Your search keyword '"Giuseppe Biamonti"' showing total 138 results

1. Post-Translational Modifications Modulate Proteinopathies of TDP-43, FUS and hnRNP-A/B in Amyotrophic Lateral Sclerosis

Author

Stefania Farina, Francesca Esposito, Martina Battistoni, Giuseppe Biamonti, and Sofia Francia

Subjects

post-translational modifications, RNA binding proteins, low-complexity domain, protein aggregations, amyotrophic lateral sclerosis, Biology (General), QH301-705.5

Abstract

It has been shown that protein low-sequence complexity domains (LCDs) induce liquid-liquid phase separation (LLPS), which is responsible for the formation of membrane-less organelles including P-granules, stress granules and Cajal bodies. Proteins harbouring LCDs are widely represented among RNA binding proteins often mutated in ALS. Indeed, LCDs predispose proteins to a prion-like behaviour due to their tendency to form amyloid-like structures typical of proteinopathies. Protein post-translational modifications (PTMs) can influence phase transition through two main events: i) destabilizing or augmenting multivalent interactions between phase-separating macromolecules; ii) recruiting or excluding other proteins and/or nucleic acids into/from the condensate. In this manuscript we summarize the existing evidence describing how PTM can modulate LLPS thus favouring or counteracting proteinopathies at the base of neurodegeneration in ALS.

Published

2021

2. The Krebs Cycle Connection: Reciprocal Influence Between Alternative Splicing Programs and Cell Metabolism

Author

Giuseppe Biamonti, Lucia Maita, and Alessandra Montecucco

Subjects

splicing regulation, histone modifications, piruvate kinase, 2-oxoglutarate-dependent dioxidases (2-OGDD), lysine demethylases (KDM), m6A demethylase, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Alternative splicing is a pervasive mechanism that molds the transcriptome to meet cell and organism needs. However, how this layer of gene expression regulation is coordinated with other aspects of the cell metabolism is still largely undefined. Glucose is the main energy and carbon source of the cell. Not surprisingly, its metabolism is finely tuned to satisfy growth requirements and in response to nutrient availability. A number of studies have begun to unveil the connections between glucose metabolism and splicing programs. Alternative splicing modulates the ratio between M1 and M2 isoforms of pyruvate kinase in this way determining the choice between aerobic glycolysis and complete glucose oxidation in the Krebs cycle. Reciprocally, intermediates in the Krebs cycle may impact splicing programs at different levels by modulating the activity of 2-oxoglutarate-dependent oxidases. In this review we discuss the molecular mechanisms that coordinate alternative splicing programs with glucose metabolism, two aspects with profound implications in human diseases.

Published

2018

3. Chronic Replication Problems Impact Cell Morphology and Adhesion of DNA Ligase I Defective Cells.

Author

Paolo Cremaschi, Matteo Oliverio, Valentina Leva, Silvia Bione, Roberta Carriero, Giulia Mazzucco, Andrea Palamidessi, Giorgio Scita, Giuseppe Biamonti, and Alessandra Montecucco

Subjects

Medicine, Science

Abstract

Moderate DNA damage resulting from metabolic activities or sub-lethal doses of exogenous insults may eventually lead to cancer onset. Human 46BR.1G1 cells bear a mutation in replicative DNA ligase I (LigI) which results in low levels of replication-dependent DNA damage. This replication stress elicits a constitutive phosphorylation of the ataxia telangiectasia mutated (ATM) checkpoint kinase that fails to arrest cell cycle progression or to activate apoptosis or cell senescence. Stable transfection of wild type LigI, as in 7A3 cells, prevents DNA damage and ATM activation. Here we show that parental 46BR.1G1 and 7A3 cells differ in important features such as cell morphology, adhesion and migration. Comparison of gene expression profiles in the two cell lines detects Bio-Functional categories consistent with the morphological and migration properties of LigI deficient cells. Interestingly, ATM inhibition makes 46BR.1G1 more similar to 7A3 cells for what concerns morphology, adhesion and expression of cell-cell adhesion receptors. These observations extend the influence of the DNA damage response checkpoint pathways and unveil a role for ATM kinase activity in modulating cell biology parameters relevant to cancer progression.

Published

2015

4. Oncogenic Alternative Splicing Switches: Role in Cancer Progression and Prospects for Therapy

Author

Serena Bonomi, Stefania Gallo, Morena Catillo, Daniela Pignataro, Giuseppe Biamonti, and Claudia Ghigna

Subjects

Cytology, QH573-671

Abstract

Alterations in the abundance or activities of alternative splicing regulators generate alternatively spliced variants that contribute to multiple aspects of tumor establishment, progression and resistance to therapeutic treatments. Notably, many cancer-associated genes are regulated through alternative splicing suggesting a significant role of this post-transcriptional regulatory mechanism in the production of oncogenes and tumor suppressors. Thus, the study of alternative splicing in cancer might provide a better understanding of the malignant transformation and identify novel pathways that are uniquely relevant to tumorigenesis. Understanding the molecular underpinnings of cancer-associated alternative splicing isoforms will not only help to explain many fundamental hallmarks of cancer, but will also offer unprecedented opportunities to improve the efficacy of anti-cancer treatments.

Published

2013

5. Alternative Splicing and Cancer

Author

Didier Auboeuf, Maria Carmo-Fonseca, Juan Valcarcel, and Giuseppe Biamonti

Subjects

Genetics, QH426-470, Biochemistry, QD415-436

Published

2012

6. Supplementary Figure Legends from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Author

Alessandra Montecucco, Giuseppe Biamonti, Samuela Soza, Maria Rosa Lidonnici, and Rossella Rossi

Abstract

Supplementary Figure Legends from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Published

2023

7. Data from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Author

Alessandra Montecucco, Giuseppe Biamonti, Samuela Soza, Maria Rosa Lidonnici, and Rossella Rossi

Abstract

In mammalian cells, DNA replication takes place in functional subnuclear compartments, called replication factories, where replicative factors accumulate. The distribution pattern of replication factories is diagnostic of the different moments (early, mid, and late) of the S phase. This dynamic organization is affected by different agents that induce cell cycle checkpoint activation via DNA damage or stalling of replication forks. Here, we explore the cell response to etoposide, an anticancer drug belonging to the topoisomerase II poisons. Etoposide does not induce an immediate block of DNA synthesis and progressively affects the distribution of replication proteins in S phase. First, it triggers the formation of large nuclear foci that contain the single-strand DNA binding protein replication protein A (RPA), suggesting that lesions produced by the drug are processed into extended single-stranded regions. These RPA foci colocalize with DNA replicated at the beginning of the treatment. Etoposide also triggers the dispersal of replicative proteins, proliferating cell nuclear antigen and DNA ligase I, from replication factories. This event requires the activity of the ataxia telangiectasia Rad3-related (ATR) checkpoint kinase. By comparing the effect of the drug in cell lines defective in different DNA repair and checkpoint pathways, we show that, along with the downstream kinase Chk1, the Nbs1 protein, mutated in the Nijmegen breakage syndrome, is also relevant for this response and for ATR-dependent phosphorylation. Finally, our analysis evidences a critical role of Nbs1 in the etoposide-induced inhibition of DNA replication in early S phase. (Cancer Res 2006; 66(3): 1675-83)

Published

2023

8. Supplementary Figure 2 from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Author

Alessandra Montecucco, Giuseppe Biamonti, Samuela Soza, Maria Rosa Lidonnici, and Rossella Rossi

Abstract

Supplementary Figure 2 from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Published

2023

9. Supplementary Figure 1 from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Author

Alessandra Montecucco, Giuseppe Biamonti, Samuela Soza, Maria Rosa Lidonnici, and Rossella Rossi

Abstract

Supplementary Figure 1 from The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Published

2023

10. Brief Report: Neuroimaging Endophenotypes of Social Robotic Applications in Autism Spectrum Disorder

Author

Giovanni Pioggia, Giuseppe Biamonti, Liliana Ruta, Flavia Marino, and Antonio Cerasa

Subjects

Male, Research Report, Treatment response, Autism Spectrum Disorder, Endophenotypes, Neuroimaging, Creativity, 03 medical and health sciences, 0302 clinical medicine, Clinical heterogeneity, Developmental and Educational Psychology, medicine, Humans, 0501 psychology and cognitive sciences, Autistic Disorder, Child, Set (psychology), Cognitive science, Social robot, 05 social sciences, Robotics, medicine.disease, Autism spectrum disorder, Endophenotype, Autism, Psychology, 030217 neurology & neurosurgery, 050104 developmental & child psychology

Abstract

A plethora of neuroimaging studies have focused on the discovery of potential neuroendophenotypes useful to understand the etiopathogenesis of autism and predict treatment response. Social robotics has recently been proposed as an effective tool to strengthen the current treatments in children with autism. However, the high clinical heterogeneity characterizing this disorder might interfere with behavioral effects. Neuroimaging is set to overcome these limitations by capturing the level of heterogeneity. Here, we provide a preliminary evaluation of the neural basis of social robotics and how extracting neural hallmarks useful to design more effective behavioral applications. Despite the endophenotype-oriented neuroimaging research approach is in its relative infancy, this preliminary evidence encourages innovation to address its current limitations.

Published

2020

11. Reduced levels of prostaglandin I

Author

Anita, Lombardi, Lavinia, Arseni, Roberta, Carriero, Emmanuel, Compe, Elena, Botta, Debora, Ferri, Martina, Uggè, Giuseppe, Biamonti, Fiorenzo A, Peverali, Silvia, Bione, and Donata, Orioli

Subjects

Xeroderma Pigmentosum, Transcription, Genetic, Ultraviolet Rays, Gene Expression Profiling, Fibroblasts, Biological Sciences, Epoprostenol, Mice, Cytochrome P-450 Enzyme System, Gene Expression Regulation, Neoplasms, Animals, Trichothiodystrophy Syndromes, Cells, Cultured, Skin

Abstract

The cancer-free photosensitive trichothiodystrophy (PS-TTD) and the cancer-prone xeroderma pigmentosum (XP) are rare monogenic disorders that can arise from mutations in the same genes, namely ERCC2/XPD or ERCC3/XPB. Both XPD and XPB proteins belong to the 10-subunit complex transcription factor IIH (TFIIH) that plays a key role in transcription and nucleotide excision repair, the DNA repair pathway devoted to the removal of ultraviolet-induced DNA lesions. Compelling evidence suggests that mutations affecting the DNA repair activity of TFIIH are responsible for the pathological features of XP, whereas those also impairing transcription give rise to TTD. By adopting a relatives-based whole transcriptome sequencing approach followed by specific gene expression profiling in primary fibroblasts from a large cohort of TTD or XP cases with mutations in ERCC2/XPD gene, we identify the expression alterations specific for TTD primary dermal fibroblasts. While most of these transcription deregulations do not impact on the protein level, very low amounts of prostaglandin I(2) synthase (PTGIS) are found in TTD cells. PTGIS catalyzes the last step of prostaglandin I(2) synthesis, a potent vasodilator and inhibitor of platelet aggregation. Its reduction characterizes all TTD cases so far investigated, both the PS-TTD with mutations in TFIIH coding genes as well as the nonphotosensitive (NPS)-TTD. A severe impairment of TFIIH and RNA polymerase II recruitment on the PTGIS promoter is found in TTD but not in XP cells. Thus, PTGIS represents a biomarker that combines all PS- and NPS-TTD cases and distinguishes them from XP.

