepatocytes of several ploidy classes. While the functional significance of hepatocyte polyploidy is becoming clearer, how it is triggered and maintained needs to be clarified. Aim of this study was to identify a major inducer of hepatocyte binucleation/polyploidization and the cellular and molecular mechanisms involved. We found that, among several cytokines analyzed, known to be involved in early liver development and/or mass control, TGFbeta1 was capable to induce, together with the expected morphological changes, binucleation in hepatocytes in culture. Most importantly, the pharmacological inhibition of TGFbeta signaling in healthy mice during weaning, when the physiological binucleation occurs, induced a significant decrease of hepatocyte binucleation rate, without affecting cell proliferation and hepatic index. The TGFbeta-induced hepatocyte binucleation resulted from a cytokinesis failure, as assessed by video microscopy, and is associated with a delocalization of the cytokinesis regulator RhoA-GTPase from the mid-body of dividing cells. The use of specific chemical inhibitors demonstrated that the observed events are Src-dependent. Finally, the restoration of a fully epithelial phenotype by TGFbeta withdrawal gave rise to a cell progeny capable to maintain the polyploid state. In conclusion, we identified TGFbeta as a major inducer of hepatocyte binucleation both in vitro and in vivo, thus ascribing a novel role to this pleiotropic cytokine. The production of binucleated/tetraploid hepatocytes is due to a cytokinesis failure controlled by the molecular axis TGFbeta/Src/RhoA.

Published
2016
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2. Human haemato-endothelial precursors: cord blood CD34+ cells produce haemogenic endothelium.

Author

Elvira Pelosi, Germana Castelli, Ines Martin-Padura, Veronica Bordoni, Simona Santoro, Alice Conigliaro, Anna Maria Cerio, Marco De Santis Puzzonia, Paola Marighetti, Mauro Biffoni, Tonino Alonzi, Laura Amicone, Myriam Alcalay, Francesco Bertolini, Ugo Testa, and Marco Tripodi

Subjects
Medicine, Science
Abstract

Embryologic and genetic evidence suggest a common origin of haematopoietic and endothelial lineages. In the murine embryo, recent studies indicate the presence of haemogenic endothelium and of a common haemato-endothelial precursor, the haemangioblast. Conversely, so far, little evidence supports the presence of haemogenic endothelium and haemangioblasts in later stages of development. Our studies indicate that human cord blood haematopoietic progenitors (CD34+45+144-), triggered by murine hepatocyte conditioned medium, differentiate into adherent proliferating endothelial precursors (CD144+CD105+CD146+CD31+CD45-) capable of functioning as haemogenic endothelium. These cells, proven to give rise to functional vasculature in vivo, if further instructed by haematopoietic growth factors, first switch to transitional CD144+45+ cells and then to haematopoietic cells. These results highlight the plasticity of haemato-endhothelial precursors in human post-natal life. Furthermore, these studies may provide highly enriched populations of human post-fetal haemogenic endothelium, paving the way for innovative projects at a basic and possibly clinical level.

Published
2012
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4. Epigenetic control of EMT/MET dynamics: HNF4α impacts DNMT3s through miRs-29

Author

Laura Amicone, Marco De Santis Puzzonia, Angela Maria Cozzolino, Valeria de Nonno, Marco Tripodi, Silvia Anna Ciafrè, Chad Brocker, Cecilia Battistelli, Carla Cicchini, and Frank J. Gonzalez

Subjects
miR-29, Epithelial-Mesenchymal Transition, Epigenetic code, DNMT3B, Biophysics, De novo DNA methylation, Biology, Biochemistry, DNA methyltransferase, Article, Gene Expression Regulation, Enzymologic, DNA Methyltransferase 3A, Epigenesis, Genetic, TGFβ, Mice, Structural Biology, microRNA, Genetics, Animals, Hepatocyte, DNA (Cytosine-5-)-Methyltransferases, Epigenetics, Molecular Biology, Epithelial–mesenchymal transition, Cells, Cultured, Mice, Knockout, Settore BIO/13, Epithelial-mesenchymal transition, MiR-29, Cell Differentiation, Cellular Reprogramming, Cell biology, Gene Expression Regulation, Neoplastic, MicroRNAs, Cell Transformation, Neoplastic, Hepatocyte Nuclear Factor 4, embryonic structures, DNA methylation, Hepatocytes, DNMT1, Reprogramming
Abstract

