Your search keyword '"Calzari L"' showing total 10 results

1. Follicular Lymphoma Microenvironment Traits Associated with Event-Free Survival

Author

Tumedei, MM, Piccinini, F, Azzali, I, Pirini, F, Bravaccini, S, De Matteis, S, Agostinelli, C, Castellani, G, Zanoni, M, Cortesi, M, Vergani, B, Leone, BE, Righi, S, Gazzola, A, Casadei, B, Gentilini, D, Calzari, L, Limarzi, F, Sabattini, E, Pession, A, Tazzari, M, Bertuzzi, C, Tumedei, M, Piccinini, F, Azzali, I, Pirini, F, Bravaccini, S, De Matteis, S, Agostinelli, C, Castellani, G, Zanoni, M, Cortesi, M, Vergani, B, Leone, B, Righi, S, Gazzola, A, Casadei, B, Gentilini, D, Calzari, L, Limarzi, F, Sabattini, E, Pession, A, Tazzari, M, and Bertuzzi, C

Subjects

Follicular Lymphoma, immunohistochemistry, tumor microenvironment, progressive disease, tumor-associated macrophages, digital pathology

Abstract

The majority of patients with Follicular Lymphoma (FL) experience subsequent phases of remission and relapse, making the disease "virtually" incurable. To predict the outcome of FL patients at diagnosis, various clinical-based prognostic scores have been proposed; nonetheless, they continue to fail for a subset of patients. Gene expression profiling has highlighted the pivotal role of the tumor microenvironment (TME) in the FL prognosis; nevertheless, there is still a need to standardize the assessment of immune-infiltrating cells for the prognostic classification of patients with early or late progressing disease. We studied a retrospective cohort of 49 FL lymph node biopsies at the time of the initial diagnosis using pathologist-guided analysis on whole slide images, and we characterized the immune repertoire for both quantity and distribution (intrafollicular, IF and extrafollicular, EF) of cell subsets in relation to clinical outcome. We looked for the natural killer (CD56), T lymphocyte (CD8, CD4, PD1) and macrophage (CD68, CD163, MA4A4A)-associated markers. High CD163/CD8 EF ratios and high CD56/MS4A4A EF ratios, according to Kaplan-Meier estimates were linked with shorter EFS (event-free survival), with the former being the only one associated with POD24. In contrast to IF CD68+ cells, which represent a more homogeneous population, higher in non-progressing patients, EF CD68+ macrophages did not stratify according to survival. We also identify distinctive MS4A4A+CD163-macrophage populations with different prognostic weights. Enlarging the macrophage characterization and combining it with a lymphoid marker in the rituximab era, in our opinion, may enable prognostic stratification for low-/high-grade FL patients beyond POD24. These findings warrant validation across larger FL cohorts.

Published

2023

2. Transcriptome Analysis of iPSC-Derived Neurons from Rubinstein-Taybi Patients Reveals Deficits in Neuronal Differentiation

Author

Calzari L, Barcella M, Alari V, Braga D, Munoz-Viana R, Barlassina C, Finelli P, Gervasini C, Barco A, Russo S, and Larizza L

Subjects

iNeurons, Defective transcriptional program, Neuronal differentiation, iPSC-derived neural progenitors, Rubinstein Taybi, Intellectual disability, RNA-Seq

