Your search keyword '"Glorymar Ibáñez"' showing total 10 results

1. Translational Strategies for Repotrectinib in Neuroblastoma

Author

Nestor Rosales, Andoyo Ndengu, Filemon S. Dela Cruz, Daoqi You, Stephen S. Roberts, Matthew Long, Armaan Siddiquee, Paul Calder, Tara O'Donohue, Andrew L. Kung, Audrey Mauguen, Glorymar Ibáñez, and Diego F. Coutinho

Subjects

Cancer Research, Chemotherapy, Macrocyclic Compounds, business.industry, medicine.medical_treatment, medicine.disease, Article, stat, Mice, Neuroblastoma, Oncology, Cell culture, In vivo, Trk receptor, Cancer research, Animals, Humans, Pyrazoles, Medicine, Cytotoxic T cell, business, Proto-oncogene tyrosine-protein kinase Src

Abstract

Limited clinical data are available regarding the utility of multikinase inhibition in neuroblastoma. Repotrectinib (TPX-0005) is a multikinase inhibitor that targets ALK, TRK, JAK2/STAT, and Src/FAK, which have all been implicated in the pathogenesis of neuroblastoma. We evaluated the preclinical activity of repotrectinib monotherapy and in combination with chemotherapy as a potential therapeutic approach for relapsed/refractory neuroblastoma. In vitro sensitivity to repotrectinib, ensartinib, and cytotoxic chemotherapy was evaluated in neuroblastoma cell lines. In vivo antitumor effect of repotrectinib monotherapy, and in combination with chemotherapy, was evaluated using a genotypically diverse cohort of patient-derived xenograft (PDX) models of neuroblastoma. Repotrectinib had comparable cytotoxic activity across cell lines irrespective of ALK mutational status. Combination with chemotherapy demonstrated increased antiproliferative activity across several cell lines. Repotrectinib monotherapy had notable antitumor activity and prolonged event-free survival compared with vehicle and ensartinib in PDX models (P < 0.05). Repotrectinib plus chemotherapy was superior to chemotherapy alone in ALK-mutant and ALK wild-type PDX models. These results demonstrate that repotrectinib has antitumor activity in genotypically diverse neuroblastoma models, and that combination of a multikinase inhibitor with chemotherapy may be a promising treatment paradigm for translation to the clinic.

Published

2021

2. Validation of a non-oncogene encoded vulnerability to exportin 1 inhibition in pediatric renal tumors

Author

Diego F. Coutinho, Prabhjot S. Mundi, Lianna J. Marks, Chelsey Burke, Michael V. Ortiz, Daniel Diolaiti, Lauren Bird, Kelly L. Vallance, Glorymar Ibáñez, Daoqi You, Matthew Long, Nestor Rosales, Adina Grunn, Andoyo Ndengu, Armaan Siddiquee, Ervin S. Gaviria, Allison R. Rainey, Ladan Fazlollahi, Hajime Hosoi, Andrea Califano, Andrew L. Kung, and Filemon S. Dela Cruz

Subjects

Child, Preschool, Cell Line, Tumor, Humans, General Medicine, Child, Xenograft Model Antitumor Assays, Kidney Neoplasms