Published

2021

12. Reduced levels of prostaglandin I 2 synthase: a distinctive feature of the cancer-free trichothiodystrophy

Author

Emmanuel Compe, Roberta Carriero, Anita Lombardi, Elena Botta, Martina Uggè, Silvia Bione, Lavinia Arseni, Giuseppe Biamonti, Donata Orioli, Fiorenzo A. Peverali, and Debora Ferri

Subjects

Multidisciplinary, Transcription Factor TFIIH, Xeroderma pigmentosum, Transcription (biology), DNA repair, medicine, Trichothiodystrophy, Transcription factor II H, ERCC2, Biology, medicine.disease, Molecular biology, Nucleotide excision repair

Abstract

The cancer-free photosensitive trichothiodystrophy (PS-TTD) and the cancer-prone xeroderma pigmentosum (XP) are rare monogenic disorders that can arise from mutations in the same genes, namely ERCC2/XPD or ERCC3/XPB Both XPD and XPB proteins belong to the 10-subunit complex transcription factor IIH (TFIIH) that plays a key role in transcription and nucleotide excision repair, the DNA repair pathway devoted to the removal of ultraviolet-induced DNA lesions. Compelling evidence suggests that mutations affecting the DNA repair activity of TFIIH are responsible for the pathological features of XP, whereas those also impairing transcription give rise to TTD. By adopting a relatives-based whole transcriptome sequencing approach followed by specific gene expression profiling in primary fibroblasts from a large cohort of TTD or XP cases with mutations in ERCC2/XPD gene, we identify the expression alterations specific for TTD primary dermal fibroblasts. While most of these transcription deregulations do not impact on the protein level, very low amounts of prostaglandin I2 synthase (PTGIS) are found in TTD cells. PTGIS catalyzes the last step of prostaglandin I2 synthesis, a potent vasodilator and inhibitor of platelet aggregation. Its reduction characterizes all TTD cases so far investigated, both the PS-TTD with mutations in TFIIH coding genes as well as the nonphotosensitive (NPS)-TTD. A severe impairment of TFIIH and RNA polymerase II recruitment on the PTGIS promoter is found in TTD but not in XP cells. Thus, PTGIS represents a biomarker that combines all PS- and NPS-TTD cases and distinguishes them from XP.

Published

2021

13. LINP1 lncRNA expression profile is modulated in response to DNA damage

Author

Giuseppe Biamonti, Roberta Carriero, Lucia Maita, Silvia Bione, and Alessandra Montecucco

Subjects

Non-homologous end joining, Genome instability, chemistry.chemical_classification, chemistry.chemical_compound, DNA ligase, chemistry, DNA damage, DNA repair, Cancer cell, DNA replication, Biology, DNA, Cell biology

Abstract

Rapidly dividing cancer cells show elevated levels of DNA double-strand breaks (DSBs) resulting from replication stress and linked to genome instability. To verify the hypothesis that a low level of endogenous replicative DNA damage may impact gene expression programs and cell biology features relevant to cancer progression, we used DNA ligase I (LigI) defective 46BR.1G1 fibroblasts, deriving from a patient who died at 19 for lymphoma, and the 7A3 cell clone, obtained from 46BR.1G1 by stably expressing ectopic wild-type LigI. LigI deficiency impairs maturation of newly synthesized DNA and increases the number of DSBs and γH2AX foci, features associated with genome instability commonly found also in pre-neoplastic lesions. In order to decipher the strategy used to cope with replicative DNA damage, we have compared gene expression profiles in 46BR.1G1 and 7A3 cells. Among the differentially expressed genes, we identified a group of long noncoding RNAs (lncRNAs) which show significant transcriptional alteration in 46BR.1G1 cells, and appear to be relevant for cancer progression. An interesting up-regulated lncRNA in 46BR.1G1 cells is LINP1 (lncRNA in nonhomologous end joining (NHEJ) pathway 1) which has been shown to be involved in DNA repair. We have observed that LINP1 up-regulation contributes to proliferation and survival of 46BR.1G1 that could account for genome instability. Moreover, we observed that LINP1 is upregulated at later times in control human fibroblasts exposed to exogenous sources of DNA damage. Our observations support the notion that LINP1 lncRNA targeting could reduce the DNA repair efficacy of tumour cells. * These authors contributed equally to this work.

Published

2021

14. HGF/c-Met Signalling in the Tumor Microenvironment

Author

Alberto, Zambelli, Giuseppe, Biamonti, and Angela, Amato

Subjects

Hepatocyte Growth Factor, Neoplasms, Tumor Microenvironment, Humans, Proto-Oncogene Proteins c-met, Signal Transduction

Abstract

Recently, it has become clearer that tumor plasticity increases the chance that cancer cells could acquire new mechanisms to escape immune surveillance, become resistant to conventional drugs, and spread to distant sites.Effectively, tumor plasticity drives adaptive response of cancer cells to hypoxia and nutrient deprivation leading to stimulation of neoangionesis or tumor escape. Therefore, tumor plasticity is believed to be a great contributor in recurrence and metastatic dissemination of cancer cells. Importantly, it could be an Achilles' heel of cancer if we could identify molecular mechanisms dictating this phenotype.The reactivation of stem-like signalling pathways is considered a great determinant of tumor plasticity; in addition, a key role has been also attributed to tumor microenvironment (TME). Indeed, it has been proved that cancer cells interact with different cells in the surrounding extracellular matrix (ECM). Interestingly, well-established communication represents a potential allied in maintenance of a plastic phenotype in cancer cells supporting tumor growth and spread. An important signalling pathway mediating cancer cell-TME crosstalk is represented by the HGF/c-Met signalling.Here, we review the role of the HGF/c-Met signalling in tumor-stroma crosstalk focusing on novel findings underlying its role in tumor plasticity, immune escape, and development of adaptive mechanisms.

Published

2020

15. HGF/c-Met Signalling in the Tumor Microenvironment

Author

Alberto Zambelli, Angela Amato, and Giuseppe Biamonti

Subjects

Tumor microenvironment, C-Met, Inflammation, Biology, medicine.disease, Hedgehog signaling pathway, Metastasis, 03 medical and health sciences, chemistry.chemical_compound, Crosstalk (biology), 0302 clinical medicine, chemistry, Tumor Escape, Cancer cell, Cancer research, medicine, 030212 general & internal medicine, medicine.symptom

Abstract

Recently, it has become clearer that tumor plasticity increases the chance that cancer cells could acquire new mechanisms to escape immune surveillance, become resistant to conventional drugs, and spread to distant sites.Effectively, tumor plasticity drives adaptive response of cancer cells to hypoxia and nutrient deprivation leading to stimulation of neoangionesis or tumor escape. Therefore, tumor plasticity is believed to be a great contributor in recurrence and metastatic dissemination of cancer cells. Importantly, it could be an Achilles' heel of cancer if we could identify molecular mechanisms dictating this phenotype.The reactivation of stem-like signalling pathways is considered a great determinant of tumor plasticity; in addition, a key role has been also attributed to tumor microenvironment (TME). Indeed, it has been proved that cancer cells interact with different cells in the surrounding extracellular matrix (ECM). Interestingly, well-established communication represents a potential allied in maintenance of a plastic phenotype in cancer cells supporting tumor growth and spread. An important signalling pathway mediating cancer cell-TME crosstalk is represented by the HGF/c-Met signalling.Here, we review the role of the HGF/c-Met signalling in tumor-stroma crosstalk focusing on novel findings underlying its role in tumor plasticity, immune escape, and development of adaptive mechanisms.

Published

2020

16. Heat Shock Affects Mitotic Segregation of Human Chromosomes Bound to Stress-Induced Satellite III RNAs

Author

Marco Biggiogera, Giuseppe Biamonti, Alessandra Montecucco, Manuela Giordano, and Lucia Infantino

Subjects

0301 basic medicine, Heterochromatin, chromosome segregation, Mitosis, Chromosome 9, DNA, Satellite, Article, Catalysis, lcsh:Chemistry, Inorganic Chemistry, Chromosome segregation, 03 medical and health sciences, 0302 clinical medicine, Heat Shock Transcription Factors, Chromosome instability, nuclear stress bodies, Chromosomes, Human, Humans, Physical and Theoretical Chemistry, lcsh:QH301-705.5, Molecular Biology, Spectroscopy, Chemistry, Organic Chemistry, Chromosome, General Medicine, Argonaute, heat shock, Computer Science Applications, Cell biology, Chromatin, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, 030220 oncology & carcinogenesis, RNA, Small Untranslated, non-coding RNAs, RNA, Long Noncoding, Transcription Initiation Site, HeLa Cells

Abstract

Heat shock activates the transcription of arrays of Satellite III (SatIII) DNA repeats in the pericentromeric heterochromatic domains of specific human chromosomes, the longest of which is on chromosome 9. Long non-coding SatIII RNAs remain associated with transcription sites where they form nuclear stress bodies or nSBs. The biology of SatIII RNAs is still poorly understood. Here, we show that SatIII RNAs and nSBs are detectable up to four days after thermal stress and are linked to defects in chromosome behavior during mitosis. Heat shock perturbs the execution of mitosis. Cells reaching mitosis during the first 3 h of recovery accumulate in pro-metaphase. During the ensuing 48 h, this block is no longer detectable, however, a significant fraction of mitoses shows chromosome segregation defects. Notably, most of lagging chromosomes and chromosomal bridges are bound to nSBs and contain arrays of SatIII DNA. Disappearance of mitotic defects at the end of day 2 coincides with the processing of long non-coding SatIII RNAs into a ladder of small RNAs associated with chromatin and ranging in size from 25 to 75 nt. The production of these molecules does not rely on DICER and Argonaute 2 components of the RNA interference apparatus. Thus, massive transcription of SatIII DNA may contribute to chromosomal instability.

Published

2020

17. CorrelaGenes: a new tool for the interpretation of the human transcriptome.

Author

Paolo Cremaschi, Sergio Rovida, Lucia Sacchi, Antonella Lisa, Francesca Calvi, Alessandra Montecucco, Giuseppe Biamonti, Silvia Bione, and Gianni Sacchi

Published

2014

18. The Krebs Cycle Connection: Reciprocal Influence Between Alternative Splicing Programs and Cell Metabolism

Author

Alessandra Montecucco, Giuseppe Biamonti, and Lucia Maita

Subjects

0301 basic medicine, Regulation of gene expression, Cancer Research, piruvate kinase, histone modifications, DNA demethylases (TETs), Alternative splicing, Review, Metabolism, 2-oxoglutarate-dependent dioxidases (2-OGDD), Biology, m6A demethylase, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Cell biology, splicing regulation, Transcriptome, 03 medical and health sciences, 030104 developmental biology, Cell metabolism, Oncology, Anaerobic glycolysis, RNA splicing, lysine demethylases (KDM), Pyruvate kinase

Abstract

Alternative splicing is a pervasive mechanism that molds the transcriptome to meet cell and organism needs. However, how this layer of gene expression regulation is coordinated with other aspects of the cell metabolism is still largely undefined. Glucose is the main energy and carbon source of the cell. Not surprisingly, its metabolism is finely tuned to satisfy growth requirements and in response to nutrient availability. A number of studies have begun to unveil the connections between glucose metabolism and splicing programs. Alternative splicing modulates the ratio between M1 and M2 isoforms of pyruvate kinase in this way determining the choice between aerobic glycolysis and complete glucose oxidation in the Krebs cycle. Reciprocally, intermediates in the Krebs cycle may impact splicing programs at different levels by modulating the activity of 2-oxoglutarate-dependent oxidases. In this review we discuss the molecular mechanisms that coordinate alternative splicing programs with glucose metabolism, two aspects with profound implications in human diseases.

