Your search keyword '"Ianari, A"' showing total 10 results

1. Discovery of a First-in-Class Inhibitor of the PRMT5–Substrate Adaptor Interaction

Author

Dale Porter, Alessandra Ianari, Merissa Brousseau, Patrick McCarren, Foxy P. Robinson, Adam Skepner, Virendar K. Kaushik, Kathleen M. Mulvaney, Arthur J. Campbell, Martin J Drysdale, Zachary Mullin-Bernstein, Brian J. McMillan, Robert Hilgraf, Ritu Singh, Matthew J. Ranaghan, Meghan O’Keefe, William R. Sellers, David C. McKinney, Jamie A. Moroco, Michael F. Mesleh, David E. Timm, Besnik Bajrami, and Florence F. Wagner

Subjects

Models, Molecular, Protein-Arginine N-Methyltransferases, Spliceosome, Dose-Response Relationship, Drug, Molecular Structure, biology, Stereochemistry, fungi, Signal transducing adaptor protein, Methylation, Small molecule, Article, Pyridazines, Structure-Activity Relationship, chemistry.chemical_compound, Histone, chemistry, Covalent bond, Drug Discovery, biology.protein, Humans, Molecular Medicine, Lead compound, Adaptor Proteins, Signal Transducing, Cysteine

Abstract

PRMT5 and its substrate adaptor proteins (SAPs), pICln and Riok1, are synthetic lethal dependencies in MTAP-deleted cancer cells. SAPs share a conserved PRMT5 binding motif (PBM) which mediates binding to a surface of PRMT5 distal to the catalytic site. This interaction is required for methylation of several PRMT5 substrates, including histone and spliceosome complexes. We screened for small molecule inhibitors of the PRMT5-PBM interaction and validated a compound series which binds to the PRMT5-PBM interface and directly inhibits binding of SAPs. Mode of action studies revealed the formation of a covalent bond between a halogenated pyridazinone group and cysteine 278 of PRMT5. Optimization of the starting hit produced a lead compound, BRD0639, which engages the target in cells, disrupts PRMT5-RIOK1 complexes, and reduces substrate methylation. BRD0639 is a first-in-class PBM-competitive inhibitor that can support studies of PBM-dependent PRMT5 activities and the development of novel PRMT5 inhibitors that selectively target these functions.

Published

2021

2. Targeted Covalent Inhibition of Plasmodium FK506 Binding Protein 35

Author

Lisl Y. Esherick, Jacquin C. Niles, Patrick McCarren, Thomas C. Atack, Charisse Flerida A. Pasaje, Alessandra Ianari, Debjani Pal, Henock B. Befekadu, Christa Blomquist, Jamie A. Moroco, Donald Raymond, Foxy P. Robinson, and William R. Sellers

Subjects

chemistry.chemical_classification, Plasmodium (life cycle), biology, 010405 organic chemistry, Organic Chemistry, Binding pocket, biology.organism_classification, 01 natural sciences, Biochemistry, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Enzyme, FKBP, chemistry, Covalent bond, Drug Discovery, Cysteine

Abstract

FK506-binding protein 35, FKBP35, has been implicated as an essential malarial enzyme. Rapamycin and FK506 exhibit antiplasmodium activity in cultured parasites. However, due to the highly conserved nature of the binding pockets of FKBPs and the immunosuppressive properties of these drugs, there is a need for compounds that selectively inhibit FKBP35 and lack the undesired side effects. In contrast to human FKBPs, FKBP35 contains a cysteine, C106, adjacent to the rapamycin binding pocket, providing an opportunity to develop targeted covalent inhibitors of Plasmodium FKBP35. Here, we synthesize inhibitors of FKBP35, show that they directly bind FKBP35 in a model cellular setting, selectively covalently modify C106, and exhibit antiplasmodium activity in blood-stage cultured parasites.

Published

2020

3. Molecular basis for substrate recruitment to the PRMT5 methylosome

Author

Andrew J. Aguirre, Nischal Acharya, Adam Skepner, Christa Blomquist, David C. McKinney, Michael J. Young, Meghan O’Keefe, Ruitong Li, Debjani Pal, Kathleen M. Mulvaney, Yelena Freyzon, Matthew E. Stokes, Fazli K. Bozal, Donald Raymond, Matthew J. Ranaghan, Devishi Kesar, Diego J. Rodriguez, Yossef Baidi, Annan Yang, William R. Sellers, Sidharth S. Jain, Dale Porter, Salvatore LaRussa, Alessandra Ianari, Josie Columbus, Zachary Mullin-Bernstein, Alissa J. Nelson, and Brian J. McMillan

