Your search keyword '"David A. Egan"' showing total 97 results

1. Small molecules to regulate the GH/IGF1 axis by inhibiting the growth hormone receptor synthesis

Author

Lieke M. van der Velden, Peter Maas, Miranda van Amersfoort, Elpetra P M. Timmermans-Sprang, Anneloes Mensinga, Elisabeth van der Vaart, Fabrice Malergue, Henk Viëtor, Patrick W B. Derksen, Judith Klumperman, Andreas van Agthoven, David A. Egan, Jan A. Mol, and Ger J. Strous

Subjects

GH inhibitor, IGF1 inhibitor, cancer, autocrine, ribosomal synthesis, BM001, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Growth hormone (GH) and insulin‐like growth factor‐1 (IGF1) play an important role in mammalian development, cell proliferation and lifespan. Especially in cases of tumor growth there is an urgent need to control the GH/IGF1 axis. In this study we screened a 38,480-compound library, and in two consecutive rounds of analogues selection, we identified active lead compounds based on the following criteria: inhibition the GH receptor (GHR) activity and its downstream effectors Jak2 and STAT5, and inhibition of growth of breast and colon cancer cells. The most active small molecule (BM001) inhibited both the GH/IGF1 axis and cell proliferation with an IC50 of 10‐30 nM of human cancer cells. BM001 depleted GHR in human lymphoblasts. In preclinical xenografted experiments, BM001 showed a strong decrease in tumor volume in mice transplanted with MDA‐MB‐231 breast cancer cells. Mechanistically, the drug acts on the synthesis of the GHR. Our findings open the possibility to inhibit the GH/IGF1 axis with a small molecule.

Published

2022

2. Small Molecule Inhibitor Targeting CDT1/Geminin Protein Complex Promotes DNA Damage and Cell Death in Cancer Cells

Author

Nikolaos Karantzelis, Michalis Petropoulos, Valeria De Marco, David A. Egan, Alexander Fish, Evangelos Christodoulou, David W. Will, Joe D. Lewis, Anastassis Perrakis, Zoi Lygerou, and Stavros Taraviras

Subjects

AlphaScreen, small molecule inhibitor, high-throughput screening, Geminin, CDT1, cancer, Therapeutics. Pharmacology, RM1-950

Abstract

DNA replication initiation requires the loading of MCM2-7 complexes at the origins of replication during G1. Replication licensing renders chromatin competent for DNA replication and its tight regulation is essential to prevent aberrant DNA replication and genomic instability. CDT1 is a critical factor of licensing and its activity is controlled by redundant mechanisms, including Geminin, a protein inhibitor of CDT1. Aberrant CDT1 and Geminin expression have been shown to promote tumorigenesis in vivo and are also evident in multiple human tumors. In this study, we developed an in vitro AlphaScreen™ high-throughput screening (HTS) assay for the identification of small-molecule inhibitors targeting the CDT1/Geminin protein complex. Biochemical characterization of the most potent compound, AF615, provided evidence of specific, dose-dependent inhibition of Geminin binding to CDT1 both in-vitro and in cells. Moreover, compound AF615 induces DNA damage, inhibits DNA synthesis and reduces viability selectively in cancer cell lines, and this effect is CDT1-dependent. Taken together, our data suggest that AF615 may serve as a useful compound to elucidate the role of CDT1/Geminin protein complex in replication licensing and origin firing as well as a scaffold for further medicinal chemistry optimisation.