Published

2018

19. From 'Cellular' RNA to 'Smart' RNA: Multiple Roles of RNA in Genome Stability and Beyond

Author

Giuseppe Biamonti, Brian Luke, Piero Carninci, Julio Aguado, Zachary Thomas Neeb, Chance Meers, Ameya P. Jalihal, Nils G. Walter, Mariusz Nowacki, Francesca Rossiello, Flavia Michelini, Fabrizio d'Adda di Fagagna, Ubaldo Gioia, Corey Winston Jones-Weinert, Francesca Storici, and Sofia Francia

Subjects

0301 basic medicine, Genome instability, Regulation of gene expression, RNA, Untranslated, Transcription, Genetic, Chemistry, RNA-Binding Proteins, RNA, RNA-binding protein, General Chemistry, Computational biology, Non-coding RNA, Article, Genomic Instability, 03 medical and health sciences, 030104 developmental biology, Gene Expression Regulation, Transcription (biology), RNA interference, Gene expression, Humans, 570 Life sciences, biology, DNA Breaks, Double-Stranded, RNA Interference, DNA Damage

Abstract

Coding for proteins has been considered the main function of RNA since the "central dogma" of biology was proposed. The discovery of noncoding transcripts shed light on additional roles of RNA, ranging from the support of polypeptide synthesis, to the assembly of subnuclear structures, to gene expression modulation. Cellular RNA has therefore been recognized as a central player in often unanticipated biological processes, including genomic stability. This ever-expanding list of functions inspired us to think of RNA as a "smart" phone, which has replaced the older obsolete "cellular" phone. In this review, we summarize the last two decades of advances in research on the interface between RNA biology and genome stability. We start with an account of the emergence of noncoding RNA, and then we discuss the involvement of RNA in DNA damage signaling and repair, telomere maintenance, and genomic rearrangements. We continue with the depiction of single-molecule RNA detection techniques, and we conclude by illustrating the possibilities of RNA modulation in hopes of creating or improving new therapies. The widespread biological functions of RNA have made this molecule a reoccurring theme in basic and translational research, warranting it the transcendence from classically studied "cellular" RNA to "smart" RNA.

Published

2018

20. A missense MT-ND5 mutation in differentiated Parkinson Disease cytoplasmic hybrid induces ROS-dependent DNA Damage Response amplified by DROSHA

Author

Antonio Torroni, Stefania Brandini, Anna Olivieri, Giuseppe Biamonti, Giulia Brenna, Sofia Francia, Daniela Pignataro, Alessandra Montecucco, and Francesca Zanetta

Subjects

0301 basic medicine, Ribonuclease III, Cytoplasm, DNA damage, Cellular differentiation, Mutation, Missense, lcsh:Medicine, Mitochondrion, Biology, medicine.disease_cause, Cytoplasmic hybrid, Article, Cell Line, Histones, 03 medical and health sciences, RNA interference, medicine, Humans, Amino Acid Sequence, Phosphorylation, lcsh:Science, Drosha, Alleles, Mutation, Multidisciplinary, lcsh:R, Cell Differentiation, NADH Dehydrogenase, Parkinson Disease, Molecular biology, Nuclear DNA, body regions, 030104 developmental biology, lcsh:Q, Reactive Oxygen Species, DNA Damage

Abstract

Genome integrity is continuously threatened by endogenous sources of DNA damage including reactive oxygen species (ROS) produced by cell metabolism. Factors of the RNA interference (RNAi) machinery have been recently involved in the cellular response to DNA damage (DDR) in proliferating cells. To investigate the impact of component of RNAi machinery on DDR activation in terminally differentiated cells, we exploited cytoplasmic hybrid (cybrid) cell lines in which mitochondria of sporadic Parkinson’s disease patients repopulate neuroblastoma SH-SY5Y-Rho(0) cells. Upon differentiation into dopaminergic neuron-like cells, PD63 cybrid showed increased intracellular level of ROS and chronic DDR activation, compared to other cybrids with the same nuclear background. Importantly, DDR activation in these cells can be prevented by ROS scavenging treatment suggesting that ROS production is indeed causative of nuclear DNA damage. Sequence analysis of the mitogenomes identified a rare and heteroplasmic missense mutation affecting a highly conserved residue of the ND5-subunit of respiratory complex I, which accounts for ROS increase. We demonstrated that the assembly of nuclear DDR foci elicited by oxidative stress in these cells relies on DROSHA, providing the first evidence that components of RNAi machinery play a crucial role also in the mounting of ROS-induced DDR in non-replicating neuronal cells.

Published

2017

21. The alternative splicing side of cancer

Author

Daniela Pignataro, Alessandra Montecucco, Morena Catillo, Claudia Ghigna, and Giuseppe Biamonti

Subjects

Epithelial-Mesenchymal Transition, Computational biology, Biology, medicine.disease_cause, Neoplasms, Tumor Microenvironment, medicine, Humans, Epigenetics, Regulation of gene expression, Genetics, Models, Genetic, Serine-Arginine Splicing Factors, Mechanism (biology), Alternative splicing, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Nucleosomes, Chromatin, Gene Expression Regulation, Neoplastic, Alternative Splicing, RNA splicing, Signal transduction, Carcinogenesis, Signal Transduction, Developmental Biology

Abstract

Alternative splicing emerges as a potent and pervasive mechanism of gene expression regulation that expands the coding capacity of the genome and forms an intermediate layer of regulation between transcriptional and post-translational networks. Indeed, alternative splicing occupies a pivotal position in developmental programs and in the cell response to external and internal stimuli. Not surprisingly, therefore, its deregulation frequently leads to human disease. In this review we provide an updated overview of the impact of alternative splicing on tumorigenesis. Moreover, we discuss the intricacy of the reciprocal interactions between alternative splicing programs and signal transduction pathways, which appear to be crucially linked to cancer progression in response to the tumor microenvironment. Finally, we focus on the recently described interplay between splicing and chromatin organization which is expected to shed new lights into gene expression regulation in normal and cancer cells.

Published

2014

22. HnRNP A1 controls a splicing regulatory circuit promoting mesenchymal-to-epithelial transition

Author

Claudia Ghigna, Giuseppe Biamonti, Anna Di Matteo, Serena Bonomi, Francisco E. Baralle, Emanuele Buratti, and Daphne S. Cabianca

Subjects

Epithelial-Mesenchymal Transition, Heterogeneous Nuclear Ribonucleoprotein A1, Regulatory Sequences, Ribonucleic Acid, Receptor tyrosine kinase, Exon, Cell Line, Tumor, Heterogeneous-Nuclear Ribonucleoprotein Group A-B, Genetics, Humans, Epithelial–mesenchymal transition, Enhancer, biology, HEK 293 cells, Alternative splicing, Receptor Protein-Tyrosine Kinases, Exons, Molecular biology, Exon skipping, Cell biology, Nonsense Mediated mRNA Decay, Alternative Splicing, HEK293 Cells, RNA splicing, biology.protein, RNA, HeLa Cells

Abstract

Epithelial-to-mesenchymal transition (EMT) is an embryonic program used by cancer cells to acquire invasive capabilities becoming metastatic. ΔRon, a constitutively active isoform of the Ron tyrosine kinase receptor, arises from skipping of Ron exon 11 and provided the first example of an alternative splicing variant causatively linked to the activation of tumor EMT. Splicing of exon 11 is controlled by two adjacent regulatory elements, a silencer and an enhancer of splicing located in exon 12. The alternative splicing factor and oncoprotein SRSF1 directly binds to the enhancer, induces the production of ΔRon and activates EMT leading to cell locomotion. Interestingly, we now find an important role for hnRNP A1 in controlling the activity of the Ron silencer. HnRNP A1 is able to antagonize the binding of SRSF1 and prevent exon skipping. Notably, hnRNP A1, by inhibiting the production of ΔRon, activates the reversal program, namely the mesenchymal-to-epithelial transition, which instead occurs at the final metastasis sites. Also, hnRNP A1 affects Ron splicing by regulating the expression level of hnRNP A2/B1, which similarly to SRSF1 can promote ΔRon production. These results shed light on how splicing regulation contributes to the tumor progression and provide potential targets to develop anticancer therapies.

Published

2013

23. First Dual AK/GSK-3β Allosteric Inhibitors Endowed with Antioxidant Properties as Multifunctional, Potential Neuroprotective Agents

Author

Alessandra Pecorelli, Stefania Butini, Lida Savi, Federico Focher, Margherita Brindisi, Gloria Alfano, Giulia Chemi, Giuseppe Valacchi, Paola Galatello, Erika Pambianchi, Simone Brogi, Giulia Compagnoni, Anna Ramunno, Giuseppe Campiani, Sandra Gemma, Giuseppe Biamonti, Brogi, Simone, Ramunno, Anna, Savi, Lida, Chemi, Giulia, Alfano, Gloria, Pecorelli, Alessandra, Pambianchi, Erika, Galatello, Paola, Compagnoni, Giulia, Focher, Federico, Biamonti, Giuseppe, Valacchi, Giuseppe, Butini, Stefania, Gemma, Sandra, Campiani, Giuseppe, and Brindisi, Margherita

Subjects

0301 basic medicine, Pharmacology, Antioxidants, Neuroblastoma, 0302 clinical medicine, Adenosine kinase (AK), Antioxidant agents, Dual inhibitors, Glycogen synthase kinase 3 beta (GSK-3β), Molecular docking, Adenosine Kinase, Cell Line, Tumor, Dose-Response Relationship, Drug, Glycogen Synthase Kinase 3 beta, Humans, Hydrogen Peroxide, Molecular Structure, Neuroprotective Agents, Oxidative Stress, Protein Kinase Inhibitors, Reactive Oxygen Species, Structure-Activity Relationship, Drug Discovery, Cytotoxicity, chemistry.chemical_classification, Tumor, biology, General Medicine, Biochemistry, Antioxidant, Drug, Reactive Oxygen Specie, Human, Antioxidant agent, Neuroprotective Agent, Allosteric regulation, Protein Kinase Inhibitor, Adenosine kinase, Glycogen synthase kinase 3 beta (GSK-3β), Neuroprotection, Cell Line, NO, Dose-Response Relationship, 03 medical and health sciences, Structure–activity relationship, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, GSK3B, Reactive oxygen species, Oxidative Stre, 030104 developmental biology, Enzyme, chemistry, biology.protein, Dual inhibitor, 030217 neurology & neurosurgery

Abstract

The manuscript deals with the design, synthesis and biological evaluation of novel benzoxazinone-based and indole-based compounds as multifunctional neuroprotective agents. These compounds inhibit human adenosine kinase (hAK) and human glycogen synthase kinase 3 beta (hGSK-3β) enzymes. Computational analysis based on a molecular docking approach underlined the potential structural requirements for simultaneously targeting both proteins' allosteric sites. In silico hints drove the synthesis of appropriately decorated benzoxazinones and indoles (5a-s, and 6a-c) and biochemical analysis revealed their behavior as allosteric inhibitors of hGSK-3β. For both our hit 4 and the best compounds of the series (5c,l and 6b) the potential antioxidant profile was assessed in human neuroblastoma cell lines (IMR 32, undifferentiated and neuronal differentiated), by evaluating the protective effect of selected compounds against H2O2 cytotoxicity and reactive oxygen species (ROS) production. Results showed a strong efficacy of the tested compounds, even at the lower doses, in counteracting the induced oxidative stress (50 μM of H2O2) and in preventing ROS formation. In addition, the tested compounds did not show any cytotoxic effect determined by the LDH release, at the concentration range analyzed (from 0.1 to 50 μM). This study allowed the identification of compound 5l, as the first dual hAK/hGSK-3β inhibitor reported to date. Compound 5l, which behaves as an effective antioxidant, holds promise for the development of new series of potential therapeutic agents for the treatment of neurodegenerative diseases characterized by an innovative pharmacological profile.