Abstract

Malignant rhabdoid tumors (MRTs) and Wilms' tumors (WTs) are rare and aggressive renal tumors of infants and young children comprising ∼5% of all pediatric cancers. MRTs are among the most genomically stable cancers, and although WTs are genomically heterogeneous, both generally lack therapeutically targetable genetic mutations.Comparative protein activity analysis of MRTs (n = 68) and WTs (n = 132) across TCGA and TARGET cohorts, using metaVIPER, revealed elevated exportin 1 (XPO1) inferred activity. In vitro studies were performed on a panel of MRT and WT cell lines to evaluate effects on proliferation and cell-cycle progression following treatment with the selective XPO1 inhibitor selinexor. In vivo anti-tumor activity was assessed in patient-derived xenograft (PDX) models of MRTs and WTs.metaVIPER analysis identified markedly aberrant activation of XPO1 in MRTs and WTs compared with other tumor types. All MRT and most WT cell lines demonstrated baseline, aberrant XPO1 activity with in vitro sensitivity to selinexor via cell-cycle arrest and induction of apoptosis. In vivo, XPO1 inhibitors significantly abrogated tumor growth in PDX models, inducing effective disease control with sustained treatment. Corroborating human relevance, we present a case report of a child with multiply relapsed WTs with prolonged disease control on selinexor.We report on a novel systems-biology-based comparative framework to identify non-genetically encoded vulnerabilities in genomically quiescent pediatric cancers. These results have provided preclinical rationale for investigation of XPO1 inhibitors in an upcoming investigator-initiated clinical trial of selinexor in children with MRTs and WTs and offer opportunities for exploration of inferred XPO1 activity as a potential predictive biomarker for response.This work was funded by CureSearch for Children's Cancer, Alan B. Slifka Foundation, NIH (U01 CA217858, S10 OD012351, and S10 OD021764), Michael's Miracle Cure, Hyundai Hope on Wheels, Cannonball Kids Cancer, Conquer Cancer the ASCO Foundation, Cycle for Survival, Paulie Strong Foundation, and the Grayson Fund.

Published

2022

3. Evaluation of Compound Optical Interference in High-Content Screening

Author

Hakim Djaballah, Glorymar Ibáñez, Christophe Antczak, Bhavneet Bhinder, Constantin Radu, Paul Calder, and David Shum

Subjects

0301 basic medicine, Green Fluorescent Proteins, Biosensing Techniques, Interference (wave propagation), 01 natural sciences, Biochemistry, Fluorescence, Analytical Chemistry, 03 medical and health sciences, Cell Line, Tumor, Humans, Microscopy, Chemistry, 0104 chemical sciences, Chemical screening, High-Throughput Screening Assays, 010404 medicinal & biomolecular chemistry, MicroRNAs, 030104 developmental biology, Pharmaceutical Preparations, Cheminformatics, High-content screening, Molecular Medicine, Biological Assay, MiRNA biogenesis, Biosensor, Biogenesis, Biotechnology, HeLa Cells

Abstract

Compound optical interference remains an inherent problem in chemical screening and has been well documented for biochemical assays and less so for automated microscopy-based assays. It has also been the assumption that the latter should not suffer from such interference because of the washing steps involved in the process, thus eliminating the residual nonspecific compound effects. Instead, these compounds may have no relevance to the actual target, and as such, compound optical interference contributes to a number of false-positives, resulting in a high attrition rate during subsequent follow-up studies. In this report, we analyze the outcome of a high-content screen using enhanced green fluorescent protein as a reporter in a gain-of-function cell-based assay in search of modulators of the micro RNA (miRNA) biogenesis pathway. Using a previously validated image-based biosensor, we screened a diverse library collection of ~315,000 compounds covering natural and synthetic derivatives in which 1130 positives were identified to enhance green fluorescence expression. Lateral confirmation and dose-response studies revealed that all of these compounds were the result of optical interference and not specific inhibition of miRNA biogenesis. Here, we highlight the chemical classes that are susceptible to compound optical interference and discuss their implications in automated microscopy-based assays.

Published

2017

4. Sinefungin Derivatives as Inhibitors and Structure Probes of Protein Lysine Methyltransferase SETD2

Author

Fengling Li, Aiping Dong, Masoud Vedadi, Wenyu Yu, Weihong Zheng, Alena Siarheyeva, Jinrong Min, Gil Blum, Abdellah Allali-Hassani, Glorymar Ibáñez, Peter Brown, Maria F. Amaya, Hong Zeng, Matthieu Schapira, Minkui Luo, Taraneh Hajian, and Hong Wu

Subjects

Models, Molecular, Adenosine, Methyltransferase, Chemistry, Lysine, Histone-Lysine N-Methyltransferase, General Chemistry, Computational biology, Biochemistry, Small molecule, Article, Catalysis, Structure-Activity Relationship, Sinefungin, Colloid and Surface Chemistry, SETD2, Molecular Probes, Humans, Epigenetics, Enzyme Inhibitors, Protein Lysine Methyltransferase