Abstract

Rubinstein-Taybi syndrome (RSTS) is a rare multisystem developmental disorder with moderate to severe intellectual disability caused by heterozygous mutations of eitherCREBBPorEP300genes encoding CBP/p300 chromatin regulators. We explored the gene programs and processes underlying the morphological and functional alterations shown by iPSC-derived neurons modeling RSTS to bridge the molecular changes resulting from defective CBP/p300 to cognitive impairment. By global transcriptome analysis, we compared the differentially expressed genes (DEGs) marking the transition from iPSC-derived neural progenitors to cortical neurons (iNeurons) of five RSTS patients carrying privateCREBBP/EP300mutations and manifesting differently graded neurocognitive signs with those of four healthy controls. Our data shows a defective and altered neuroprogenitor to neuron transcriptional program in the cells from RSTS patients. First, transcriptional regulation is weaker in RSTS as less genes than in controls are modulated, including genes of key processes of mature functional neurons, such as those for voltage-gated channels and neurotransmitters and their receptors. Second, regulation is subverted as genes acting at pre-terminal stages of neural differentiation in cell polarity and adhesive functions (members of the cadherin family) and axon extension/guidance (members of the semaphorins and SLIT receptors families) are improperly upregulated. Impairment or delay of RSTS neuronal differentiation program is also evidenced by decreased modulation of the overall number of neural differentiation markers, significantly impacting the initial and final stages of the differentiation cascade. Last, extensive downregulation of genes for RNA/DNA metabolic processes confirms that RSTS is a global transcription disorder, consistent with a syndrome driven by chromatin dysregulation. Interestingly, the morphological and functional alterations we have previously appointed as biomarkers of RSTS iNeurons provide functional support to the herein designed transcriptome profile pointing to key dysregulated neuronal genes as main contributors to patients' cognitive deficit. The impact of RSTS transcriptome may go beyond RSTS as comparison of dysregulated genes across modeled neurodevelopmental disorders could unveil convergent genes of cognitive impairment.

Published

2020

3. Involvement of the yeast metacaspase Yca1 in ubp10Delta-programmed cell death

Author

BETTIGA, MAURIZIO, ORLANDI, IVAN, ALBERGHINA, LILIA, VAI, MARINA, Calzari, L, Bettiga, M, Calzari, L, Orlandi, I, Alberghina, L, and Vai, M

Subjects

Saccharomyces cerevisiae Proteins, Nuclear Proteins, Apoptosis, Ascorbic Acid, Saccharomyces cerevisiae, Spheroplasts, BIO/11 - BIOLOGIA MOLECOLARE, Flow Cytometry, Recombinant Proteins, Mutagenesis, Insertional, apoptosis, deubiquitinating enzyme, metacaspase,ascorbic acid, Microscopy, Fluorescence, Caspases, Gene Expression Regulation, Fungal, DNA, Fungal, Reactive Oxygen Species, Ubiquitin Thiolesterase

Abstract

UBP10 encodes a deubiquitinating enzyme of Saccharomyces cerevisiae. Its inactivation results in a complex phenotype characterized by a subpopulation of cells that exhibits the typical cellular markers of apoptosis. Here, we show that additional deletion of YCA1, coding for the yeast metacaspase, suppressed the ubp10 disruptant phenotype. Moreover, YCA1 overexpression, without any external stimulus, had a detrimental effect on growth and viability of ubp10 cells accompanied by an increase of apoptotic cells. This response was completely abrogated by ascorbic acid addition. We also observed that cells lacking UBP10 had an endogenous caspase activity, revealed by incubation in vivo with FITC-labeled VAD-fmk. All these results argue in favour of an involvement of the yeast metacaspase in the active cell death triggered by loss of UBP10 function. © 2004 Federation of European Microbiological Societies. Published by Elsevier B.V. All rights reserved.

Published

2004

4. Stochastic epigenetic mutations as possible explanation for phenotypical discordance among twins with congenital hypothyroidism

Author

D. Gentilini, M. Muzza, T. de Filippis, M. C. Vigone, G. Weber, L. Calzari, A. Cassio, M. Di Frenna, M. Bartolucci, E. S. Grassi, E. Carbone, A. Olivieri, L. Persani, Gentilini, D, Muzza, M, de Filippis, T, Vigone, M C, Weber, G, Calzari, L, Cassio, A, Di Frenna, M, Bartolucci, M, Grassi, E S, Carbone, E, Olivieri, A, and Persani, L