Subjects

Male, Spliceosome, Cytoplasm, Protein-Arginine N-Methyltransferases, Mice, Nude, Protein Serine-Threonine Kinases, Methylation, Article, Ion Channels, Histones, Mice, Cell Line, Tumor, Animals, Humans, Molecular Biology, Peptide sequence, Methylosome, biology, Protein arginine methyltransferase 5, Intron, Intracellular Signaling Peptides and Proteins, Signal transducing adaptor protein, Nuclear Proteins, Cell Biology, HCT116 Cells, Cell biology, Histone, HEK293 Cells, RNA splicing, biology.protein, Spliceosomes, Female, Peptides, Protein Processing, Post-Translational, Protein Binding

Abstract

PRMT5 is an essential arginine methyltransferase and a therapeutic target in MTAP-null cancers. PRMT5 uses adaptor proteins for substrate recruitment through a previously undefined mechanism. Here, we identify an evolutionarily conserved peptide sequence shared among the three known substrate adaptors (CLNS1A, RIOK1, and COPR5) and show that it is necessary and sufficient for interaction with PRMT5. We demonstrate that PRMT5 uses modular adaptor proteins containing a common binding motif for substrate recruitment, comparable with other enzyme classes such as kinases and E3 ligases. We structurally resolve the interface with PRMT5 and show via genetic perturbation that it is required for methylation of adaptor-recruited substrates including the spliceosome, histones, and ribosomal complexes. Furthermore, disruption of this site affects Sm spliceosome activity, leading to intron retention. Genetic disruption of the PRMT5-substrate adaptor interface impairs growth of MTAP-null tumor cells and is thus a site for development of therapeutic inhibitors of PRMT5.

Published

2021

4. Molecular basis for substrate recruitment to the PRMT5 methylosome

Author

Yossef Baidi, Brian J. McMillan, Alissa J. Nelson, Josie Columbus, Sidharth S. Jain, Nischal Acharya, Matthew J. Ranaghan, Meghan O’Keefe, William R. Sellers, Kathleen M. Mulvaney, Yelena Freyzon, Fazli K. Bozal, Christa Blomquist, Ruitong Li, Adam Skepner, David C. McKinney, Dale Porter, Alessandra Ianari, Donald Raymond, and Matthew E. Stokes

Subjects

Spliceosome, Histone, biology, Chemistry, Protein arginine methyltransferase 5, biology.protein, Signal transducing adaptor protein, Methylation, Peptide sequence, Ribosome assembly, Methylosome, Cell biology

Abstract

PRMT5 is an arginine methyltransferase and a therapeutic target in MTAP null cancers. PRMT5 utilizes adaptor proteins for substrate recruitment through a previously undefined mechanism. Here, we identify an evolutionarily conserved peptide sequence shared among the three known substrate adaptors (pICln/CLNS1A, RIOK1 and COPR5) and show it is necessary and sufficient for interaction with PRMT5. We structurally resolve the interface with PRMT5 and show via genetic perturbation that it is required for methylation of adaptor-recruited substrates including the spliceosome, histones, and ribosome assembly complexes. Genetic disruption of the PRMT5-substrate adaptor interface leads to a hypomorphic decrease in growth of MTAP null tumor cells and is thus a novel site for development of therapeutic inhibitors of PRMT5.

Published

2020

5. Foxm1 controls a pro-stemness microRNA network in neural stem cells

Author

Elisabetta Ferretti, Luigi Grassi, Enrico De Smaele, Marta Moretti, Angela Mastronuzzi, Evelina Miele, Luana Abballe, Mauro Chinappi, Franco Locatelli, Francesco Cicconardi, Loredana Le Pera, Alessandra Ianari, Agnese Po, Daniel D'Andrea, Arjun Bhutkar, Alessandra Vacca, Zein Mersini Besharat, Besharat, Zein Mersini [0000-0003-0317-9854], Le Pera, Loredana [0000-0002-0076-9878], De Smaele, Enrico [0000-0003-4524-4423], Miele, Evelina [0000-0002-4747-1032], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Cellular differentiation, Inbred C57BL, Mice, Neural Stem Cells, Cerebellum, Animals, Animals, Newborn, Cell Differentiation, Cell Proliferation, Forkhead Box Protein M1, Hedgehog Proteins, High-Throughput Nucleotide Sequencing, Mice, Inbred C57BL, MicroRNAs, Nanog Homeobox Protein, Neurogenesis, Primary Cell Culture, Signal Transduction, Spheroids, Cellular, Zinc Finger Protein GLI1, Gene Expression Regulation, Developmental, Developmental, reproductive and urinary physiology, Regulation of gene expression, Gene knockdown, Multidisciplinary, microRNA, Neural stem cell, Cell biology, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Medicine, Signal transduction, biological phenomena, cell phenomena, and immunity, Homeobox protein NANOG, Science, Biology, Article, 03 medical and health sciences, Neurosphere, Settore BIO/10, Newborn, nervous system diseases, 030104 developmental biology, Gene Expression Regulation, nervous system, Cellular, Spheroids