Abstract

Epigenetic regulation is involved in numerous physiological and pathogenic processes. Among the key regulators that orchestrate epigenetic signaling are over 50 human protein lysine methyltransferases (PKMTs). Interrogation of the functions of individual PKMTs can be facilitated by target-specific PKMT inhibitors. Given the emerging need for such small molecules, we envisioned an approach to identify target-specific methyltransferase inhibitors by screening privileged small-molecule scaffolds against diverse methyltransferases. In this work, we demonstrated the feasibility of such an approach by identifying the inhibitors of SETD2. N-propyl sinefungin (Pr-SNF) was shown to interact preferentially with SETD2 by matching the distinct transition-state features of SETD2's catalytically active conformer. With Pr-SNF as a structure probe, we further revealed the dual roles of SETD2's post-SET loop in regulating substrate access through a distinct topological reconfiguration. Privileged sinefungin scaffolds are expected to have broad use as structure and chemical probes of methyltransferases.

Published

2012

5. A High Throughput Scintillation Proximity Imaging Assay for Protein Methyltransferases

Author

David Shum, Constantin Radu, Christophe Antczak, Gil Blum, Bhavneet Bhinder, Hakim Djaballah, Glorymar Ibáñez, and Minkui Luo

Subjects

chemistry.chemical_classification, Streptavidin, Drug discovery, Organic Chemistry, Lysine, Peptide, Histone-Lysine N-Methyltransferase, General Medicine, Methylation, Biology, Small molecule, Article, High-Throughput Screening Assays, Computer Science Applications, chemistry.chemical_compound, chemistry, Biochemistry, Biotinylation, Drug Discovery, Humans, Scintillation Counting, Protein Methyltransferases, Enzyme Inhibitors

Abstract

Protein methyltransferases (PMTs) orchestrate epigenetic modifications through post-translational methylation of various protein substrates including histones. Since dysregulation of this process is widely implicated in many cancers, it is of pertinent interest to screen inhibitors of PMTs, as they offer novel target-based opportunities to discover small molecules with potential chemotherapeutic use. We have thus developed an enzymatic screening strategy, which can be adapted to scintillation proximity imaging assay (SPIA) format, to identify these inhibitors. We took advantage of S-adenosyl-L-[3H-methyl]-methionine availability and monitored the enzymatically catalyzed [3H]-methyl addition on lysine residues of biotinylated peptide substrates. The radiolabeled peptides were subsequently captured by streptavidin coated SPA imaging PS beads. We applied this strategy to four PMTs: SET7/9, SET8, SETD2, and EuHMTase1, and optimized assay conditions to achieve Z' values ranging from 0.48 to 0.91. The robust performance of this SPIA for the four PMTs was validated in a pilot screen of approximately 7,000 compounds. We identified 80 cumulative hits across the four targets. NF279, a suramin analogue, was found to specifically inhibit SET7/9 and SETD2 with IC50 values of 1.9 and 1.1 μ M, respectively. Another identified compound, Merbromin, a topical antiseptic, was classified as a pan-active inhibitor of the four PMTs. These findings demonstrate that our proposed SPIA strategy is generic for multiple PMTs and can be successfully implemented to identify novel and specific inhibitors of PMTs. The specific PMT inhibitors may constitute a new class of anti-proliferative agents for potential therapeutic use.