Subjects

Thyroid, Congenital disease, Endocrinology, Congenital diseases, Endocrinology, Diabetes and Metabolism, Genome-wide DNA methylation, Preterm delivery, Thyroid dysgenesis, Thyroid dysgenesi, Twin gestation, Settore MED/13 - Endocrinologia

Abstract

Purpose The elevated frequency of discordance for congenital hypothyroidism (CH) phenotype between monozygotic twins suggests the involvement of non-mendelian mechanisms. The aim of the study was to investigate the role of epigenetics in CH pathogenesis. Methods A genome-wide DNA methylation analysis was performed on the peripheral blood of 23 twin pairs (10 monozygotic and 13 dizygotic), 4 concordant and 19 discordant pairs for CH at birth. Results Differential methylation analysis did not show significant differences in methylation levels between CH cases and controls, but a different methylation status of several genes may explain the CH discordance of a monozygotic twin couple carrying a monoallelic nonsense mutation of DUOX2. In addition, the median number of hypo-methylated Stochastic Epigenetic Mutations (SEMs) resulted significantly increased in cases compared to controls. The prioritization analysis for CH performed on the genes epimutated exclusively in the cases identified SLC26A4, FOXI1, NKX2-5 and TSHB as the genes with the highest score. The analysis of significantly SEMs-enriched regions led to the identification of two genes (FAM50B and MEG8) that resulted epigenetically dysregulated in cases. Conclusion Epigenetic modifications may potentially account for CH pathogenesis and explain discordance among monozygotic twins.

Published

2022

5. Fetal growth patterns in Beckwith-Wiedemann syndrome

Author

A, Mussa, S, Russo, A, de Crescenzo, A, Freschi, L, Calzari, S, Maitz, M, Macchiaiolo, C, Molinatto, G, Baldassarre, M, Mariani, L, Tarani, M F, Bedeschi, D, Milani, D, Melis, A, Bartuli, M V, Cubellis, A, Selicorni, M C, Silengo, L, Larizza, A, Riccio, G B, Ferrero, Mussa, A, Russo, S, de Crescenzo, A, Freschi, A, Calzari, L, Maitz, S, Macchiaiolo, M, Molinatto, C, Baldassarre, G, Mariani, M, Tarani, L, Bedeschi, M. F, Milani, D, Melis, D, Bartuli, A, Cubellis, MARIA VITTORIA, Selicorni, A, Silengo, M. C, Larizza, L, Riccio, A, Ferrero, G. B., Russo, S., de Crescenzo, A., Freschi, A., Calzari, L., Maitz, S., Macchiaiolo, M., Molinatto, C., Baldassarre, G., Mariani, M., Tarani, L., Bedeschi, M. F., Milani, D., Melis, D., Bartuli, A., Cubellis, M. V., Selicorni, A., Silengo, M. C., Larizza, L., and Riccio, Andrea

Subjects

Beckwith-Wiedemann Syndrome, phenotype, genotype, Beckwith–Wiedemann, Gene Expression, Gestational Age, fetal growth, overgrowth, Anthropometry, Chromosomes, Human, Pair 11, Cyclin-Dependent Kinase Inhibitor p57, Fetal Development, Fetus, Genotype, Humans, Infant, Newborn, Mutation, Phenotype, Premature Birth, DNA Methylation, Genomic Imprinting, Uniparental Disomy, Chromosomes, Beckwith-Wiedemann, Fetal growth, Overgrowth, Genetics (clinical), Genetics, Pair 11, Infant, Newborn, Human