Abstract

Cerebellar neural stem cells (NSCs) require Hedgehog-Gli (Hh-Gli) signalling for their maintenance and Nanog expression for their self-renewal. To identify novel molecular features of this regulatory pathway, we used next-generation sequencing technology to profile mRNA and microRNA expression in cerebellar NSCs, before and after induced differentiation (Diff-NSCs). Genes with higher transcript levels in NSCs (vs. Diff-NSCs) included Foxm1, which proved to be directly regulated by Gli and Nanog. Foxm1 in turn regulated several microRNAs that were overexpressed in NSCs: miR-130b, miR-301a, and members of the miR-15~16 and miR-17~92 clusters and whose knockdown significantly impaired the neurosphere formation ability. Our results reveal a novel Hh-Gli-Nanog-driven Foxm1-microRNA network that controls the self-renewal capacity of NSCs.

Published

2018

6. Proapoptotic Function of the Retinoblastoma Tumor Suppressor Protein

Author

Alessandra Ianari, Edoardo Alesse, Eliezer Calo, Jacqueline A. Lees, Elisabetta Ferretti, Tiziana Natale, Alberto Gulino, Isabella Screpanti, and Kevin M. Haigis

Subjects

Cancer Research, cellcycle, tumor suppressor, DNA damage, Blotting, Western, Context (language use), Biology, Retinoblastoma Protein, Article, retinoblastoma, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Animals, Humans, Immunoprecipitation, E2F1, Promoter Regions, Genetic, E2F, neoplasms, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Reverse Transcriptase Polymerase Chain Reaction, Retinoblastoma, apoptosis, Retinoblastoma protein, Cell Biology, Cell cycle, Flow Cytometry, medicine.disease, E2F Transcription Factors, 3. Good health, Gene Expression Regulation, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Phosphorylation, biological phenomena, cell phenomena, and immunity, DNA Damage

Abstract

Summary The retinoblastoma protein (pRB) tumor suppressor blocks cell proliferation by repressing the E2F transcription factors. This inhibition is relieved through mitogen-induced phosphorylation of pRB, triggering E2F release and activation of cell-cycle genes. E2F1 can also activate proapoptotic genes in response to genotoxic or oncogenic stress. However, pRB's role in this context has not been established. Here we show that DNA damage and E1A-induced oncogenic stress promote formation of a pRB-E2F1 complex even in proliferating cells. Moreover, pRB is bound to proapoptotic promoters that are transcriptionally active, and pRB is required for maximal apoptotic response in vitro and in vivo. Together, these data reveal a direct role for pRB in the induction of apoptosis in response to genotoxic or oncogenic stress.

Published

2009

7. Differential regulation of E2F1 apoptotic target genes in response to DNA damage

Author

Laura Belloni, Alessandra Ianari, Natalia Pediconi, Antonio Porcellini, Edoardo Alesse, Massimo Levrero, Isabella Screpanti, Rita Gallo, Letizia Cimino, Alberto Gulino, Clara Balsano, Antonio Costanzo, Pediconi, N, Ianari, A, Costanzo, A, Belloni, L, Gallo, R, Cimino, L, Porcellini, Antonio, Screpanti, L, Balsano, C, Alesse, E, Gulino, A, and Levrero, M.