Background and aims Epithelial-to-mesenchymal transition (EMT) and the reverse mesenchymal-to-epithelial transition (MET) are manifestations of cellular plasticity that imply a dynamic and profound gene expression reprogramming. While a major epigenetic code controlling the coordinated regulation of a whole transcriptional profile is guaranteed by DNA methylation, DNA methyltransferase (DNMT) activities in EMT/MET dynamics are still largely unexplored. Here, we investigated the molecular mechanisms directly linking HNF4α, the master effector of MET, to the regulation of both de novo of DNMT 3A and 3B. Methods Correlation among EMT/MET markers, microRNA29 and DNMT3s expression was evaluated by RT-qPCR, Western blotting and immunocytochemical analysis. Functional roles of microRNAs and DNMT3s were tested by anti-miRs, microRNA precursors and chemical inhibitors. ChIP was utilized for investigating HNF4α DNA binding activity. Results HNF4α silencing was sufficient to induce positive modulation of DNMT3B, in in vitro differentiated hepatocytes as well as in vivo hepatocyte-specific Hnf4α knockout mice, and DNMT3A, in vitro, but not DNMT1. In exploring the molecular mechanisms underlying these observations, evidence have been gathered for (i) the inverse correlation between DNMT3 levels and the expression of their regulators miR-29a and miR-29b and (ii) the role of HNF4α as a direct regulator of miR-29a-b transcription. Notably, during TGFβ-induced EMT, DNMT3s' pivotal function has been proved, thus suggesting the need for the repression of these DNMTs in the maintenance of a differentiated phenotype. Conclusions HNF4α maintains hepatocyte identity by regulating miR-29a and -29b expression, which in turn control epigenetic modifications by limiting DNMT3A and DNMT3B levels.

Published
2015

5. Tetraploid cells produced by absence of substrate adhesion during cytokinesis are limited in their proliferation and enter senescence after DNA replication

Author

Marco De Santis Puzzonia, Laetitia Gonzalez, Enrico Cundari, Sonia Ascenzi, and F. Degrassi

Subjects
0301 basic medicine, p53, DNA Replication, senescence, Binucleated cells, Mitosis, Ataxia Telangiectasia Mutated Proteins, Biology, Cell Line, 03 medical and health sciences, Report, Chromosomal Instability, Humans, Cleavage furrow, Neoplastic transformation, Molecular Biology, Cellular Senescence, Cell Proliferation, Cytokinesis, cytokinesis failure, Cell growth, Nocodazole, food and beverages, Cell Biology, Cell cycle, Fibroblasts, Cell biology, loss of adherence, tetraploidy, Developmental Biology, G2 Phase Cell Cycle Checkpoints, Tetraploidy, 030104 developmental biology, Gene Expression Regulation, Checkpoint Kinase 1, Camptothecin, Tumor Suppressor Protein p53, Cell aging, Protein Kinases, Signal Transduction
Abstract

Tetraploidy has been proposed as an intermediate state in neoplastic transformation due to the intrinsic chromosome instability of tetraploid cells. Despite the identification of p53 as a major factor in growth arrest of tetraploid cells, it is still unclear whether the p53-dependent mechanism for proliferation restriction is intrinsic to the tetraploid status or dependent on the origin of tetraploidy. Substrate adherence is fundamental for cytokinesis completion in adherent untransformed cells. Here we show that untransformed fibroblast cells undergoing mitosis in suspension produce binucleated tetraploid cells due to defective cleavage furrow constriction that leads to incomplete cell abscission. Binucleated cells obtained after loss of substrate adhesion maintain an inactive p53 status and are able to progress into G1 and S phase. However, binucleated cells arrest in G2, accumulate p53 and are not able to enter mitosis as no tetraploid metaphases were recorded after one cell cycle time. In contrast, tetraploid metaphases were found following pharmacological inhibition of Chk1 kinase, suggesting the involvement of the ATR/Chk1 pathway in the G2 arrest of binucleated cells. Interestingly, after persistence in the G2 phase of the cell cycle, a large fraction of binucleated cells become senescent. These findings identify a new pathway of proliferation restriction for tetraploid untransformed cells that seems to be specific for loss of adhesion-dependent cytokinesis failure. This involves Chk1 and p53 activation during G2. Inhibition of growth and entrance into senescence after cytokinesis in suspension may represent an important mechanism to control tumor growth. In fact, anchorage independent growth is a hallmark of cancer and it has been demonstrated that binucleated transformed cells can enter a cycle of anchorage independent growth.