Published

2017

24. DNA and RNA Metabolism Meet at Chromatin to Control Genome Stability

Author

Alessandra Montecucco and Giuseppe Biamonti

Subjects

0301 basic medicine, DNA re-replication, DNA Replication, lcsh:QH426-470, DNA repair, Eukaryotic DNA replication, Biology, DNA damage response, 03 medical and health sciences, Control of chromosome duplication, DNA damge respon, Genetics, Replication protein A, Genetics (clinical), Epigenomics, RNA metabolism, Histone Modifications, Cell biology, Chromatin, lcsh:Genetics, Editorial, 030104 developmental biology, Oncology, Molecular Medicine, Origin recognition complex, genome stability

Abstract

The integrity of the genome is continuously challenged by endogenous and exogenous DNA damaging agents and by lesions arising during DNA replication and transcription. To prevent the severe biological consequences that may arise from DNA injuries, cells have evolved an intricate network of genome surveillance mechanisms, collectively designated as DNA damage response (DDR). In addition to damage-specific repair machineries, perturbations in the structure and continuity of the DNA molecule trigger checkpoint pathways that delay or arrest cell-cycle progression thus providing more time for repair mechanisms. Moreover, checkpoint pathways coordinate DNA repair with DNA replication and transcription. Functional alterations in any of these processes and in their crosstalk may result in uncontrolled cell proliferation or programmed cell death, two opposite events that are harmful both at the cellular and organismal level. DNA in the eukaryotic genome folds, for most part, into the canonical B-form and is packaged into chromatin that is the substrate of all DNA transactions. Complex DNA secondary structures (G-quadruplexes), hybrid DNA/RNA structures (R-loops), and changes in chromatin architecture induced by reversible histone post-translational modifications, incorporation of histone variants and ATP-dependent chromatin remodeling enzymes, occur in response to external and cellular cues and affect vital processes such as regulation of gene expression, DNA replication, and repair. Histone modifications are best understood for their effects on transcription, but it is becoming increasingly evident that they also function in the DDR, where chromatin reorganization is required to allow access of repair proteins to DNA lesions. However, we are still far from a clear and comprehensive picture of chromatin dynamics in relation to DDR. Finally, recent data implicate splicing factors, small non-coding RNAs, and components of the RNA interference machinery in chromatin organization both in unstressed cells and in response to DNA damage. The articles in this special issue provide a view of the complex network of interactions between DNA and RNA metabolism that contribute to genome stability in eukaryotic cells. DNA replication is an extremely risky process. Cea et al. address the problem of complex secondary structures such as G-quadruplexes (G4) that can constitute an obstacle to DNA and RNA metabolism. The resolution and replication of structured DNA is therefore crucial to prevent genetic and epigenetic instability across the genome. The authors focus on how G4 DNA is resolved during replication, and how its successful bypass requires the coordinated activity of single stranded DNA (ssDNA) binding proteins, helicases, and specialized DNA polymerases. G-rich elements with potential to form G-quadruplex structures have been described in most of the replication origins in mouse and human cells (Besnard et al., 2012). In their intriguing perspective Lombrana et al. propose that R-loops form at CpG island promoters during transcription and can contribute to DNA replication origin specification just activating the formation of G4 structures that recruit the Origin Recognition Complex. In this hypothesis R-loop dysregulation at CpG islands associated with promoter-origin regions might contribute to the phenotype of DNA replication abnormalities and to the loss of genome integrity detected in cancer cells. R-loops can also be the pathological outcome of replication and transcription collisions. Brambati et al. review the current knowledge on replication and transcription conflicts in eukaryotes, their consequences on genome instability and the pathways involved in their resolution, whose understanding is relevant to clarify the molecular basis of cancer and neurodegenerative diseases. R-loop structures also form at telomeres in yeast and in mammalian cells where the TERRA (telomeric repeat-containing RNA) transcripts can base pair with their template DNA. Cusanelli and Chartrand discuss the recent developments on TERRA's role in telomere biology and genome integrity, and its implication in cancer. A growing body of evidence suggests that different types of non-coding RNAs (ncRNAs) can directly affect chromatin conformation, and in this way may impact transcription and splicing, as well as promote the activation of DDR. Recently, it has been suggested that small ncRNAs generated by the RNA interference machinery are involved in DDR signaling and homology-mediated DNA repair. Francia reviews the experimental evidence that ncRNAs act at the genomic loci from which they are transcribed to modulate chromatin organization, DDR and DNA repair. Mounting evidence supports the idea that RNA-binding proteins involved in different steps of mRNA life can affect genome stability programs (Montecucco and Biamonti). In this issue Naro et al. focus on the non-canonical role of splicing factors and DNA repair proteins as gatekeepers of genome stability. In fact, several splicing factors have been recently shown to play direct function in DNA repair, beyond their expected splicing activity, and at the same time evidence is emerging that DNA repair proteins can act as post-transcriptional regulators of gene expression. This finding suggests the existence of a tight interplay between splicing regulation and DNA safeguard mechanisms ensuring genome stability. Among reversible protein modifications, ubiquitination is broadly implicated in cellular functions. In particular, signaling processes mediated by ubiquitin are crucial for the cellular response to DNA double-strand breaks (DSBs). Citterio discusses the current knowledge of how ubiquitin-mediated signaling at DSBs is controlled by deubiquitinating enzymes (DUBs) with particular emphasis on histone DUBs and their recent involvement in stem cell biology and cancer.

Published

2016

25. Making alternative splicing decisions during epithelial-to-mesenchymal transition (EMT)

Author

Stefania Gallo, Claudia Ghigna, Serena Bonomi, and Giuseppe Biamonti

Subjects

rac1 GTP-Binding Protein, Epithelial-Mesenchymal Transition, Computational biology, Biology, Cellular and Molecular Neuroscience, Proto-Oncogenes, Gene expression, Tumor Microenvironment, medicine, Animals, Humans, Neoplasm Invasiveness, Epithelial–mesenchymal transition, Neoplasm Metastasis, Molecular Biology, Gene, Pharmacology, Genetics, Models, Genetic, Serine-Arginine Splicing Factors, Carcinoma, Alternative splicing, Nuclear Proteins, RNA-Binding Proteins, Receptor Protein-Tyrosine Kinases, Cancer, Cell Biology, medicine.disease, Alternative Splicing, Hyaluronan Receptors, Tumor progression, Cancer cell, Molecular Medicine

Abstract

Alternative splicing generates multiple mRNAs from a single transcript and is a major contributor to proteomic diversity and to the control of gene expression in complex organisms. Not surprisingly, this post-transcriptional event is tightly regulated in different tissues and developmental stages. An increasing body of evidences supports a causative role of aberrant alternative splicing in cancer. However, very little is known about its impact on cellular processes crucially involved in tumor progression. The aim of this review is to discuss the link between alternative splicing and the epithelial-to-mesenchymal transition (EMT), one of the major routes by which cancer cells acquire invasive capabilities and become metastatic. We begin with a brief overview of alternative splicing. Next, we discuss alternative splicing factors that regulate EMT. Finally, we provide examples of target genes presenting alternative splicing changes that contribute to the morphological conversions in the EMT process.

Published

2012

26. Phosphorylation of SRSF1 is modulated by replicational stress

Author

Alessandra Montecucco, Anna Bardoni, Antonella Lisa, Serena Camerini, Giuseppe Biamonti, Marco Crescenzi, Serena Giuliano, and Valentina Leva

Subjects

DNA Replication, Proteomics, DNA Ligases, DNA repair, DNA damage, Hyperphosphorylation, Genome Integrity, Repair and Replication, Biology, DNA Ligase I Deficiency, DNA Ligase ATP, Splicing factor, Stress, Physiological, Genetics, Humans, Phosphorylation, Cell Line, Transformed, chemistry.chemical_classification, DNA ligase, Serine-Arginine Splicing Factors, Alternative splicing, DNA replication, Nuclear Proteins, RNA-Binding Proteins, Molecular biology, Alternative Splicing, chemistry, DNA Damage

Abstract

DNA ligase I-deficient 46BR.1G1 cells show a delay in the maturation of replicative intermediates resulting in the accumulation of single- and double-stranded DNA breaks. As a consequence the ataxia telangiectasia mutated protein kinase (ATM) is constitutively phosphorylated at a basal level. Here, we use 46BR.1G1 cells as a model system to study the cell response to chronic replication-dependent DNA damage. Starting from a proteomic approach, we demonstrate that the phosphorylation level of factors controlling constitutive and alternative splicing is affected by the damage elicited by DNA ligase I deficiency. In particular, we show that SRSF1 is hyperphosphorylated in 46BR.1G1 cells compared to control fibroblasts. This hyperphosphorylation can be partially prevented by inhibiting ATM activity with caffeine. Notably, hyperphosphorylation of SRSF1 affects the subnuclear distribution of the protein and the alternative splicing pattern of target genes. We also unveil a modulation of SRSF1 phosphorylation after exposure of MRC-5V1 control fibroblasts to different exogenous sources of DNA damage. Altogether, our observations indicate that a relevant aspect of the cell response to DNA damage involves the post-translational regulation of splicing factor SRSF1 which is associated with a shift in the alternative splicing program of target genes to control cell survival or cell death.