Published

2012

6. Small-molecule inhibitors of SETD8 with cellular activity

Author

Constantin Radu, Judd C. Rice, David Shum, Xiangjun Rao, Minkui Luo, Glorymar Ibáñez, Hakim Djaballah, and Gil Blum

Subjects

0303 health sciences, Methyltransferase, DNA damage, HEK 293 cells, DNA replication, General Medicine, Histone-Lysine N-Methyltransferase, Biology, Cell cycle, Biochemistry, Small molecule, 3. Good health, High-Throughput Screening Assays, Histone H4, 03 medical and health sciences, 0302 clinical medicine, HEK293 Cells, Transcription (biology), 030220 oncology & carcinogenesis, Molecular Medicine, Humans, Letters, 030304 developmental biology

Abstract

SETD8/SET8/Pr-SET7/KMT5A is the sole protein lysine methyltransferase (PKMT) known to monomethylate lysine 20 of histone H4 in vivo. SETD8's methyltransferase activity has been implicated in many essential cellular processes including DNA replication, DNA damage response, transcription modulation, and cell cycle regulation. Developing SETD8 inhibitors with cellular activity is a key step toward elucidating the diverse roles of SETD8 via convenient pharmacological perturbation. From the hits of a prior high throughput screen (HTS), SPS8I1-3 (NSC663284, BVT948, and ryuvidine) were validated as potent SETD8 inhibitors. These compounds contain different structural motifs and inhibit SETD8 via distinct modes. More importantly, these compounds show cellular activity by suppressing the H4K20me1 mark of SETD8 and recapitulate characteristic S/G2/M-phase cell cycle defects as observed for RNAi-mediated SETD8 knockdown. The commonality of SPS8I1-3 against SETD8, together with their distinct structures and mechanisms for SETD8 inhibition, argues for the collective application of these compounds as SETD8 inhibitors.

Published

2014

7. Discovery of a dicer-independent, cell-type dependent alternate targeting sequence generator: implications in gene silencing & pooled RNAi screens

Author

Mu Li, Hakim Djaballah, Bhavneet Bhinder, Susan Magdaleno, Glorymar Ibáñez, Alexander V. Vlassov, and David Shum

Subjects

Ribonuclease III, Small interfering RNA, Science, Trans-acting siRNA, Computational biology, DEAD-box RNA Helicases, Small hairpin RNA, RNA interference, Genetics, Humans, RNA, Small Interfering, Drosha, Multidisciplinary, Biology and life sciences, biology, Sequence Analysis, RNA, Computational Biology, Gene targeting, Genomics, Functional Genomics, RNA silencing, Genetic interference, Gene Targeting, biology.protein, Medicine, Gene expression, Gene Function, HeLa Cells, Research Article, Dicer

Abstract

There is an acceptance that plasmid-based delivery of interfering RNA always generates the intended targeting sequences in cells, making it as specific as its synthetic counterpart. However, recent studies have reported on cellular inefficiencies of the former, especially in light of emerging gene discordance at inter-screen level and across formats. Focusing primarily on the TRC plasmid-based shRNA hairpins, we reasoned that alleged specificities were perhaps compromised due to altered processing; resulting in a multitude of random interfering sequences. For this purpose, we opted to study the processing of hairpin TRCN#40273 targeting CTTN; which showed activity in a miRNA-21 gain-of-function shRNA screen, but inactive when used as an siRNA duplex. Using a previously described walk-through method, we identified 36 theoretical cleavage variants resulting in 78 potential siRNA duplexes targeting 53 genes. We synthesized and tested all of them. Surprisingly, six duplexes targeting ASH1L, DROSHA, GNG7, PRKCH, THEM4, and WDR92 scored as active. QRT-PCR analysis on hairpin transduced reporter cells confirmed knockdown of all six genes, besides CTTN; revealing a surprising 7 gene-signature perturbation by this one single hairpin. We expanded our qRT-PCR studies to 26 additional cell lines and observed unique knockdown profiles associated with each cell line tested; even for those lacking functional DICER1 gene suggesting no obvious dependence on dicer for shRNA hairpin processing; contrary to published models. Taken together, we report on a novel dicer independent, cell-type dependent mechanism for non-specific RNAi gene silencing we coin Alternate Targeting Sequence Generator (ATSG). In summary, ATSG adds another dimension to the already complex interpretation of RNAi screening data, and provides for the first time strong evidence in support of arrayed screening, and questions the scientific merits of performing pooled RNAi screens, where deconvolution of up to genome-scale pools is indispensable for target identification.