Abstract

We provide data on fetal growth pattern on the molecular subtypes of Beckwith-Wiedemann syndrome (BWS): IC1 gain of methylation (IC1-GoM), IC2 loss of methylation (IC2-LoM), 11p15.5 paternal uniparental disomy (UPD), and CDKN1C mutation. In this observational study, gestational ages and neonatal growth parameters of 247 BWS patients were compared by calculating gestational age-corrected standard deviation scores (SDS) and proportionality indexes to search for differences among IC1-GoM (n = 21), UPD (n = 87), IC2-LoM (n = 147), and CDKN1C mutation (n = 11) patients. In IC1-GoM subgroup, weight and length are higher than in other subgroups. Body proportionality indexes display the following pattern: highest in IC1-GoM patients, lowest in IC2-LoM/CDKN1C patients, intermediate in UPD ones. Prematurity was significantly more prevalent in the CDKN1C (64%) and IC2-LoM subgroups (37%). Fetal growth patterns are different in the four molecular subtypes of BWS and remarkably consistent with altered gene expression primed by the respective molecular mechanisms. IC1-GoM cases show extreme macrosomia and severe disproportion between weight and length excess. In IC2-LoM/CDKN1C patients, macrosomia is less common and associated with more proportionate weight/length ratios with excess of preterm birth. UPD patients show growth patterns closer to those of IC2-LoM, but manifest a body mass disproportion rather similar to that seen in IC1-GoM cases.

Published

2016

6. DNA methylation in the diagnosis of monogenic diseases

Author

Maurizio Genuardi, Cristiana Lo Lo Nigro, Andrea Riccio, Flavia Cerrato, Eugenio Sangiorgi, Elisabetta Tabolacci, Francesca Ariani, Giovanni Neri, Fabio Coppedè, Luciano Calzari, Fiorella Gurrieri, Alessandro De Luca, Gabriella Maria Squeo, Angela Sparago, Giuseppe Merla, Fulvia Brugnoletti, Isabella Torrente, Monica Miozzo, Silvia Russo, Silvia Tabano, Silvia M. Sirchia, Cristina Gervasini, Emiliano Giardina, Cerrato, F., Sparago, A., Ariani, F., Brugnoletti, F., Calzari, L., Coppede, F., De Luca, A., Gervasini, C., Giardina, E., Gurrieri, F., Nigro, C. L., Merla, G., Miozzo, M., Russo, S., Sangiorgi, E., Sirchia, S. M., Squeo, G. M., Tabano, S., Tabolacci, E., Torrente, I., Genuardi, M., Neri, G., Riccio, A., and Lo Nigro, C.

Subjects

0301 basic medicine, Epigenomics, Methyltransferase, Genetic testing, lcsh:QH426-470, Prenatal diagnosis, neuromuscular diseases, Review, 030105 genetics & heredity, Settore MED/03 - GENETICA MEDICA, Genome, Imprinting disorder, 03 medical and health sciences, chemistry.chemical_compound, Developmental delay/intellectual disability disorder, Genetics, medicine, imprinting disorders, Humans, Genetics (clinical), DNA methylation, developmental delay/intellectual disability disorders, epi-signatures, genetic testing, hereditary tumors, high-throughput analysis, prenatal diagnosis, biology, medicine.diagnostic_test, Genome, Human, High-throughput analysi, Genetic Diseases, Inborn, Methylation, Developmental delay/intellectual disability disorders, Epi-signatures, Hereditary tumors, High-throughput analysis, Imprinting disorders, Neuromuscular diseases, Neuromuscular disease, lcsh:Genetics, 030104 developmental biology, Histone, Phenotype, chemistry, Settore MED/03, biology.protein, Hereditary tumor, Human genome, Epi-signature, DNA

Abstract

DNA methylation in the human genome is largely programmed and shaped by transcription factor binding and interaction between DNA methyltransferases and histone marks during gamete and embryo development. Normal methylation profiles can be modified at single or multiple loci, more frequently as consequences of genetic variants acting in cis or in trans, or in some cases stochastically or through interaction with environmental factors. For many developmental disorders, specific methylation patterns or signatures can be detected in blood DNA. The recent use of high-throughput assays investigating the whole genome has largely increased the number of diseases for which DNA methylation analysis provides information for their diagnosis. Here, we review the methylation abnormalities that have been associated with mono/oligogenic diseases, their relationship with genotype and phenotype and relevance for diagnosis, as well as the limitations in their use and interpretation of results.