Published
2015

6. Amorphous silica nanoparticles alter microtubule dynamics and cell migration

Author

Laetitia Gonzalez, Enrico Cundari, Francesco Cubadda, Raffaele Ricci, Giulia Guarguaglini, Marco De Santis Puzzonia, Luc Leyns, Micheline Kirsch-Volders, Federica Aureli, Gonzalez, L, De Santis Puzzonia, M, Ricci, R, Aureli, F, Guarguaglini, G, Cubadda, F, Leyns, L, Cundari, E, Kirsch-Volders, M, and Cell Genetics

Subjects
Surface Properties, Biomedical Engineering, Cell Culture Techniques, Motility, Mitosis, Microtubule, Spindle Apparatus, Biology, silica nanoparticles, Toxicology, Microtubules, Nanoparticle, mode of action, Cell Movement, Cell Line, Tumor, Humans, Cell migration, Particle Size, A549 cell, Microscopy, Video, Spindle Apparatu, Microtubule-Associated Protein, in vitro, Acetylation, respiratory system, microtubule dynamics, Mitosi, Silicon Dioxide, Cell biology, Spindle apparatus, Microscopy, Fluorescence, silica nanoparticle, Nanoparticles, Interphase, Multipolar spindles, Microtubule-Associated Proteins, Cell Culture Technique, microtubule dynamic, Human
Abstract

Amorphous silica nanoparticles (SiO2-NPs) have been studied for their toxic and genotoxic potential. Although contradictory data have been reported and the possible modes of action are not fully elucidated, aneugenic events have been reported, indicating the microtubule (MT) network as a potential target. To investigate this, we examined the effects of 59 nm (10 µg/ml) and 174 nm (7.5 µg/ml) SiO2-NPs on MTs in mitotic and interphase A549 human lung carcinoma cells. No gross morphological changes of the mitotic spindle or induction of multipolar spindles were observed upon SiO2-NPs treatment. The influence of SiO2-NPs on the interphase MTs network dynamics was investigated by in situ depolymerisation/repolymerisation experiments. Results showed a clear increase in MT dynamics after SiO2-NP treatment. Consistent with this, reduced levels of MT acetylation were observed. In addition, live cell microscopy demonstrated that SiO2-NP treatment reduced A549 cell motility. The SiO2-NP doses and conditions (serum-free) used in this study did not induce significant cell toxicity or MN frequencies. Therefore, the effects on MT dynamics, MT acetylation and migration observed, are direct effects of the SiO2-NPs and not a consequence of NP overload or toxic or genotoxic effects.

Published
2015

8. TGFbeta Induces Binucleation/Polyploidization in Hepatocytes through a Src-Dependent Cytokinesis Failure

Author

Giulia Guarguaglini, Franca Citarella, Raffaele Strippoli, Angela Maria Cozzolino, Laura Amicone, Germana Grassi, Marco Tripodi, Marco De Santis Puzzonia, Francesca Bisceglia, Alessandra Marchetti, and Benedetto Sacchetti

Subjects
Genetics and Molecular Biology (all), 0301 basic medicine, RHOA, Physiology, Liver cytology, Immunofluorescence, hepatocyte polyploidization, Cell, lcsh:Medicine, Video microscopy, Medicine (all), Biochemistry, Genetics and Molecular Biology (all), Agricultural and Biological Sciences (all), Biochemistry, Mice, Animal Cells, Ploidy, Transforming Growth Factor beta, Immune Physiology, Medicine and Health Sciences, Cell Cycle and Cell Division, lcsh:Science, Cells, Cultured, Innate Immune System, Microscopy, Multidisciplinary, biology, Chromosome Biology, Light Microscopy, Cell biology, src-Family Kinases, medicine.anatomical_structure, Liver, Cell Processes, TGFbeta, Hepatocyte, Cytokines, Cellular Types, Anatomy, Research Article, Video Microscopy, Immunology, Mitosis, Research and Analysis Methods, Polyploidy, 03 medical and health sciences, Genetics, medicine, Animals, Immunoassays, Cytokinesis, Cell Proliferation, Cell Nucleus, Evolutionary Biology, cytokinesis failure, Population Biology, Cell growth, lcsh:R, Biology and Life Sciences, RhoA, Cell Biology, Molecular Development, Mice, Inbred C57BL, 030104 developmental biology, Immune System, Hepatocytes, Immunologic Techniques, biology.protein, lcsh:Q, Src kinase, Departures from Diploidy, Population Genetics, Developmental Biology
Abstract