Published

2011

27. DNA replication, development and cancer: a homeotic connection?

Author

Arturo Falaschi, Gulnara Abdurashidova, and Giuseppe Biamonti

Subjects

DNA Replication, Homeodomain Proteins, Genetics, Genome, Human, DNA replication, Gene Expression Regulation, Developmental, Replication Origin, Eukaryotic DNA replication, Biology, Pre-replication complex, Biochemistry, Substrate Specificity, DNA replication factor CDT1, Licensing factor, Control of chromosome duplication, Neoplasms, biology.protein, Animals, Humans, Origin recognition complex, Homeotic gene, Molecular Biology, Cell Proliferation

Abstract

The homeotic proteins are transcription factors, highly conserved in metazoan organisms, exerting a pivotal role in development and differentiation. They individually display a loose specificity for the DNA sequence they can bind, but operate mainly in multi-molecular associations that assure their target and function specificity. Homeotic proteins are known to play a role in the positive or negative regulation of cell proliferation. Furthermore, many homeotic proteins are actually proto-oncogenes, since different translocations involving their genes cause tumors, particularly in the hematopoietic system. A one-hybrid screen to detect proteins with affinity for the lamin B2 replication origin identified three homeotic proteins, namely HoxA13, HoxC10 and HoxC13. Recent data demonstrate that the HoxC13 oncoprotein specifically associates with replication foci and binds in vitro and in vivo to several human DNA replication origins. Moreover, Hox proteins interact with geminin, a regulator of cell cycle progression, and control the interaction of this protein with the DNA replication licensing factor Ctd1. Thus, the homeotic proteins, by participating directly in the function of DNA replication origins, may provide a direct link between the accurate regulation of DNA replication required by the morphogenetic program and the deregulation of this process typical of cancer.

Published

2009

28. DNA Ligase I Deficiency Leads to Replication-Dependent DNA Damage and Impacts Cell Morphology without Blocking Cell Cycle Progression

Author

Riccardo Vago, Giovanni Ferrari, Samuela Soza, Valentina Leva, Giuseppe Biamonti, Giuliano Mazzini, and Alessandra Montecucco

Subjects

DNA Replication, DNA Ligases, DNA repair, DNA damage, Eukaryotic DNA replication, Biology, Cell Line, DNA Ligase I Deficiency, Histones, DNA Ligase ATP, Humans, DNA Breaks, Double-Stranded, CHEK1, Phosphorylation, Cell Shape, Molecular Biology, Cytoskeleton, Skin, Cell Cycle, DNA replication, Articles, Cell Biology, Cell cycle, G2-M DNA damage checkpoint, Molecular biology, Cell biology, Mutant Proteins, DNA Damage

Abstract

46BR.1G1 cells derive from a patient with a genetic syndrome characterized by drastically reduced replicative DNA ligase I (LigI) activity and delayed joining of Okazaki fragments. Here we show that the replication defect in 46BR.1G1 cells results in the accumulation of both single-stranded and double-stranded DNA breaks. This is accompanied by phosphorylation of the H2AX histone variant and the formation of gammaH2AX foci that mark damaged DNA. Single-cell analysis demonstrates that the number of gammaH2AX foci in LigI-defective cells fluctuates during the cell cycle: they form in S phase, persist in mitosis, and eventually diminish in G(1) phase. Notably, replication-dependent DNA damage in 46BR.1G1 cells only moderately delays cell cycle progression and does not activate the S-phase-specific ATR/Chk1 checkpoint pathway that also monitors the execution of mitosis. In contrast, the ATM/Chk2 pathway is activated. The phenotype of 46BR.1G1 cells is efficiently corrected by the wild-type LigI but is worsened by a LigI mutant that mimics the hyperphosphorylated enzyme in M phase. Notably, the expression of the phosphomimetic mutant drastically affects cell morphology and the organization of the cytoskeleton, unveiling an unexpected link between endogenous DNA damage and the structural organization of the cell.

Published

2009

29. Alternative Splicing and Tumor Progression

Author

Giuseppe Biamonti, Cristina Valacca, and Claudia Ghigna

Subjects

Genetics, Alternative splicing, EMT, Computational biology, Biology, Article, Malignant transformation, biomarkers, Tumor progression, Transcription (biology), splicing factors, Proteome, RNA splicing, splicing correction, cancer, Signal transduction, Gene, Genetics (clinical)

Abstract

Alternative splicing is a key molecular mechanism for increasing the functional diversity of the eukaryotic proteomes. A large body of experimental data implicates aberrant splicing in various human diseases, including cancer. Both mutations in cis-acting splicing elements and alterations in the expression and/or activity of splicing regulatory factors drastically affect the splicing profile of many cancer-associated genes. In addition, the splicing profile of several cancer-associated genes is altered in particular types of cancer arguing for a direct role of specific splicing isoforms in tumor progression. Deciphering the mechanisms underlying aberrant splicing in cancer may prove crucial to understand how splicing machinery is controlled and integrated with other cellular processes, in particular transcription and signaling pathways. Moreover, the characterization of splicing deregulation in cancer will lead to a better comprehension of malignant transformation. Cancer-associated alternative splicing variants may be new tools for the diagnosis and classification of cancers and could be the targets for innovative therapeutical interventions based on highly selective splicing correction approaches.

Published

2008

30. Transcription of Satellite III non-coding RNAs is a general stress response in human cells

Author

Claudia Ghigna, Rut Valgardsdottir, Silvano Riva, Ilaria Chiodi, Giuseppe Biamonti, Antonio Rossi, Manuela Giordano, and Silvia Bazzini

Subjects

Transcriptional Activation, RNA, Untranslated, CHO Cells, Biology, DNA, Satellite, chemistry.chemical_compound, Cricetulus, Heat Shock Transcription Factors, Transcription (biology), Osmotic Pressure, Cricetinae, Genetics, Animals, Humans, HSF1, Transcription factor, Molecular Biology, General transcription factor, NFATC Transcription Factors, Reverse Transcriptase Polymerase Chain Reaction, RNA, Promoter, Molecular biology, Long non-coding RNA, Cell Nucleus Structures, DNA-Binding Proteins, chemistry, DNA, Heat-Shock Response, HeLa Cells, Transcription Factors

Abstract

In heat-shocked human cells, heat shock factor 1 activates transcription of tandem arrays of repetitive Satellite III (SatIII) DNA in pericentromeric heterochromatin. Satellite III RNAs remain associated with sites of transcription in nuclear stress bodies (nSBs). Here we use real-time RT-PCR to study the expression of these genomic regions. Transcription is highly asymmetrical and most of the transcripts contain the G-rich strand of the repeat. A low level of G-rich RNAs is detectable in unstressed cells and a 10(4)-fold induction occurs after heat shock. G-rich RNAs are induced by a wide range of stress treatments including heavy metals, UV-C, oxidative and hyper-osmotic stress. Differences exist among stressing agents both for the kinetics and the extent of induction (>100- to 80.000-fold). In all cases, G-rich transcripts are associated with nSBs. On the contrary, C-rich transcripts are almost undetectable in unstressed cells and modestly increase after stress. Production of SatIII RNAs after hyper-osmotic stress depends on the Tonicity Element Binding Protein indicating that activation of the arrays is triggered by different transcription factors. This is the first example of a non-coding RNA whose transcription is controlled by different transcription factors under different growth conditions.

Published

2007

31. Cellular response to etoposide treatment

Author

Alessandra Montecucco and Giuseppe Biamonti

Subjects

DNA Replication, Cancer Research, DNA damage, DNA repair, Apoptosis, Biology, medicine, Animals, Humans, Topoisomerase II Inhibitors, Etoposide, Topoisomerase, Cell Cycle, DNA, Cell cycle, G2-M DNA damage checkpoint, Antineoplastic Agents, Phytogenic, Chromatin, Oncology, Cancer research, biology.protein, Topoisomerase-II Inhibitor, DNA Damage, medicine.drug

Abstract

Etoposide is a potent anti-tumor drug that belongs to the class of topoisomerase poisons. Although its molecular target, i.e. DNA topoisomerase II, has been identified more than 20 years ago, the cellular response to etoposide is still poorly understood. The cytotoxicity of the drug stems from its ability to stabilize a covalent complex between DNA topoisomerase II and DNA that results in a high level of DNA damage. Here, we review the present knowledge about the strategy used by the cells to deal with the etoposide-induced DNA damage. New and unanticipated effects of topoisomerase II poisoning on cell metabolism are recently emerging, among which the ability to activate cell cycle checkpoint pathways and to affect gene expression at different levels, including chromatin remodeling and alternative splicing of gene transcripts. The elucidation of the effects of etoposide on cell metabolism will increase our ability to exploit this drug in cancer therapy and will expand our comprehension of the cancerous cell.

Published

2007

32. Chronic Replication Problems Impact Cell Morphology and Adhesion of DNA Ligase I Defective Cells

Author

Alessandra Montecucco, Paolo Cremaschi, Matteo Oliverio, Roberta Carriero, Giulia Mazzucco, Silvia Bione, Andrea Palamidessi, Valentina Leva, Giorgio Scita, and Giuseppe Biamonti

Subjects

DNA Replication, DNA Ligases, DNA damage, DNA repair, Blotting, Western, lcsh:Medicine, Ataxia Telangiectasia Mutated Proteins, Biology, Cell morphology, Time-Lapse Imaging, Cell Line, DNA Ligase ATP, Cell Movement, Cell Adhesion, Humans, CHEK1, Phosphorylation, lcsh:Science, Cell adhesion, Cell Shape, Cell Line, Transformed, Multidisciplinary, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, lcsh:R, Cell Cycle, DNA replication, Cell cycle, G2-M DNA damage checkpoint, Fibroblasts, Cell biology, Microscopy, Fluorescence, Mutation, lcsh:Q, Research Article, DNA Damage

Abstract

Moderate DNA damage resulting from metabolic activities or sub-lethal doses of exogenous insults may eventually lead to cancer onset. Human 46BR.1G1 cells bear a mutation in replicative DNA ligase I (LigI) which results in low levels of replication-dependent DNA damage. This replication stress elicits a constitutive phosphorylation of the ataxia telangiectasia mutated (ATM) checkpoint kinase that fails to arrest cell cycle progression or to activate apoptosis or cell senescence. Stable transfection of wild type LigI, as in 7A3 cells, prevents DNA damage and ATM activation. Here we show that parental 46BR.1G1 and 7A3 cells differ in important features such as cell morphology, adhesion and migration. Comparison of gene expression profiles in the two cell lines detects Bio-Functional categories consistent with the morphological and migration properties of LigI deficient cells. Interestingly, ATM inhibition makes 46BR.1G1 more similar to 7A3 cells for what concerns morphology, adhesion and expression of cell-cell adhesion receptors. These observations extend the influence of the DNA damage response checkpoint pathways and unveil a role for ATM kinase activity in modulating cell biology parameters relevant to cancer progression.