Published

2020

7. A KHDC3L mutation resulting in recurrent hydatidiform mole causes genome-wide DNA methylation loss in oocytes and persistent imprinting defects post-fertilisation

Author

Luciano Calzari, Zahra Anvar, Bahia Namavar Jahromi, Mojgan Akbarzadeh Jahromi, Ankit Verma, Simon Andrews, Angela Sparago, Maryam Davari, Gavin Kelsey, Hannah Demond, Silvia Russo, David Monk, Andrea Riccio, Kelsey, Gavin [0000-0002-9762-5634], Apollo - University of Cambridge Repository, Demond, H., Anvar, Z., Jahromi, B. N., Sparago, A., Verma, A., Davari, M., Calzari, L., Russo, S., Jahromi, M. A., Monk, D., Andrews, S., Riccio, A., and Kelsey, G.

Subjects

Embryology, Oocyte, Genomic imprinting, Placenta, ADN, Bisulfite sequencing, lcsh:Medicine, Germline, 0302 clinical medicine, Pregnancy, Imprinting (psychology), Genetics (clinical), Genetics, 0303 health sciences, DNA methylation, 030219 obstetrics & reproductive medicine, Epigenetic, Hydatidiform Mole, Methylation, Single-cell analysis, Embryo, Single-cell analysi, Uterine Neoplasms, Molecular Medicine, Epigenetics, Female, Adult, lcsh:QH426-470, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, Humans, Molecular Biology, 030304 developmental biology, Embriologia, Research, lcsh:R, Embryos, Proteins, DNA, Sequence Analysis, DNA, Epigenètica, Oocytes, lcsh:Genetics, Blastocyst, Differentially methylated regions, Neoplasm Recurrence, Local

Abstract

Background Maternal effect mutations in the components of the subcortical maternal complex (SCMC) of the human oocyte can cause early embryonic failure, gestational abnormalities and recurrent pregnancy loss. Enigmatically, they are also associated with DNA methylation abnormalities at imprinted genes in conceptuses: in the devastating gestational abnormality biparental complete hydatidiform mole (BiCHM) or in multi-locus imprinting disease (MLID). However, the developmental timing, genomic extent and mechanistic basis of these imprinting defects are unknown. The rarity of these disorders and the possibility that methylation defects originate in oocytes have made these questions very challenging to address. Methods Single-cell bisulphite sequencing (scBS-seq) was used to assess methylation in oocytes from a patient with BiCHM identified to be homozygous for an inactivating mutation in the human SCMC component KHDC3L. Genome-wide methylation analysis of a preimplantation embryo and molar tissue from the same patient was also performed. Results High-coverage scBS-seq libraries were obtained from five KHDC3Lc.1A>G oocytes, which revealed a genome-wide deficit of DNA methylation compared with normal human oocytes. Importantly, germline differentially methylated regions (gDMRs) of imprinted genes were affected similarly to other sequence features that normally become methylated in oocytes, indicating no selectivity towards imprinted genes. A range of methylation losses was observed across genomic features, including gDMRs, indicating variable sensitivity to defects in the SCMC. Genome-wide analysis of a pre-implantation embryo and molar tissue from the same patient showed that following fertilisation methylation defects at imprinted genes persist, while most non-imprinted regions of the genome recover near-normal methylation post-implantation. Conclusions We show for the first time that the integrity of the SCMC is essential for de novo methylation in the female germline. These findings have important implications for understanding the role of the SCMC in DNA methylation and for the origin of imprinting defects, for counselling affected families, and will help inform future therapeutic approaches.