Subjects

Messenger, Apoptosis, Cell Cycle Proteins, Histones, Genes, Reporter, Tumor Cells, Cultured, E2F1, Tumor Protein p73, Genes, Tumor Suppressor, Promoter Regions, Genetic, Etoposide, Settore MED/35 - Malattie Cutanee e Veneree, Cultured, Nuclear Proteins, E2F1 Transcription Factor, Acetylation, Chromatin, Cell biology, Tumor Cells, DNA-Binding Proteins, biological phenomena, cell phenomena, and immunity, E2F Transcription Factors, Tumor Suppressor, Transcriptional Activation, endocrine system, DNA damage, Biology, Promoter Regions, Genetic, DNA Damage, Humans, Doxorubicin, Tumor Suppressor Proteins, Fibroblasts, Gene Deletion, RNA, Messenger, Transcription Factors, Gene Expression Regulation, E2F, Transcription factor, Reporter, Cell Biology, Genes, Cancer research, RNA, Chromatin immunoprecipitation

Abstract

E2F1, a member of the E2F family of transcription factors, in addition to its established proliferative effect, has also been implicated in the induction of apoptosis through p53-dependent and p53-independent pathways. Several genes involved in the activation or execution of the apoptotic programme have recently been shown to be upregulated at the transcriptional level by E2F1 overexpression, including the genes encoding INK4a/ARF, Apaf-1, caspase 7 and p73 (refs 3-5). E2F1 is stabilized in response to DNA damage but it has not been established how this translates into the activation of specific subsets of E2F target genes. Here, we applied a chromatin immunoprecipitation approach to show that, in response to DNA damage, E2F1 is directed from cell cycle progression to apoptotic E2F target genes. We identify p73 as an important E2F1 apoptotic target gene in DNA damage response and we show that acetylation is required for E2F1 recruitment on the P1p73 promoter and for its transcriptional activation.

Published

2003

8. The retinoblastoma protein induces apoptosis directly at the mitochondria

Author

Simona Nedelcu, Loren D. Walensky, Jacqueline A. Lees, Alessandra Ianari, Keren I. Hilgendorf, Elizaveta S. Leshchiner, Mindy Maynard, and Eliezer Calo

Subjects

Mutant, Transplantation, Heterologous, Mice, Nude, Endogeny, Apoptosis, Mice, SCID, Mitochondrion, Retinoblastoma Protein, Mice, Cell Line, Tumor, Genetics, Animals, Humans, neoplasms, bcl-2-Associated X Protein, Cell Nucleus, biology, Tumor Necrosis Factor-alpha, Retinoblastoma protein, Cytochromes c, Translation (biology), In vitro, Cell biology, Mitochondria, Gene Expression Regulation, Neoplastic, Perspective, biology.protein, Cancer research, Tumor necrosis factor alpha, biological phenomena, cell phenomena, and immunity, Developmental Biology, Protein Binding

Abstract

The retinoblastoma protein gene RB-1 is mutated in one-third of human tumors. Its protein product, pRB (retinoblastoma protein), functions as a transcriptional coregulator in many fundamental cellular processes. Here, we report a nonnuclear role for pRB in apoptosis induction via pRB's direct participation in mitochondrial apoptosis. We uncovered this activity by finding that pRB potentiated TNFα-induced apoptosis even when translation was blocked. This proapoptotic function was highly BAX-dependent, suggesting a role in mitochondrial apoptosis, and accordingly, a fraction of endogenous pRB constitutively associated with mitochondria. Remarkably, we found that recombinant pRB was sufficient to trigger the BAX-dependent permeabilization of mitochondria or liposomes in vitro. Moreover, pRB interacted with BAX in vivo and could directly bind and conformationally activate BAX in vitro. Finally, by targeting pRB specifically to mitochondria, we generated a mutant that lacked pRB's classic nuclear roles. This mito-tagged pRB retained the ability to promote apoptosis in response to TNFα and also additional apoptotic stimuli. Most importantly, induced expression of mito-tagged pRB in Rb−/−;p53−/− tumors was sufficient to block further tumor development. Together, these data establish a nontranscriptional role for pRB in direct activation of BAX and mitochondrial apoptosis in response to diverse stimuli, which is profoundly tumor-suppressive.

Published

2013

9. DTL/CDT2 is essential for both CDT1 regulation and the early G2/M checkpoint

Author

Paul S. Danielian, Jacqueline A. Lees, Alessandra Ianari, Kevin Lai, Christopher L. Sansam, Adam Amsterdam, Nancy Hopkins, and Jennifer L. Shepard

Subjects

DNA re-replication, G2 Phase, Cell cycle checkpoint, Embryo, Nonmammalian, Ubiquitin-Protein Ligases, Mitosis, Cell Cycle Proteins, Models, Biological, DNA replication factor CDT1, Radiation, Ionizing, Genetics, Animals, Humans, CHEK1, Genetic Testing, Zebrafish, Adaptor Proteins, Signal Transducing, biology, Nuclear Proteins, G2-M DNA damage checkpoint, Cell cycle, Zebrafish Proteins, Cullin Proteins, HCT116 Cells, Cell biology, Ubiquitin ligase, DNA-Binding Proteins, Mutagenesis, Insertional, embryonic structures, Mutation, biology.protein, Developmental Biology, DNA Damage, HeLa Cells, Protein Binding, Research Paper