Published

2015

33. Studies on the ATP Binding Site of Fyn Kinase for the Identification of New Inhibitors and Their Evaluation as Potential Agents against Tauopathies and Tumors

Author

Mirko Garbelli, Cristina Tintori, Emmanuele Crespan, Lorenzo Botta, Anna Lucia Fallacara, Federico Falchi, Lucia Dello Iacono, Silvia Schenone, Andrea Lossani, Giulia Vignaroli, Giuseppe Biamonti, Giuseppina La Sala, Tiziano Tuccinardi, Marco Radi, Chiara Brullo, Giovanni Maga, Donata Orioli, Maurizio Botta, Elena Dreassi, A. Desogus, Ilaria Laurenzana, Adriano Angelucci, Claudio Zamperini, Francesca Musumeci, and Francesca Gasparrini

Subjects

pyrazolo-pyrimidines, Models, Molecular, PROTEIN, TYROSINE KINASE, Proto-Oncogene Proteins c-fyn, Settore CHIM/06, T-CELL-ACTIVATION, Adenosine Triphosphate, Models, Neoplasms, Drug Discovery, Tumor Cells, Cultured, Phosphorylation, Cultured, biology, Molecular Structure, Kinase, Chemistry, Medicine (all), SRC-FAMILY KINASES, CANCER, Fyn inhibitors, Tumor Cells, ALZHEIMERS-DISEASE, Molecular Docking Simulation, Biochemistry, Tauopathies, Molecular Medicine, Signal transduction, Tyrosine kinase, Signal Transduction, Antineoplastic Agents, Binding Sites, Cell Proliferation, Humans, Protein Kinase Inhibitors, Pyrazoles, Pyrimidines, Structure-Activity Relationship, Drug Discovery3003 Pharmaceutical Science, AMBER FORCE-FIELD, Tau protein, anticancer agents, FYN, SRC-FAMILY KINASES, T-CELL-ACTIVATION, AMBER FORCE-FIELD, ALZHEIMERS-DISEASE, TYROSINE KINASE, IN-VITRO, BIOLOGICAL EVALUATION, CANCER, PROTEIN, BIOLOGICAL EVALUATION, Binding site, Fyn inhibitors, anticancer agents, pyrazolo-pyrimidines, Cell growth, Molecular, IN-VITRO, biology.protein

Abstract

Fyn is a member of the Src-family of nonreceptor protein-tyrosine kinases. Its abnormal activity has been shown to be related to various human cancers as well as to severe pathologies, such as Alzheimer's and Parkinson's diseases. Herein, a structure-based drug design protocol was employed aimed at identifying novel Fyn inhibitors. Two hits from commercial sources (1, 2) were found active against Fyn with K(i) of about 2 μM, while derivative 4a, derived from our internal library, showed a K(i) of 0.9 μM. A hit-to-lead optimization effort was then initiated on derivative 4a to improve its potency. Slightly modifications rapidly determine an increase in the binding affinity, with the best inhibitors 4c and 4d having K(i)s of 70 and 95 nM, respectively. Both compounds were found able to inhibit the phosphorylation of the protein Tau in an Alzheimer's model cell line and showed antiproliferative activities against different cancer cell lines.

Published

2015

34. The Dispersal of Replication Proteins after Etoposide Treatment Requires the Cooperation of Nbs1 with the Ataxia Telangiectasia Rad3-Related/Chk1 Pathway

Author

Samuela Soza, Alessandra Montecucco, Giuseppe Biamonti, Maria Rosa Lidonnici, and Rossella Rossi

Subjects

DNA Replication, Cancer Research, DNA Ligases, Cell Cycle Proteins, Eukaryotic DNA replication, Ataxia Telangiectasia Mutated Proteins, Protein Serine-Threonine Kinases, Biology, S Phase, DNA replication factor CDT1, DNA Ligase ATP, Replication factor C, Control of chromosome duplication, Proliferating Cell Nuclear Antigen, Replication Protein A, Humans, Replication protein A, S phase, Etoposide, DNA replication, Nuclear Proteins, Antineoplastic Agents, Phytogenic, Chromatin, Oncology, Checkpoint Kinase 1, Cancer research, biology.protein, Origin recognition complex, Protein Kinases, HeLa Cells

Abstract

In mammalian cells, DNA replication takes place in functional subnuclear compartments, called replication factories, where replicative factors accumulate. The distribution pattern of replication factories is diagnostic of the different moments (early, mid, and late) of the S phase. This dynamic organization is affected by different agents that induce cell cycle checkpoint activation via DNA damage or stalling of replication forks. Here, we explore the cell response to etoposide, an anticancer drug belonging to the topoisomerase II poisons. Etoposide does not induce an immediate block of DNA synthesis and progressively affects the distribution of replication proteins in S phase. First, it triggers the formation of large nuclear foci that contain the single-strand DNA binding protein replication protein A (RPA), suggesting that lesions produced by the drug are processed into extended single-stranded regions. These RPA foci colocalize with DNA replicated at the beginning of the treatment. Etoposide also triggers the dispersal of replicative proteins, proliferating cell nuclear antigen and DNA ligase I, from replication factories. This event requires the activity of the ataxia telangiectasia Rad3-related (ATR) checkpoint kinase. By comparing the effect of the drug in cell lines defective in different DNA repair and checkpoint pathways, we show that, along with the downstream kinase Chk1, the Nbs1 protein, mutated in the Nijmegen breakage syndrome, is also relevant for this response and for ATR-dependent phosphorylation. Finally, our analysis evidences a critical role of Nbs1 in the etoposide-induced inhibition of DNA replication in early S phase. (Cancer Res 2006; 66(3): 1675-83)

Published

2006

35. Cell Motility Is Controlled by SF2/ASF through Alternative Splicing of the Ron Protooncogene

Author

Silvano Riva, Fabio Castiglioni, Paolo M. Comoglio, Michael R. Green, Silvia Giordano, Haihong Shen, Giuseppe Biamonti, Federica Benvenuto, and Claudia Ghigna

Subjects

Motility, Breast Neoplasms, Biology, Receptor tyrosine kinase, Splicing factor, Exon, Cell Movement, Cell Line, Tumor, Humans, Protein Isoforms, Tissue Distribution, RNA, Messenger, Enhancer, Molecular Biology, Gene knockdown, Serine-Arginine Splicing Factors, Alternative splicing, Nuclear Proteins, RNA-Binding Proteins, Receptor Protein-Tyrosine Kinases, Exons, Cell Biology, Molecular biology, Alternative Splicing, Enhancer Elements, Genetic, Gene Expression Regulation, RNA splicing, Colonic Neoplasms, biology.protein, Female, RNA Interference

Abstract

Ron, the tyrosine kinase receptor for the Macrophage-stimulating protein, is involved in cell dissociation, motility, and matrix invasion. DeltaRon, a constitutively active isoform that confers increased motility to expressing cells, is generated through the skipping of exon 11. We show that abnormal accumulation of DeltaRon mRNA occurs in breast and colon tumors. Skipping of exon 11 is controlled by a silencer and an enhancer of splicing located in the constitutive exon 12. The strength of the enhancer parallels the relative abundance of DeltaRon mRNA and depends on a sequence directly bound by splicing factor SF2/ASF. Overexpression and RNAi experiments demonstrate that SF2/ASF, by controlling the production of DeltaRon, activates epithelial to mesenchymal transition leading to cell locomotion. The effect of SF2/ASF overexpression is reverted by specific knockdown of DeltaRon mRNA. This demonstrates a direct link between SF2/ASF-regulated splicing and cell motility, an activity important for embryogenesis, tissue formation, and tumor metastasis.

Published

2005

36. Structural and Functional Characterization of Noncoding Repetitive RNAs Transcribed in Stressed Human Cells

Author

Silvano Riva, Fabio Cobianchi, Ilaria Chiodi, Manuela Giordano, Giuseppe Biamonti, and Rut Valgardsdottir

Subjects

RNA, Untranslated, Transcription, Genetic, Euchromatin, RNA-induced silencing complex, Heterochromatin, Eukaryotic Initiation Factor-2, Down-Regulation, DNA, Satellite, Biology, Cell Fusion, Mice, Heat Shock Transcription Factors, Peptide Initiation Factors, Stress, Physiological, medicine, Animals, Humans, RNA-Induced Silencing Complex, RNA, Small Interfering, Small nucleolar RNA, Molecular Biology, Cell Nucleus, Genetics, Dose-Response Relationship, Drug, Sequence Analysis, RNA, RNA, Articles, Cell Biology, Oligonucleotides, Antisense, Argonaute, Cell Nucleus Structures, Coculture Techniques, Long non-coding RNA, DNA-Binding Proteins, Cell nucleus, medicine.anatomical_structure, Argonaute Proteins, NIH 3T3 Cells, Heat-Shock Response, HeLa Cells, Transcription Factors

Abstract

Thermal and chemical stresses induce the formation in human cells of novel and transient nuclear structures called nuclear stress bodies (nSBs). These contain heat shock factor 1 (HSF-1) and a specific subset of pre-mRNA processing factors. Nuclear stress bodies are assembled on specific pericentromeric heterochromatic domains containing satellite III (SatIII) DNA. In response to stress, these domains change their epigenetic status from heterochromatin to euchromatin and are transcribed in poly-adenylated RNAs that remain associated with nSBs. In this article, we describe the cloning, sequencing, and functional characterization of these transcripts. They are composed of SatIII repeats and originate from the transcription of multiple sites within the SatIII arrays. Interestingly, the level of SatIII RNAs can be down-regulated both by antisense oligonucleotides and small interfering RNAs (siRNA). Knockdown of SatIII RNA by siRNAs requires the activity of Argonaute 2, a component of the RNA-induced silencing complex. Down-regulation of satellite III RNAs significantly affects the recruitment of RNA processing factors to nSBs without altering the association of HSF-1 with these structures nor the presence of acetylated histones within nSBs. Thus, satellite III RNAs have a major role in the formation of nSBs.

Published

2005

37. Nuclear stress bodies: a heterochromatin affair?

Author

Giuseppe Biamonti

Subjects

Genetics, Regulation of gene expression, Heterochromatin, Cell Biology, Biology, Molecular Biology, Chromatin, Nuclear function, Cell biology

Abstract

It is still largely unknown how the various nuclear subcompartments are formed, why they form in particular locations and how they are linked to nuclear function. Nuclear stress bodies provide a new opportunity to address these questions and to test models of self-organization of nuclear structures. The assembly of these bodies requires the synthesis of non-coding RNAs with a probable role in the post-transcriptional regulation of gene expression and in higher-order chromatin organization.

Published

2004

38. A single polypyrimidine tract binding protein (PTB) binding site mediates splicing inhibition at mouse IgM exons M1 and M2

Author

Haihong Shen, Giuseppe Biamonti, Michael R. Green, Claudia Ghigna, and Julie L.C. Kan

Subjects

Binding Sites, Alternative splicing, Exonic splicing enhancer, Intron, Down-Regulation, Biology, Molecular biology, Alternative Splicing, Mice, Exon, Enhancer Elements, Genetic, Gene Expression Regulation, Immunoglobulin M, Polypyrimidine tract, Protein splicing, Report, RNA splicing, RNA Precursors, biology.protein, Animals, RNA, Messenger, Polypyrimidine tract-binding protein, Molecular Biology, Polypyrimidine Tract-Binding Protein

Abstract

Splicing of mouse immunoglobulin (IgM) exons M1 and M2 is directed by two juxtaposed regulatory elements, an enhancer and an inhibitor, located within the M2 exon. A primary function of the enhancer is to counteract the inhibitor, allowing splicing to occur. Here we show that the inhibitor contains two binding sites for polypyrimidine tract binding protein (PTB). Mutational analysis indicates that only one of these sites is necessary and sufficient to direct splicing inhibition both in vitro and in vivo. We demonstrate that the difference in activity of the two sites is explained by proximity to the intron. We further show that the presence of the enhancer results in the disruption of the PTB-inhibitor interaction, enabling splicing to occur. In the absence of the enhancer, splicing can be artificially activated by immuno-inhibition of PTB. Collectively, our results indicate that a single PTB binding site can function as an inhibitor that regulates alternative splicing both in vitro and in vivo.