Published

2022

3. CD40/anti-CD40 antibody complexes which illustrate agonist and antagonist structural switches

Author

Maria A. Argiriadi, Lorenzo Benatuil, Ievgeniia Dubrovska, David A. Egan, Lei Gao, Amy Greischar, Jennifer Hardman, John Harlan, Ramesh B. Iyer, Russell A. Judge, Marc Lake, Denise C. Perron, Ramkrishna Sadhukhan, Bernhard Sielaff, Silvino Sousa, Rui Wang, and Bradford L. McRae

Subjects

CD40, Crystal structure, Agonist, Antagonist, Antibody, Cytology, QH573-671

Abstract

Abstract Background CD40 is a 48 kDa type I transmembrane protein that is constitutively expressed on hematopoietic cells such as dendritic cells, macrophages, and B cells. Engagement of CD40 by CD40L expressed on T cells results in the production of proinflammatory cytokines, induces T helper cell function, and promotes macrophage activation. The involvement of CD40 in chronic immune activation has resulted in CD40 being proposed as a therapeutic target for a range of chronic inflammatory diseases. CD40 antagonists are currently being explored for the treatment of autoimmune diseases and several anti-CD40 agonist mAbs have entered clinical development for oncological indications. Results To better understand the mode of action of anti-CD40 mAbs, we have determined the x-ray crystal structures of the ABBV-323 (anti-CD40 antagonist, ravagalimab) Fab alone, ABBV-323 Fab complexed to human CD40 and FAB516 (anti-CD40 agonist) complexed to human CD40. These three crystals structures 1) identify the conformational CD40 epitope for ABBV-323 recognition 2) illustrate conformational changes which occur in the CDRs of ABBV-323 Fab upon CD40 binding and 3) develop a structural hypothesis for an agonist/antagonist switch in the LCDR1 of this proprietary class of CD40 antibodies. Conclusions The structure of ABBV-323 Fab demonstrates a unique method for antagonism by stabilizing the proposed functional antiparallel dimer for CD40 receptor via novel contacts to LCDR1, namely residue position R32 which is further supported by a closely related agonist antibody FAB516 which shows only monomeric recognition and no contacts with LCDR1 due to a mutation to L32 on LCDR1. These data provide a structural basis for the full antagonist activity of ABBV-323.

Published

2019

4. Paired image‐ and FACS‐based toxicity assays for high content screening of spheroid‐type tumor cell cultures

Author

Kari Trumpi, David A. Egan, Thomas T. Vellinga, Inne H.M. Borel Rinkes, and Onno Kranenburg

Subjects

Toxicity assay, High-throughput, Spheroid-type tumor cell culture, Biology (General), QH301-705.5

Abstract

Novel spheroid‐type tumor cell cultures directly isolated from patients’ tumors preserve tumor characteristics better than traditionally grown cell lines. However, such cultures are not generally used for high‐throughput toxicity drug screens. In addition, the assays that are commonly used to assess drug‐induced toxicity in such screens usually measure a proxy for cell viability such as mitochondrial activity or ATP‐content per culture well, rather than actual cell death. This generates considerable assay‐dependent differences in the measured toxicity values. To address this problem we developed a robust method that documents drug‐induced toxicity on a per‐cell, rather than on a per‐well basis. The method involves automated drug dispensing followed by paired image‐ and FACS‐based analysis of cell death and cell cycle changes. We show that the two methods generate toxicity data in 96‐well format which are highly concordant. By contrast, the concordance of these methods with frequently used well‐based assays was generally poor. The reported method can be implemented on standard automated microscopes and provides a low‐cost approach for accurate and reproducible high‐throughput toxicity screens in spheroid type cell cultures. Furthermore, the high versatility of both the imaging and FACS platforms allows straightforward adaptation of the high‐throughput experimental setup to include fluorescence‐based measurement of additional cell biological parameters.

Published

2015

5. In vitro induction of alkaline phosphatase levels predicts in vivo bone forming capacity of human bone marrow stromal cells

Author

Henk-Jan Prins, A. Koen Braat, D. Gawlitta, Wouter J.A. Dhert, David A. Egan, Estel Tijssen-Slump, Huipin Yuan, Paul J. Coffer, Henk Rozemuller, and Anton C. Martens