Abstract

Checkpoint genes maintain genomic stability by arresting cells after DNA damage. Many of these genes also control cell cycle events in unperturbed cells. By conducting a screen for checkpoint genes in zebrafish, we found that dtl/cdt2 is an essential component of the early, radiation-induced G2/M checkpoint. We subsequently found that dtl/cdt2 is required for normal cell cycle control, primarily to prevent rereplication. Both the checkpoint and replication roles are conserved in human DTL. Our data indicate that the rereplication reflects a requirement for DTL in regulating CDT1, a protein required for prereplication complex formation. CDT1 is degraded in S phase to prevent rereplication, and following DNA damage to prevent origin firing. We show that DTL associates with the CUL4–DDB1 E3 ubiquitin ligase and is required for CDT1 down-regulation in unperturbed cells and following DNA damage. The cell cycle defects of Dtl-deficient zebrafish are suppressed by reducing Cdt1 levels. In contrast, the early G2/M checkpoint defect appears to be Cdt1-independent. Thus, DTL promotes genomic stability through two distinct mechanisms. First, it is an essential component of the CUL4–DDB1 complex that controls CDT1 levels, thereby preventing rereplication. Second, it is required for the early G2/M checkpoint.

Published

2006

10. Specific role for p300/CREB-binding protein-associated factor activity in E2F1 stabilization in response to DNA damage

Author

Alberto Gulino, Marzia Palma, Edoardo Alesse, Rita Gallo, and Alessandra Ianari

Subjects

endocrine system, Time Factors, DNA damage, Immunoblotting, Apoptosis, Cell Cycle Proteins, P300-CBP Transcription Factors, Ataxia Telangiectasia Mutated Proteins, Biology, Protein Serine-Threonine Kinases, Transfection, Biochemistry, Cell Line, Mice, Acetyltransferases, E2F1, Animals, Humans, p300-CBP Transcription Factors, CREB-binding protein, Cycloheximide, Phosphorylation, Promoter Regions, Genetic, Molecular Biology, Transcription factor, acetylation, acetyltransferases, animals, apoptosis, cell cycle proteins, cell line, chemistry/metabolism, cisplatin, cycloheximide, dna damage, dna-binding proteins, doxorubicin, e2f transcription factors, e2f1 transcription factor, genetic, histone acetyltransferases, humans, immunoblotting, metabolism, metabolism/physiology, mice, p300-cbp transcription factors, pharmacology, phosphorylation, plasmids, precipitin tests, promoter regions, protein binding, protein synthesis inhibitors, protein-serine-threonine kinases, signal transduction, time factors, transcription factors, transfection, tumor suppressor proteins, Histone Acetyltransferases, Protein Synthesis Inhibitors, Tumor Suppressor Proteins, E2F1 Transcription Factor, Acetylation, Cell Biology, Molecular biology, Precipitin Tests, E2F Transcription Factors, DNA-Binding Proteins, Doxorubicin, biology.protein, biological phenomena, cell phenomena, and immunity, Signal transduction, Cisplatin, DNA Damage, Plasmids, Protein Binding, Signal Transduction, Transcription Factors

Abstract

E2F1, a member of the E2F family of transcription factors, plays a pivotal role in controlling both physiological cell-cycle progression and apoptotic cell death in response to DNA damage and oncogene activation. In response to genotoxic stresses, E2F1 is stabilized by signals that include ATM-dependent phosphorylation. We recently demonstrated that DNA damage induces also E2F1 acetylation, which is required for its recruitment onto apoptotic gene promoters. Here we show that E2F1 is stabilized in response to doxorubicin and cisplatin treatments even in the absence of either ATM-dependent phosphorylation or p53 and cAbl, two major transducers of DNA damage signaling. We found that acetylation of E2F1 is, instead, required to stabilize the protein in response to doxorubicin. Finally, we report that the formation of E2F1-p300/CREB-binding protein-associated factor (P/CAF) complexes is preferentially induced in doxorubicin-treated cells, and that P/CAF acetyltransferase (HAT), but not p300 HAT activity, is required for a significant E2F1 stabilization and accumulation. Our results unveil a differential role of P/CAF and p300 in acetylation-induced stabilization of E2F1, thus supporting a specific role for P/CAF HAT activity in E2F1-dependent apoptosis in response to DNA damage.

Published

2004