Published

2014

8. Formulating a fluorogenic assay to evaluate S-adenosyl-L-methionine analogues as protein methyltransferase cofactors

Author

Glorymar Ibáñez, Weihong Zheng, Gil Blum, Rui Wang, Caitlin Sengelaub, Kabirul Islam, and Minkui Luo

Subjects

Protein-Arginine N-Methyltransferases, S-Adenosylmethionine, Methyltransferase, CARM1, High-throughput screening, Lysine, Coenzymes, Methylation, Biology, Small molecule, Article, High-Throughput Screening Assays, Biochemistry, Luminescent Measurements, Humans, Protein Methyltransferases, Molecular Biology, Biotechnology

Abstract

Protein methyltransferases (PMTs) catalyze arginine and lysine methylation of diverse histone and nonhistone targets. These posttranslational modifications play essential roles in regulating multiple cellular events in an epigenetic manner. In the recent process of defining PMT targets, S-adenosyl-L-methionine (SAM) analogues have emerged as powerful small molecule probes to label and profile PMT targets. To examine efficiently the reactivity of PMTs and their variants on SAM analogues, we transformed a fluorogenic PMT assay into a ready high throughput screening (HTS) format. The reformulated fluorogenic assay is featured by its uncoupled but more robust character with the first step of accumulation of the commonly-shared reaction byproduct S-adenosyl-L-homocysteine (SAH), followed by SAH-hydrolase-mediated fluorogenic quantification. The HTS readiness and robustness of the assay were demonstrated by its excellent Z′ values of 0.83–0.95 for the so-far-examined 8 human PMTs with SAM as a cofactor (PRMT1, PRMT3, CARM1, SUV39H2, SET7/9, SET8, G9a and GLP1). The fluorogenic assay was further implemented to screen the PMTs against five SAM analogues (allyl-SAM, propargyl-SAM, (E)-pent-2-en-4-ynyl-SAM (EnYn-SAM), (E)-hex-2-en-5-ynyl-SAM (Hey-SAM) and 4-propargyloxy-but-2-enyl-SAM (Pob-SAM)). Among the examined 8 × 5 pairs of PMTs and SAM analogues, native SUV39H2, G9a and GLP1 showed promiscuous activity on allyl-SAM. In contrast, the bulky SAM analogues, such as EnYn-SAM, Hey-SAM and Pob-SAM, are inert toward the panel of human PMTs. These findings therefore provide the useful structure–activity guidance to further evolve PMTs and SAM analogues for substrate labeling. The current assay format is ready to screen methyltransferase variants on structurally-diverse SAM analogues.

Published

2011

9. An enzyme-coupled ultrasensitive luminescence assay for protein methyltransferases

Author

Minkui Luo, Yaritzy M. Astudillo, Jamie L. McBean, and Glorymar Ibáñez

Subjects

Adenosine monophosphate, S-Adenosylmethionine, Methyltransferase, Biophysics, Biochemistry, Sensitivity and Specificity, chemistry.chemical_compound, Histocompatibility Antigens, medicine, Protein methylation, Humans, Luciferase, Protein Methyltransferases, Molecular Biology, Enzyme Assays, chemistry.chemical_classification, Cell Biology, Methylation, Histone-Lysine N-Methyltransferase, Luciferin, Adenosine, Molecular biology, S-Adenosylhomocysteine, Enzyme, chemistry, Luminescent Measurements, medicine.drug