Subjects

Biology (General), QH301-705.5

Abstract

One of the applications of bone marrow stromal cells (BMSCs) that are produced by ex vivo expansion is for use in in vivo bone tissue engineering. Cultured stromal cells are a mixture of cells at different stages of commitment and expansion capability, leading to a heterogeneous cell population that each time can differ in the potential to form in vivo bone. A parameter that predicts for in vivo bone forming capacity is thus far lacking. We employed single colony-derived BMSC cultures to identify such predictive parameters. Using limiting dilution, we have produced sixteen single CFU-F derived BMSC cultures from human bone marrow and found that only five of these formed bone in vivo. The single colony-derived BMSC strains were tested for proliferation, osteogenic-, adipogenic- and chondrogenic differentiation capacity and the expression of a variety of associated markers. The only robust predictors of in vivo bone forming capacity were the induction of alkaline phosphatase, (ALP) mRNA levels and ALP activity during in vitro osteogenic differentiation. The predictive value of in vitro ALP induction was confirmed by analyzing “bulk-cultured” BMSCs from various bone marrow biopsies. Our findings show that in BMSCs, the additional increase in ALP levels over basal levels during in vitro osteogenic differentiation is predictive of in vivo performance.

Published

2014

6. Supplementary Data from High-Throughput Screening Identifies Idasanutlin as a Resensitizing Drug for Venetoclax-Resistant Neuroblastoma Cells

Author

M. Emmy M. Dolman, Jan J. Molenaar, Kelly C. Goldsmith, Jan Koster, Ronald W. Stam, Mark Kerstjens, David A. Egan, Daphne Lelieveld, Linda Schild, Nil A. Schubert, Hunter C. Jonus, Bianca Koopmans, Jasmine Y. Lee, Lindy K. Alles, Laurel T. Bate-Eya, and Lindy Vernooij

Abstract

Supplementary data including supplementary figures S1 to S6 and supplementary tables S1 to S3.

Published

2023

7. Supplementary Materials and Methods from High-Throughput Screening Identifies Idasanutlin as a Resensitizing Drug for Venetoclax-Resistant Neuroblastoma Cells

Author

M. Emmy M. Dolman, Jan J. Molenaar, Kelly C. Goldsmith, Jan Koster, Ronald W. Stam, Mark Kerstjens, David A. Egan, Daphne Lelieveld, Linda Schild, Nil A. Schubert, Hunter C. Jonus, Bianca Koopmans, Jasmine Y. Lee, Lindy K. Alles, Laurel T. Bate-Eya, and Lindy Vernooij

Abstract

Supplementary information on the used materials and methods.

Published

2023

8. Data from High-Throughput Screening Identifies Idasanutlin as a Resensitizing Drug for Venetoclax-Resistant Neuroblastoma Cells

Author

M. Emmy M. Dolman, Jan J. Molenaar, Kelly C. Goldsmith, Jan Koster, Ronald W. Stam, Mark Kerstjens, David A. Egan, Daphne Lelieveld, Linda Schild, Nil A. Schubert, Hunter C. Jonus, Bianca Koopmans, Jasmine Y. Lee, Lindy K. Alles, Laurel T. Bate-Eya, and Lindy Vernooij

Abstract

Neuroblastoma tumors frequently overexpress the anti-apoptotic protein B-cell lymphoma/leukemia 2 (BCL-2). We previously showed that treating BCL-2–dependent neuroblastoma cells with the BCL-2 inhibitor venetoclax results in apoptosis, but unfortunately partial therapy resistance is observed. The current study describes the identification of drugs capable of resensitizing venetoclax-resistant neuroblastoma cells to venetoclax. To examine these effects, venetoclax resistance was induced in BCL-2–dependent neuroblastoma cell lines KCNR and SJNB12 by continuous exposure to high venetoclax concentrations. Non-resistant and venetoclax-resistant neuroblastoma cell lines were exposed to a 209-compound library in the absence and presence of venetoclax to identify compounds that were more effective in the venetoclax-resistant cell lines under venetoclax pressure. Top hits were further validated in combination with venetoclax using BCL-2–dependent neuroblastoma model systems. Overall, high-throughput drug screening identified the MDM2 inhibitor idasanutlin as a promising resensitizing agent for venetoclax-resistant neuroblastoma cell lines. Idasanutlin treatment induced BAX-mediated apoptosis in venetoclax-resistant neuroblastoma cells in the presence of venetoclax, whereas it caused p21-mediated growth arrest in control cells. In vivo combination treatment showed tumor regression and superior efficacy over single-agent therapies in a BCL-2–dependent neuroblastoma cell line xenograft and a patient-derived xenograft. However, xenografts less dependent on BCL-2 were not sensitive to venetoclax–idasanutlin combination therapy. This study demonstrates that idasanutlin can overcome resistance to the BCL-2 inhibitor venetoclax in preclinical neuroblastoma model systems, which supports clinical development of a treatment strategy combining the two therapies.