Published

2004

39. Transcriptional Activation of a Constitutive Heterochromatic Domain of the Human Genome in Response to Heat Shock

Author

Margherita Corioni, Marco Denegri, Rut Valgardsdottir, Giuseppe Biamonti, Silvano Riva, Ilaria Chiodi, Fabio Cobianchi, and Nicoletta Rizzi

Subjects

Transcriptional Activation, Euchromatin, Heterochromatin, Heat Stroke, Methylation, Histones, Histone H3, medicine, Humans, Constitutive heterochromatin, Hepatocyte Nuclear Factor 1-alpha, Molecular Biology, Cell Nucleus, Genetics, biology, Genome, Human, Nuclear Proteins, Acetylation, Articles, Cell Biology, DNA-Binding Proteins, Cell nucleus, Histone, medicine.anatomical_structure, Hepatocyte Nuclear Factor 1, biology.protein, RNA, Human genome, Heterochromatin protein 1, Chromosomes, Human, Pair 9, HeLa Cells, Transcription Factors

Abstract

Heat shock triggers the assembly of nuclear stress bodies that contain heat shock factor 1 and a subset of RNA processing factors. These structures are formed on the pericentromeric heterochromatic regions of specific human chromosomes, among which chromosome 9. In this article we show that these heterochromatic domains are characterized by an epigenetic status typical of euchromatic regions. Similarly to transcriptionally competent portions of the genome, stress bodies are, in fact, enriched in acetylated histone H4. Acetylation peaks at 6 h of recovery from heat shock. Moreover, heterochromatin markers, such as HP1 and histone H3 methylated on lysine 9, are excluded from these nuclear districts. In addition, heat shock triggers the transient accumulation of RNA molecules, heterogeneous in size, containing the subclass of satellite III sequences found in the pericentromeric heterochromatin of chromosome 9. This is the first report of a transcriptional activation of a constitutive heterochromatic portion of the genome in response to stress stimuli.

Published

2004

40. Cell Cycle-dependent Phosphorylation of Human DNA Ligase I at the Cyclin-dependent Kinase Sites

Author

Daniele Arosio, Giovanni Ferrari, Alessandra Montecucco, Giuseppe Biamonti, Alessandro Vindigni, and Rossella Rossi

Subjects

DNA Replication, inorganic chemicals, DNA Ligases, Amino Acid Motifs, Molecular Sequence Data, Eukaryotic DNA replication, Biology, environment and public health, Biochemistry, DNA Ligase ATP, Cyclin-dependent kinase, Cyclins, Proliferating Cell Nuclear Antigen, Humans, Protein phosphorylation, Amino Acid Sequence, Phosphorylation, Molecular Biology, chemistry.chemical_classification, DNA ligase, Binding Sites, Cell Cycle, Cyclin-dependent kinase 2, Cell Biology, Cell cycle, Cyclin-Dependent Kinases, enzymes and coenzymes (carbohydrates), chemistry, biology.protein, bacteria, Origin recognition complex, Casein kinase 2

Abstract

We have described previously that, during S-phase, human DNA ligase I is phosphorylated on Ser66, a casein kinase II site. Here we investigate the phosphorylation status of DNA ligase I during the cell cycle by gel shift analysis and electrospray mass spectrometry. We show that three residues (Ser51, Ser76, and Ser91), which are part of cyclin-dependent kinase sites, are phosphorylated in a cell cycle-dependent manner. Phosphorylation of Ser91 occurs at G1/S transition and depends on a cyclin binding site in the C-terminal part of the protein. This modification is required for the ensuing phosphorylation of Ser76 detectable in G2/M extracts. The substitution of serines at positions 51, 66, 76, and 91 with aspartic acid to mimic the phosphorylated enzyme hampers the association of DNA ligase I with the replication foci. We suggest that the phosphorylation of DNA ligase I and possibly other replicative enzymes is part of the mechanism that directs the disassembly of the replication machinery at the completion of S-phase.

Published

2003

41. [Untitled]

Author

Arturo Falaschi, Sónia Paixão, Fiorenzo A. Peverali, Alessandra Montecucco, Silvano Riva, and Giuseppe Biamonti

Subjects

Genetics, DNA re-replication, DNA replication factor CDT1, Control of chromosome duplication, DNA replication, biology.protein, Origin recognition complex, Eukaryotic DNA replication, Biology, Pre-replication complex, DNA replication origin, Cell biology

Abstract

DNA replication occupies a central position in the cell cycle and, therefore, in the development and life of multicellular organisms. During the last 10 years, our comprehension of this important process has considerably improved. Although the mechanisms that coordinate DNA replication with the other moments of the cell cycle are not yet fully understood, it is known that they mainly operate through DNA replication origins and the protein complexes bound to them. In eukaryotes, the packaging status of chromatin seems to be part of the mechanism that controls whether or not and when during the S-phase a particular origin will be activated. Intriguingly, the protein complexes bound to DNA replication origins appear to be directly involved in controlling chromatin packaging. In this manner they can also affect gene expression. In this review we focus on DNA replication origins in metazoan cells and on the relationship between these elements and the structural and functional organization of the genome.

Published

2003

42. DNA-protein interaction dynamics at the Lamin B2 replication origin

Author

Fiorenzo A. Peverali, Luca Puzzi, Laura Marchetti, Mauro Giacca, Giuseppe Biamonti, Puzzi, Luca, Marchetti, Laura, Peverali, Fiorenzo A., Biamonti, Giuseppe, and Giacca, Mauro

Subjects

Proto-Oncogene Proteins c-jun, Origin Recognition Complex, Eukaryotic DNA replication, Pre-replication complex, HeLa Cell, DNA replication origin, Topoisomerase II Inhibitor, Mitochondrial Membrane Transport Proteins, DNA replication factor CDT1, Mitochondrial Precursor Protein Import Complex Proteins, Topoisomerase II Inhibitors, Promoter Regions, Genetic, Genetics, AP-1, Fos, Jun, Origin recognition complex, Transcription factor, Cell Line, Tumor, DNA, DNA Replication, G1 Phase, HeLa Cells, Homeodomain Proteins, Humans, Immunoprecipitation, Lamin Type B, Protein Binding, Proto-Oncogene Proteins c-fos, Replication Origin, Thiobarbiturates, Transcription Factor AP-1, Upstream Stimulatory Factors, Molecular Biology, Developmental Biology, Cell Biology, Tumor, biology, Homeodomain Protein, Fo, Thiobarbiturate, Human, Proto-Oncogene Proteins c-fo, Upstream Stimulatory Factor, Cell Line, Promoter Regions, Control of chromosome duplication, Genetic, DNA replication, Mitochondrial Membrane Transport Protein, Licensing factor, biology.protein, Reports

Abstract

To date, a complete understanding of the molecular events leading to DNA replication origin activation in mammalian cells still remains elusive. In this work, we report the results of a high resolution chromatin immunoprecipitation study to detect proteins interacting with the human Lamin B2 replication origin. In addition to the pre-RC component ORC4 and to the transcription factors USF and HOXC13, we found that 2 components of the AP-1 transcription factor, c-Fos and c-Jun, are also associated with the origin DNA during the late G1 phase of the cell cycle and that these factors interact with ORC4. Both DNA replication and AP-1 factor binding to the origin region were perturbed by cell treatment with merbarone, a topoisomerase II inhibitor, suggesting that DNA topology is essential for determining origin function.

Published

2015

43. The alternative splicing factor Nova2 regulates vascular development and lumen formation

Author

Claudia Ghigna, Stefania Gallo, Carla Taveggia, Federica Pisati, Elisabetta Ferrero, Elisa Belloni, Gianluca Deflorian, Valeria Quaranta, Fabrizio Orsenigo, Benjamin J. Blencowe, Serena Bonomi, Christopher D. R. Wyatt, Daniel Nyqvist, Pier Paolo Di Fiore, Costanza Giampietro, Stefano Confalonieri, Anna Di Matteo, Elisabetta Dejana, Giuseppe Biamonti, Manuel Irimia, Davide Pradella, Giovanni Bertalot, and Evelien Fredrickx

Subjects

Endothelium, Angiogenesis, Regulator, General Physics and Astronomy, Lumen (anatomy), Neovascularization, Physiologic, RNA-binding protein, Biology, Neurones -- Fisiologia, General Biochemistry, Genetics and Molecular Biology, Article, Neovascularization, Exon, Mice, Antigens, Neoplasm, Neuro-Oncological Ventral Antigen, medicine, Animals, Cardiac and Cardiovascular Systems, Cells, Cultured, Multidisciplinary, Kardiologi, Alternative splicing, Endothelial Cells, RNA-Binding Proteins, General Chemistry, Anatomy, Cell biology, Angiogènesi, Alternative Splicing, medicine.anatomical_structure, Endothelium, Vascular, medicine.symptom

Abstract

Vascular lumen formation is a fundamental step during angiogenesis; yet, the molecular mechanisms underlying this process are poorly understood. Recent studies have shown that neural and vascular systems share common anatomical, functional and molecular similarities. Here we show that the organization of endothelial lumen is controlled at the post-transcriptional level by the alternative splicing (AS) regulator Nova2, which was previously considered to be neural cell-specific. Nova2 is expressed during angiogenesis and its depletion disrupts vascular lumen formation in vivo. Similarly, Nova2 depletion in cultured endothelial cells (ECs) impairs the apical distribution and the downstream signalling of the Par polarity complex, resulting in altered EC polarity, a process required for vascular lumen formation. These defects are linked to AS changes of Nova2 target exons affecting the Par complex and its regulators. Collectively, our results reveal that Nova2 functions as an AS regulator in angiogenesis and is a novel member of the ‘angioneurins' family., The alternative splicing factor Nova2 is best known for its pivotal function in the brain. Giampietro et al. reveal an important role for Nova2 in the regulation of alternative splicing of transcripts in the vascular endothelium that are crucial for the maintenance of endothelial cell polarity and vessel lumen formation in zebrafish.

Published

2015

44. Human Chromosomes 9, 12, and 15 Contain the Nucleation Sites of Stress-Induced Nuclear Bodies

Author

Silvano Riva, Fabio Cobianchi, Giuseppe Biamonti, Marco Biggiogera, Mariano Rocchi, Luigi De Carli, Daniela Moralli, Marco Denegri, and Elena Raimondi

Subjects

Nucleolus, Heterochromatin, Mitosis, Hamster, Chromosome 9, Biology, Transfection, Article, Cell Line, Mice, Cricetinae, Chlorocebus aethiops, medicine, Animals, Humans, Fluorescent Antibody Technique, Indirect, Molecular Biology, Cell Nucleus, Chromosomes, Human, Pair 15, Chromosomes, Human, Pair 12, medicine.diagnostic_test, 3T3 Cells, Cell Biology, Molecular biology, Microscopy, Electron, Cell nucleus, medicine.anatomical_structure, COS Cells, Stress, Mechanical, Chromosomes, Human, Pair 9, HeLa Cells, Fluorescence in situ hybridization

Abstract

We previously reported the identification of a novel nuclear compartment detectable in heat-shocked HeLa cells that we termed stress-induced Src-activated during mitosis nuclear body (SNB). This structure is the recruitment center for heat shock factor 1 and for a number of RNA processing factors, among a subset of Serine-Arginine splicing factors. In this article, we show that stress-induced SNBs are detectable in human but not in hamster cells. By means of hamster>human cell hybrids, we have identified three human chromosomes (9, 12, and 15) that are individually able to direct the formation of stress bodies in hamster cells. Similarly to stress-induced SNB, these bodies are sites of accumulation of hnRNP A1-interacting protein and heat shock factor 1, are usually associated to nucleoli, and consist of clusters of perichromatin granules. We show that the p13-q13 region of human chromosome 9 is sufficient to direct the formation of stress bodies in hamster>human cell hybrids. Fluorescence in situ hybridization experiments demonstrate that the pericentromeric heterochromatic q12 band of chromosome 9 and the centromeric regions of chromosomes 12 and 15 colocalize with stress-induced SNBs in human cells. Our data indicate that human chromosomes 9, 12, and 15 contain the nucleation sites of stress bodies in heat-shocked HeLa cells.