Published

2019

8. Molecular Etiology Disclosed by Array CGH in Patients With Silver–Russell Syndrome or Similar Phenotypes

Author

Milena Crippa, Maria Teresa Bonati, Luciano Calzari, Chiara Picinelli, Cristina Gervasini, Alessandra Sironi, Ilaria Bestetti, Sara Guzzetti, Simonetta Bellone, Angelo Selicorni, Alessandro Mussa, Andrea Riccio, Giovanni Battista Ferrero, Silvia Russo, Lidia Larizza, Palma Finelli, Crippa, M., Bonati, M. T., Calzari, L., Picinelli, C., Gervasini, C., Sironi, A., Bestetti, I., Guzzetti, S., Bellone, S., Selicorni, A., Mussa, A., Riccio, A., Ferrero, G. B., Russo, S., Larizza, L., and Finelli, P.

Subjects

0301 basic medicine, lcsh:QH426-470, array CGH, differential diagnosis, Netchine–Harbison clinical scoring system, pathogenic CNVs, Silver–Russell syndrome, differential diagnosi, Bioinformatics, pathogenic CNV, 03 medical and health sciences, 0302 clinical medicine, parasitic diseases, medicine, Genetics, Copy-number variation, Epigenetics, Gene, Genetics (clinical), Original Research, business.industry, medicine.disease, Phenotype, lcsh:Genetics, 030104 developmental biology, 030220 oncology & carcinogenesis, Etiology, Molecular Medicine, Differential diagnosis, business, Comparative genomic hybridization

Abstract

Introduction: Silver-Russell syndrome (SRS) is an imprinting disorder primarily caused by genetic and epigenetic aberrations on chromosomes 11 and 7. SRS is a rare growth retardation disorder often misdiagnosed due to its heterogeneous and non-specific clinical features. The Netchine-Harbison clinical scoring system (NH-CSS) is the recommended tool for differentiating patients into clinical SRS or unlikely SRS. However, the clinical diagnosis is molecularly confirmed only in about 60% of patients, leaving the remaining substantial proportion of SRS patients with unknown genetic etiology. Materials and Methods: A cohort of 34 Italian patients with SRS or SRS-like features scored according to the NH-CSS and without any SRS-associated (epi)genetic alterations was analyzed by high-resolution array-based comparative genomic hybridization (CGH) in order to identify potentially pathogenic copy number variants (CNVs). Results and Discussion: In seven patients, making up 21% of the initial cohort, five pathogenic and two potentially pathogenic CNVs were found involving distinct genomic regions either previously associated with growth delay conditions (1q24.3-q25.3, 17p13.3, 17q22, and 22q11.2-q11.22) and with SRS spectrum (7p12.1 and 7p15.3-p14.3) or outlined for the first time (19q13.42), providing a better definition of reported and as yet unreported SRS overlapping syndromes. All the variants involve genes with a defined role in growth pathways, and for two genes mapping at 7p, IGF2BP3 and GRB10, the association with SRS turns out to be reinforced. The deleterious effect of the two potentially pathogenic variants, comprising GRB10 and ZNF331 genes, was explored by targeted approaches, though further studies are needed to validate their pathogenic role in the SRS etiology. In conclusion, we reconfirm the utility of performing a genome-wide scan to achieve a differential diagnosis in patients with SRS or similar features and to highlight novel chromosome alterations associated with SRS and growth retardation disorders.

Published

2019

9. The phenotypic variations of multi-locus imprinting disturbances associated with maternal-effect variants of NLRP5 range from overt imprinting disorder to apparently healthy phenotype

Author

Faisal I. Rezwan, Flavia Cerrato, Andrea Riccio, Laura Pignata, Deborah J G Mackay, Maria Vittoria Cubellis, Ankit Verma, Claudia Angelini, Maria Grazia Patricelli, Massimo Carella, Luciano Calzari, Naomi De Francesco, Rosita Del Prete, Angela Sparago, Silvia Russo, Orazio Palumbo, Sparago, A., Verma, A., Patricelli, M. G., Pignata, L., Russo, S., Calzari, L., De Francesco, N., Del Prete, R., Palumbo, O., Carella, M., Mackay, D. J. G., Rezwan, F. I., Angelini, C., Cerrato, F., Cubellis, M. V., and Riccio, A.