Published

2023

9. Data from A High-Throughput Pharmaceutical Screen Identifies Compounds with Specific Toxicity against BRCA2-Deficient Tumors

Author

Jos Jonkers, Peter Bouwman, Richard Wade-Martins, David J. Adams, Pauline Edser, Henne Holstege, David A. Egan, Tanya M. Braumuller, Eline van der Burg, Eva Schut, and Bastiaan Evers

Abstract

Purpose: Hereditary breast cancer is partly explained by germline mutations in BRCA1 and BRCA2. Although patients carry heterozygous mutations, their tumors have typically lost the remaining wild-type allele. Selectively targeting BRCA deficiency may therefore constitute an important therapeutic approach. Clinical trials applying this principle are underway, but it is unknown whether the compounds tested are optimal. It is therefore important to identify alternative compounds that specifically target BRCA deficiency and to test new combination therapies to establish optimal treatment strategies.Experimental Design: We did a high-throughput pharmaceutical screen on BRCA2-deficient mouse mammary tumor cells and isogenic controls with restored BRCA2 function. Subsequently, we validated positive hits in vitro and in vivo using mice carrying BRCA2-deficient mammary tumors.Results: Three alkylators—chlorambucil, melphalan, and nimustine—displayed strong and specific toxicity against BRCA2-deficient cells. In vivo, these showed heterogeneous but generally strong BRCA2-deficient antitumor activity, with melphalan and nimustine doing better than cisplatin and the poly-(ADP-ribose)-polymerase inhibitor olaparib (AZD2281) in this small study. In vitro drug combination experiments showed synergistic interactions between the alkylators and olaparib. Tumor intervention studies combining nimustine and olaparib resulted in recurrence-free survival exceeding 330 days in 3 of 5 animals tested.Conclusions: We generated and validated a platform for identification of compounds with specific activity against BRCA2-deficient cells that translates well to the preclinical setting. Our data call for the re-evaluation of alkylators, especially melphalan and nimustine, alone or in combination with the poly-(ADP-ribose)-polymerase inhibitors, for the treatment of breast cancers with a defective BRCA pathway. Clin Cancer Res; 16(1); 99–108

Published

2023

10. Identification of lysosome‐targeting drugs with anti‐inflammatory activity as potential invasion inhibitors of treatment resistant HER2 positive cancers

Author

Marja Jäättelä, David A. Egan, Christoffel Dinant, Tiina Naumanen Dietrich, Inger Ødum Nielsen, Maria Postol, Kenji Maeda, Siri Amanda Tvingsholm, Tuula Kallunki, Malene Hansen, Pietri Puustinen, and Robert Strauss

Subjects

Cancer Research, Anti‐inflammatory activity, Auranofin, Receptor, ErbB-2, Lysosome targeting drug, Anti-Inflammatory Agents, Antineoplastic Agents, Breast Neoplasms, Mice, SCID, Tumor spheroid, Lapatinib, Breast cancer, Mice, Inbred NOD, Trastuzumab, Cell Line, Tumor, Drug multipurposing, Autophagy, medicine, Animals, Humans, Neoplasm Invasiveness, skin and connective tissue diseases, neoplasms, HER2/ErbB2, Mice, Knockout, business.industry, Cancer, General Medicine, Invasive growth, Tumor organoid, medicine.disease, Xenograft Model Antitumor Assays, Oncology, Drug Resistance, Neoplasm, Cancer cell, MCF-7 Cells, Cancer research, Molecular Medicine, Original Article, Female, Lysosomes, Ovarian cancer, business, medicine.drug