Published

2002

45. hnRNP L inhibits CD44 V10 exon splicing through interacting with its upstream intron

Author

Il Chul Kim, Sunghee Cho, Tiing Jen Loh, Xuexiu Zheng, Da-Woon Jung, Heegyum Moon, Haihong Shen, Claudia Ghigna, Giuseppe Biamonti, Darren R. Williams, and Ha Na Jang

Subjects

RNA Splicing, Biophysics, Exonic splicing enhancer, Endogeny, environment and public health, Biochemistry, Exon, Heterogeneous-Nuclear Ribonucleoprotein L, Structural Biology, Genetics, Cell Adhesion, Humans, Molecular Biology, biology, Chemistry, CD44, Alternative splicing, Intron, Nuclear Proteins, Exons, Splicing Factor U2AF, Molecular biology, Introns, Hyaluronan Receptors, Gene Expression Regulation, Ribonucleoproteins, RNA splicing, biology.protein, Mutation testing, HeLa Cells

Abstract

CD44 is a complex cell adhesion molecule that mediates communication and adhesion between adjacent cells as well as between cells and the extracellular matrix. CD44 pre-mRNA produces various mRNA isoforms through alternative splicing of 20 exons, among which exons 1–5 (C 1 –C 5 ) and 16–20 (C 6 –C 10 ) are constant exons, whereas exons 6–15 (V 1 –V 10 ) are variant exons. CD44 V 10 exon has important roles in breast tumor progression and Hodgkin lymphoma. Here we show that increased expression of hnRNP L inhibits V 10 exon splicing of CD44 pre-mRNA, whereas reduced expression of hnRNP L promotes V 10 exon splicing. In addition, hnRNP L also promotes V 10 splicing of endogenous CD44 pre-mRNA. Through mutation analysis, we demonstrate that the effects of hnRNP L on V 10 splicing are abolished when the CA-rich sequence on the upstream intron of V 10 exon is disrupted. However, hnRNP L effects are stronger if more CA-repeats are provided. Furthermore, we show that hnRNP L directly contacts the CA-rich sequence. Importantly, we provide evidences that hnRNP L inhibits U2AF 65 binding on the upstream Py tract of V 10 exon. Our results reveal that hnRNP L is a new regulator for CD44 V 10 exon splicing.

Published

2014

46. SRSF2 promotes splicing and transcription of exon 11 included isoform in Ron proto-oncogene

Author

Heegyum Moon, Claudia Ghigna, Haihong Shen, Giuseppe Biamonti, Young Soo Kwon, Sunghee Cho, Tiing Jen Loh, Jianhua Zhou, D. Joshua Liao, Michael R. Green, Xuexiu Zheng, Ha Na Jang, Hyun Kyung Oh, Soo Hyun Eom, and Youngsoo Jun

Subjects

Transcription, Genetic, RNA Splicing, Biophysics, Exonic splicing enhancer, Biology, Biochemistry, Proto-Oncogene Mas, Article, Exon, Structural Biology, Transcription (biology), Proto-Oncogenes, Genetics, Humans, Nuclear protein, Molecular Biology, Cells, Cultured, Ribonucleoprotein, Splice site mutation, Serine-Arginine Splicing Factors, Intron, Nuclear Proteins, Receptor Protein-Tyrosine Kinases, Exons, Molecular biology, Isoenzymes, Ribonucleoproteins, RNA splicing, HeLa Cells

Abstract

The product of proto-oncogene Ron is a human receptor for the macrophage-stimulating protein (MSP). Upon activation, Ron is able to induce cell dissociation, migration and matrix invasion. Exon 11 skipping of Ron pre-mRNA produces Ron△165 protein that is constitutively active even in the absence of its ligand. Here we show that knockdown of SRSF2 promotes the decrease of exon 11 inclusion, whereas overexpression of SRSF2 promotes exon 11 inclusion. We demonstrate that SRSF2 promotes exon 11 inclusion through splicing and transcription procedure. We also present evidence that reduced expression of SRSF2 induces a decrease in the splicing of both introns 10 and 11; by contrast, overexpression of SRSF2 induces an increase in the splicing of introns 10 and 11. Through mutation analysis, we show that SRSF2 functionally targets and physically interacts with CGAG sequence on exon 11. In addition, we reveal that the weak strength of splice sites of exon 11 is not required for the function of SRSF2 on the splicing of Ron exon 11. Our results indicate that SRSF2 promotes exon 11 inclusion of Ron proto-oncogene through targeting exon 11. Our study provides a novel mechanism by which Ron is expressed.

Published

2014

47. Molecular mechanisms of etoposide

Author

Alessandra, Montecucco, Francesca, Zanetta, and Giuseppe, Biamonti

Subjects

Review Article

Abstract

Etoposide derives from podophyllotoxin, a toxin found in the American Mayapple. It was first synthesized in 1966 and approved for cancer therapy in 1983 by the U.S. Food and Drug Administration (Hande, 1998[25]). Starting from 1980s several studies demonstrated that etoposide targets DNA topoisomerase II activities thus leading to the production of DNA breaks and eliciting a response that affects several aspects of cell metabolisms. In this review we will focus on molecular mechanisms that account for the biological effect of etoposide.

Published

2014

48. Stress-induced Nuclear Bodies Are Sites of Accumulation of Pre-mRNA Processing Factors

Author

Margherita Corioni, Giuseppe Biamonti, Ilaria Chiodi, Fabio Cobianchi, Silvano Riva, and Marco Denegri

Subjects

Nucleocytoplasmic Transport Proteins, Heterogeneous nuclear ribonucleoprotein, Heterogeneous Nuclear Ribonucleoprotein A1, RNA Splicing, Recombinant Fusion Proteins, RNA-binding protein, Biology, Heterogeneous ribonucleoprotein particle, Article, Heterogeneous-Nuclear Ribonucleoproteins, stomatognathic system, Heterogeneous-Nuclear Ribonucleoprotein Group A-B, RNA Precursors, medicine, Humans, RNA, Messenger, Nuclear protein, Molecular Biology, Adaptor Proteins, Signal Transducing, Ribonucleoprotein, Cell Nucleus, Binding Sites, Serine-Arginine Splicing Factors, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Phosphoproteins, Molecular biology, Cell biology, DNA-Binding Proteins, Cell nucleus, medicine.anatomical_structure, Ribonucleoproteins, RNA splicing, Adenovirus E1A Proteins, Heat-Shock Response, HeLa Cells

Abstract

Heterogeneous nuclear ribonucleoprotein (hnRNP) HAP (hnRNP A1 interacting protein) is a multifunctional protein with roles in RNA metabolism, transcription, and nuclear structure. After stress treatments, HAP is recruited to a small number of nuclear bodies, usually adjacent to the nucleoli, which consist of clusters of perichromatin granules and are depots of transcripts synthesized before stress. In this article we show that HAP bodies are sites of accumulation for a subset of RNA processing factors and are related to Sam68 nuclear bodies (SNBs) detectable in unstressed cells. Indeed, HAP and Sam68 are both present in SNBs and in HAP bodies, that we rename “stress-induced SNBs.” The determinants required for the redistribution of HAP lie between residue 580 and 788. Different portions of this region direct the recruitment of the green fluorescent protein to stress-induced SNBs, suggesting an interaction of HAP with different components of the bodies. With the use of the 580–725 region as bait in a two-hybrid screening, we have selected SRp30c and 9G8, two members of the SR family of splicing factors. Splicing factors are differentially affected by heat shock: SRp30c and SF2/ASF are efficiently recruited to stress-induced SNBs, whereas the distribution of SC35 is not perturbed. We propose that the differential sequestration of splicing factors could affect processing of specific transcripts. Accordingly, the formation of stress-induced SNBs is accompanied by a change in the splicing pattern of the adenovirus E1A transcripts.

Published

2001

49. Selection of homeotic proteins for binding to a human DNA replication origin 1 1Edited by M. Yaniv

Author

Paolo Norio, Fiorenzo A. Peverali, Silvano Riva, Mauro Giacca, Giuseppe Biamonti, Arturo Falaschi, Davide Gabellini, and Elisa de Stanchina

Subjects

Genetics, Open reading frame, Structural Biology, Three prime untranslated region, Biology, Drosophila melanogaster, biology.organism_classification, Molecular Biology, Gene, DNA replication origin, Footprinting, Lamin, Nucleoprotein

Abstract

We have previously shown that a cell cycle-dependent nucleoprotein complex assembles in vivo on a 74 bp sequence within the human DNA replication origin associated to the Lamin B2 gene. Here, we report the identification, using a one-hybrid screen in yeast, of three proteins interacting with the 74 bp sequence. All of them, namely HOXA13, HOXC10 and HOXC13, are orthologues of the Abdominal-B gene of Drosophila melanogaster and are members of the homeogene family of developmental regulators. We describe the complete open reading frame sequence of HOXC10 and HOXC13 along with the structure of the HoxC13 gene. The specificity of binding of these two proteins to the Lamin B2 origin is confirmed by both band-shift and in vitro footprinting assays. In addition, the ability of HOXC10 and HOXC13 to increase the activity of a promoter containing the 74 bp sequence, as assayed by CAT-assay experiments, demonstrates a direct interaction of these homeoproteins with the origin sequence in mammalian cells. We also show that HOXC10 expression is cell-type-dependent and positively correlates with cell proliferation.

Published

2000

50. Alternative splicing of tumor suppressors and oncogenes

Author

Claudia, Ghigna, Silvano, Riva, and Giuseppe, Biamonti

Subjects

Alternative Splicing, Neoplasms, Mutation, RNA Precursors, Humans, Signal Transduction

Abstract

Alternative splicing is a fundamental mechanism to modulate gene expression programs in response to different growth and environmental stimuli. There is now ample evidence that alternative splicing errors, caused by mutations in cis-acting elements and defects and/or imbalances in trans-acting factors, may be causatively associated to cancer progression. Recent work indicates the existence of an intricate network of interactions between alternative splicing events and signal transduction pathways. In this network, splicing factors occupy a central position and appear to function both as targets and effectors of regulatory circuits. Thus, a change in their activity deeply affects alternative splicing profiles and hence the cell behavior. Here, we discuss a number of cases that exemplify the involvement of deregulated alternative splicing in tumor progression.

Published

2013