Subjects

Male, Genomic imprinting, Multi-locus imprinting disturbance, Beckwith–Wiedemann syndrome, Short Report, DNA- methylation, Biology, Compound heterozygosity, Autoantigens, NLRP5, Mitochondrial Proteins, Young Adult, Loss of Function Mutation, Exome Sequencing, Genetics, medicine, Humans, Imprinting (psychology), Maternal-effect variants, Child, Molecular Biology, Genetics (clinical), Maternal-effect variant, Nuclear Proteins, Sequence Analysis, DNA, medicine.disease, Phenotype, Human genetics, Pedigree, Abortion, Spontaneous, Differentially methylated regions, Multi-locus imprinting disturbances, DNA methylation, Beckwith-Wiedemann syndrome, Female, Maternal Inheritance, DNA-methylation, Developmental Biology, Genome-Wide Association Study

Abstract

Background A subset of individuals affected by imprinting disorders displays multi-locus imprinting disturbances (MLID). MLID has been associated with maternal-effect variants that alter the maintenance of methylation at germline-derived differentially methylated regions (gDMRs) in early embryogenesis. Pedigrees of individuals with MLID also include siblings with healthy phenotype. However, it is unknown if these healthy individuals have MLID themselves or if their methylation patterns differ from those associated with imprinting disorders, and in general, if MLID affects the clinical phenotype. Methods We have investigated gDMR methylation by locus-specific and whole-genome analyses in a family with multiple pregnancy losses, a child with Beckwith-Wiedemann syndrome (BWS) and a further child with no clinical diagnosis of imprinting disorder or other pathologies. Results We detected MLID with different methylation profiles in the BWS-affected and healthy siblings. Whole-exome sequencing demonstrated the presence of novel loss-of-function variants of NLRP5 in compound heterozygosity in the mother. The methylation profiles of the two siblings were compared with those of other cases with MLID and control groups by principal component analysis and unsupervised hierarchical clustering, but while their patterns were clearly separated from those of controls, we were unable to cluster those associated with specific clinical phenotypes among the MLID cases. Conclusion The identification of two novel maternal-effect variants of NLRP5 associated with poly-abortivity and MLID adds further evidence to the role of this gene in the maintenance of genomic imprinting in early embryos. Furthermore, our results demonstrate that within these pedigrees, MLID can also be present in the progeny with healthy phenotype, indicating that some sort of compensation occurs between altered imprinted loci in these individuals. The analysis of larger cohorts of patients with MLID is needed to formulate more accurate epigenotype-phenotype correlations.

Published

2019

10. The Histone Deubiquitinating Enzyme Ubp10 Is Involved in rDNA Locus Control in Saccharomyces cerevisiae by Affecting Sir2p Association

Author

Ivan Orlandi, Lilia Alberghina, Marina Vai, Luciano Calzari, Calzari, L, Orlandi, I, Alberghina, L, and Vai, M

Subjects

Saccharomyces cerevisiae Proteins, Transcription, Genetic, Saccharomyces cerevisiae, Biology, DNA, Ribosomal, Methylation, Histone Deacetylases, Chromatin remodeling, Histones, Sirtuin 2, Histone H1, Histone methylation, Histone H2A, Genetics, Immunoprecipitation, Sirtuins, Histone code, Gene Silencing, Silent Information Regulator Proteins, Saccharomyces cerevisiae, Histone modification, Ubp10p, rDNA, Sir2p, silencing, Ubiquitin, Nuclear Proteins, Acetylation, Note, Chromatin, Histone methyltransferase, Ubiquitin Thiolesterase, Chromatin immunoprecipitation

Abstract

Histone modifications influence chromatin structure and thus regulate the accessibility of DNA to replication, recombination, repair, and transcription. We show here that the histone deubiquitinating enzyme Ubp10 contributes to the formation/maintenance of silenced chromatin at the rDNA by affecting Sir2p association.

Published

2006