Abstract

Purpose Most HER2 positive invasive cancers are either intrinsic non-responsive or develop resistance when treated with 1st line HER2 targeting drugs. Both 1st and 2nd line treatments of HER2 positive cancers are aimed at targeting the HER2 receptor directly, thereby strongly limiting the treatment options of HER2/ErbB2 inhibition resistant invasive cancers. Methods We used phenotypic high throughput microscopy screening to identify efficient inhibitors of ErbB2-induced invasion using 1st line HER2 inhibitor trastuzumab- and pertuzumab-resistant, p95-ErbB2 expressing breast cancer cells in conjunction with the Prestwick Chemical Library®. The screening entailed a drug’s ability to inhibit ErbB2-induced, invasion-promoting positioning of lysosomes at the cellular periphery, a phenotype that defines their invasiveness. In addition, we used high throughput microscopy and biochemical assays to assess the effects of the drugs on lysosomal membrane permeabilization (LMP) and autophagy, two features connected to cancer treatment. Using 2nd line HER2 inhibitor lapatinib resistant 3-dimensional model systems, we assessed the effects of the drugs on ErbB2 positive breast cancer spheroids and developed a high-throughput invasion assay for HER2 positive ovarian cancer organoids for further evaluation. Results We identified Auranofin, Colchicine, Monensin, Niclosamide, Podophyllotoxin, Quinacrine and Thiostrepton as efficient inhibitors of invasive growth of 2nd line HER2 inhibitor lapatinib resistant breast cancer spheroids and ovarian cancer organoids. We classified these drugs into four groups based on their ability to target lysosomes by inducing autophagy and/or LMP, i.e., drugs inducing early LMP, early autophagy with late LMP, late LMP, or neither. Conclusions Our results indicate that targetable lysosome-engaging cellular pathways downstream of ErbB2 contribute to invasion. They support lysosomal trafficking as an attractive target for therapy aiming at preventing the spreading of cancer cells. Since these drugs additionally possess anti-inflammatory activities, they could serve as multipurpose drugs simultaneously targeting infection/inflammation and cancer spreading.

Published

2021

11. HTS-IA: High Throughput Screening Information Architecture for Genomics.

Author

Wienand A. Omta, David A. Egan, Judith Klumperman, Marco R. Spruit, and Sjaak Brinkkemper

Published

2013

12. Targeting mutant RAS in patient-derived colorectal cancer organoids by combinatorial drug screening

Author

Carla S Verissimo, René M Overmeer, Bas Ponsioen, Jarno Drost, Sander Mertens, Ingrid Verlaan-Klink, Bastiaan van Gerwen, Marieke van der Ven, Marc van de Wetering, David A Egan, René Bernards, Hans Clevers, Johannes L Bos, and Hugo J Snippert

Subjects

organoids, colorectal cancer, targeted therapy, KRAS, Medicine, Science, Biology (General), QH301-705.5

Abstract

Colorectal cancer (CRC) organoids can be derived from almost all CRC patients and therefore capture the genetic diversity of this disease. We assembled a panel of CRC organoids carrying either wild-type or mutant RAS, as well as normal organoids and tumor organoids with a CRISPR-introduced oncogenic KRAS mutation. Using this panel, we evaluated RAS pathway inhibitors and drug combinations that are currently in clinical trial for RAS mutant cancers. Presence of mutant RAS correlated strongly with resistance to these targeted therapies. This was observed in tumorigenic as well as in normal organoids. Moreover, dual inhibition of the EGFR-MEK-ERK pathway in RAS mutant organoids induced a transient cell-cycle arrest rather than cell death. In vivo drug response of xenotransplanted RAS mutant organoids confirmed this growth arrest upon pan-HER/MEK combination therapy. Altogether, our studies demonstrate the potential of patient-derived CRC organoid libraries in evaluating inhibitors and drug combinations in a preclinical setting.