In all mammals, the adult liver shows binucleated as well as mononucleated polyploid hepatocytes. The hepatic polyploidization starts after birth with an extensive hepatocyte binucleation and generates hepatocytes of several ploidy classes. While the functional significance of hepatocyte polyploidy is becoming clearer, how it is triggered and maintained needs to be clarified. Aim of this study was to identify a major inducer of hepatocyte binucleation/polyploidization and the cellular and molecular mechanisms involved. We found that, among several cytokines analyzed, known to be involved in early liver development and/or mass control, TGFbeta1 was capable to induce, together with the expected morphological changes, binucleation in hepatocytes in culture. Most importantly, the pharmacological inhibition of TGFbeta signaling in healthy mice during weaning, when the physiological binucleation occurs, induced a significant decrease of hepatocyte binucleation rate, without affecting cell proliferation and hepatic index. The TGFbeta-induced hepatocyte binucleation resulted from a cytokinesis failure, as assessed by video microscopy, and is associated with a delocalization of the cytokinesis regulator RhoA-GTPase from the mid-body of dividing cells. The use of specific chemical inhibitors demonstrated that the observed events are Src-dependent. Finally, the restoration of a fully epithelial phenotype by TGFbeta withdrawal gave rise to a cell progeny capable to maintain the polyploid state. In conclusion, we identified TGFbeta as a major inducer of hepatocyte binucleation both in vitro and in vivo, thus ascribing a novel role to this pleiotropic cytokine. The production of binucleated/tetraploid hepatocytes is due to a cytokinesis failure controlled by the molecular axis TGFbeta/Src/RhoA.

Published
2016

9. Aneuploidy in mitosis of PtK1 cells is generated by random loss and nondisjunction of individual chromosomes

Author

Liliana Torosantucci, Marco De Santis Puzzonia, Francesca Degrassi, Chiara Cenciarelli, and Willem Rens

Subjects
Genetics, Kinetochore, Cells, Aneuploidy, Mitosis, Cell Biology, Biology, medicine.disease, Cell Line, Chromosome segregation, Nondisjunction, Nondisjunction, Genetic, Potoroidae, Chromosome Segregation, medicine, Sister chromatids, Animals, Metaphase, Anaphase
Abstract

Chromosome lagging at anaphase and migration of both sister chromatids to the same pole, i.e. nondisjunction, are two chromosome-segregation errors producing aneuploid cell progeny. Here, we developed an assay for the simultaneous detection of both chromosome-segregation errors in the marsupial PtK1 cell line by using multiplex fluorescence in situ hybridization with specific painting probes obtained by chromosome flow sorting. No differential susceptibility of the six PtK1 chromosomes to undergo nondisjunction and/or chromosome loss was observed in ana-telophase cells recovering from a nocodazole- or a monastrol-induced mitotic arrest, suggesting that the recurrent presence of specific chromosomes in several cancer types reflects selection effects rather than differential propensities of specific chromosomes to undergo missegregation. Experiments prolonging metaphase duration during drug recovery and inhibiting Aurora-B kinase activity on metaphase-aligned chromosomes provided evidence that some type of merotelic orientations was involved in the origin of both chromosome-segregation errors. Visualization of mero-syntelic kinetochore-microtubule attachments (a merotelic kinetochore in which the thicker microtubule bundle is attached to the same pole to which the sister kinetochore is connected) identified a peculiar malorientation that might participate in the generation of nondisjunction. Our findings imply random missegregation of chromosomes as the initial event in the generation of aneuploidy in mammalian somatic cells.

Published
2009

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