Abstract

Epigenetic regulation through protein posttranslational modifications is essential in development and disease. Among the key chemical modifications is protein methylation carried out by protein methyltransferases (PMTs). Quantitative and sensitive PMT activity assays can provide valuable tools to investigate PMT functions. Here we developed an enzyme-coupled luminescence assay for S-adenosyl-l-methionine (AdoMet/SAM)-based PMTs. In this assay, S-adenosyl-l-homocystine (AdoHcy/SAH), the by-product of PMT-involved methylation, is sequentially converted to adenine, adenosine monophosphate, and then adenosine 5'-triphosphate (ATP) by 5'-methylthio-adenosine/AdoHcy nucleosidase (MTAN), adenine phosphoribosyl transferase (APRT), and pyruvate orthophosphate dikinase (PPDK), respectively. The resultant ATP can be readily quantified with a luciferin/luciferase kit. This assay is featured for its quantitative linear response to AdoHcy and the ultrasensitivity to 0.3 pmol of AdoHcy. With this assay, the kinetic parameters of SET7/9 methylation were characterized and unambiguously support an ordered mechanism with AdoMet binding as the initial step, followed by the substrate binding and the rate-limiting methylation. The luminescence assay is also expected to be generally applicable to many other AdoMet-dependent enzymes. In addition, the mix-and-measure 96-/384-well format of our assay makes it suitable for automation and high throughput. Our enzyme-coupled luminescence assay, therefore, represents a convenient and ultrasensitive approach to examine methyltransferase activities and identify methyltransferase inhibitors.

Published

2009

10. Therapeutic targeting of ATR in alveolar rhabdomyosarcoma

Author

Heathcliff Dorado García, Fabian Pusch, Yi Bei, Jennifer von Stebut, Glorymar Ibáñez, Kristina Guillan, Koshi Imami, Dennis Gürgen, Jana Rolff, Konstantin Helmsauer, Stephanie Meyer-Liesener, Natalie Timme, Victor Bardinet, Rocío Chamorro González, Ian C. MacArthur, Celine Y. Chen, Joachim Schulz, Antje M. Wengner, Christian Furth, Birgit Lala, Angelika Eggert, Georg Seifert, Patrick Hundsoerfer, Marieluise Kirchner, Philipp Mertins, Matthias Selbach, Andrej Lissat, Frank Dubois, David Horst, Johannes H. Schulte, Simone Spuler, Daoqi You, Filemon Dela Cruz, Andrew L. Kung, Kerstin Haase, Michela DiVirgilio, Monika Scheer, Michael V. Ortiz, and Anton G. Henssen

Subjects

Cancer Research, Multidisciplinary, Oncogene Proteins, Fusion, General Physics and Astronomy, General Chemistry, Ataxia Telangiectasia Mutated Proteins, General Biochemistry, Genetics and Molecular Biology, Gene Expression Regulation, Neoplastic, Cardiovascular and Metabolic Diseases, Cell Line, Tumor, Rhabdomyosarcoma, Humans, Paired Box Transcription Factors, Rhabdomyosarcoma, Embryonal, Technology Platforms, Function and Dysfunction of the Nervous System, PAX3 Transcription Factor, Rhabdomyosarcoma, Alveolar

Abstract

Despite advances in multi-modal treatment approaches, clinical outcomes of patients suffering from PAX3-FOXO1 fusion oncogene-expressing alveolar rhabdomyosarcoma (ARMS) remain dismal. Here we show that PAX3-FOXO1-expressing ARMS cells are sensitive to pharmacological ataxia telangiectasia and Rad3 related protein (ATR) inhibition. Expression of PAX3-FOXO1 in muscle progenitor cells is not only sufficient to increase sensitivity to ATR inhibition, but PAX3-FOXO1-expressing rhabdomyosarcoma cells also exhibit increased sensitivity to structurally diverse inhibitors of ATR. Mechanistically, ATR inhibition leads to replication stress exacerbation, decreased BRCA1 phosphorylation and reduced homologous recombination-mediated DNA repair pathway activity. Consequently, ATR inhibitor treatment increases sensitivity of ARMS cells to PARP1 inhibition in vitro, and combined treatment with ATR and PARP1 inhibitors induces complete regression of primary patient-derived ARMS xenografts in vivo. Lastly, a genome-wide CRISPR activation screen (CRISPRa) in combination with transcriptional analyses of ATR inhibitor resistant ARMS cells identifies the RAS-MAPK pathway and its targets, the FOS gene family, as inducers of resistance to ATR inhibition. Our findings provide a rationale for upcoming biomarker-driven clinical trials of ATR inhibitors in patients suffering from ARMS.