Published

2016

13. PJM: Probabilistic Risk Assessment for Spare Transformer Planning

Author

Hong Chen, David M. Egan, Kenneth Seiler, Michael E. Bryson, and Frederick S. S. Bresler

Published

2022

14. CD40/anti-CD40 antibody complexes which illustrate agonist and antagonist structural switches

Author

Ramesh Iyer, Ramkrishna Sadhukhan, Amy Greischar, Rui Wang, Jennifer Hardman, Denise C. Perron, B. Sielaff, Maria A. Argiriadi, Ievgeniia Dubrovska, Russell A. Judge, John Harlan, David A. Egan, Lei Gao, Marc R. Lake, Bradford L. McRae, Lorenzo Benatuil, and Silvino Sousa

Subjects

Models, Molecular, Agonist, medicine.drug_class, Static Electricity, Antigen-Antibody Complex, Epitope, Proinflammatory cytokine, Immunoglobulin Fab Fragments, medicine, CD40, Humans, CD40 Antigens, lcsh:QH573-671, Receptor, Molecular Biology, Antibody, biology, Chemistry, lcsh:Cytology, Crystal structure, Antagonist, Antibodies, Monoclonal, hemic and immune systems, Cell Biology, T helper cell, Cell biology, HEK293 Cells, medicine.anatomical_structure, biology.protein, Signal Transduction, Research Article

Abstract

Background CD40 is a 48 kDa type I transmembrane protein that is constitutively expressed on hematopoietic cells such as dendritic cells, macrophages, and B cells. Engagement of CD40 by CD40L expressed on T cells results in the production of proinflammatory cytokines, induces T helper cell function, and promotes macrophage activation. The involvement of CD40 in chronic immune activation has resulted in CD40 being proposed as a therapeutic target for a range of chronic inflammatory diseases. CD40 antagonists are currently being explored for the treatment of autoimmune diseases and several anti-CD40 agonist mAbs have entered clinical development for oncological indications. Results To better understand the mode of action of anti-CD40 mAbs, we have determined the x-ray crystal structures of the ABBV-323 (anti-CD40 antagonist, ravagalimab) Fab alone, ABBV-323 Fab complexed to human CD40 and FAB516 (anti-CD40 agonist) complexed to human CD40. These three crystals structures 1) identify the conformational CD40 epitope for ABBV-323 recognition 2) illustrate conformational changes which occur in the CDRs of ABBV-323 Fab upon CD40 binding and 3) develop a structural hypothesis for an agonist/antagonist switch in the LCDR1 of this proprietary class of CD40 antibodies. Conclusions The structure of ABBV-323 Fab demonstrates a unique method for antagonism by stabilizing the proposed functional antiparallel dimer for CD40 receptor via novel contacts to LCDR1, namely residue position R32 which is further supported by a closely related agonist antibody FAB516 which shows only monomeric recognition and no contacts with LCDR1 due to a mutation to L32 on LCDR1. These data provide a structural basis for the full antagonist activity of ABBV-323. Electronic supplementary material The online version of this article (10.1186/s12860-019-0213-4) contains supplementary material, which is available to authorized users.

Published

2019

15. Identification of Selective Dual ROCK1 and ROCK2 Inhibitors Using Structure-Based Drug Design

Author

Adrian D. Hobson, Russell A. Judge, Ana L. Aguirre, Brian S. Brown, Yifang Cui, Ping Ding, Eric Dominguez, Enrico DiGiammarino, David A. Egan, Gail M. Freiberg, Sujatha M. Gopalakrishnan, Christopher M. Harris, Marie P. Honore, Karen L. Kage, Nicolas J. Kapecki, Christopher Ling, Junli Ma, Helmut Mack, Mulugeta Mamo, Stefan Maurus, Bradford McRae, Nigel S. Moore, Bernhard K. Mueller, Reinhold Mueller, Marian T. Namovic, Kaushal Patel, Steve D. Pratt, C. Brent Putman, Kara L. Queeney, Kathy K. Sarris, Lisa M. Schaffter, Vincent Stoll, Anil Vasudevan, Lei Wang, Lu Wang, William Wirthl, and Kimberly Yach

Subjects

0301 basic medicine, rho-Associated Kinases, Cytochrome P-450 CYP2C9 Inhibitors, Drug Evaluation, Preclinical, Administration, Oral, Biological Availability, Crystallography, X-Ray, Mice, Inbred C57BL, Rats, Sprague-Dawley, Structure-Activity Relationship, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Drug Design, Optic Nerve Injuries, 030220 oncology & carcinogenesis, Drug Discovery, Animals, Cytochrome P-450 CYP3A Inhibitors, Humans, Molecular Medicine, Protein Kinase Inhibitors, Half-Life

Abstract

A HTS campaign identified compound 1, an excellent hit-like molecule to initiate medicinal chemistry efforts to optimize a dual ROCK1 and ROCK2 inhibitor. Substitution (2-Cl, 2-NH

Published

2018

16. Epigenetic drug screen identifies the histone deacetylase inhibitor NSC3852 as a potential novel drug for the treatment of pediatric acute myeloid leukemia

Author

Marije Bartels, Edwin Sonneveld, Paul J. Coffer, Daphne Lelieveld, David A. Egan, Anita M.A.P. Govers, C. Michel Zwaan, Caroline R.M. Wiggers, Pediatrics, and Ophthalmology

Subjects

Myeloid, Apoptosis, epigenetic treatment, Drug Screening Assays, Leukemia, Megakaryoblastic, Acute/drug therapy, Pediatrics, Epigenesis, Genetic, Acute megakaryoblastic leukemia, 0302 clinical medicine, Immunophenotyping, Neutrophil differentiation, Leukemia, Megakaryoblastic, Acute, hemic and lymphatic diseases, Tumor Cells, Cultured, Non-U.S. Gov't, Leukemoid Reaction/drug therapy, Child, Leukemia, Cultured, Hematology, Research Support, Non-U.S. Gov't, HDACi, Histone deacetylase inhibitor, Myeloid leukemia, Prognosis, Perinatology, Tumor Cells, and Child Health, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Down Syndrome/drug therapy, Oncology, 030220 oncology & carcinogenesis, Hydroxyquinolines, Nitroso Compounds, Megakaryoblastic, medicine.medical_specialty, Down syndrome, Histone Deacetylases/chemistry, medicine.drug_class, Leukemia, Myeloid, Acute/drug therapy, Antitumor/methods, Drug Screening Assays, Antitumor/methods, Research Support, Histone Deacetylases, Leukemoid Reaction, 03 medical and health sciences, Genetic, NSC3852, Internal medicine, DS-AMKL, Journal Article, medicine, Acute/drug therapy, Humans, Pediatrics, Perinatology, and Child Health, pediatric AML, Cell Proliferation, business.industry, Hydroxyquinolines/pharmacology, medicine.disease, High-Throughput Screening Assays, Histone Deacetylase Inhibitors, Pediatrics, Perinatology and Child Health, Cancer research, Nitroso Compounds/pharmacology, Down Syndrome, Drug Screening Assays, Antitumor, business, Histone Deacetylase Inhibitors/pharmacology, Epigenesis, 030215 immunology

Abstract

Background Acute myeloid leukemia (AML) is a heterogeneous disease regarding morphology, immunophenotyping, genetic abnormalities, and clinical behavior. The overall survival rate of pediatric AML is 60% to 70%, and has not significantly improved over the past two decades. Children with Down syndrome (DS) are at risk of developing acute megakaryoblastic leukemia (AMKL), which can be preceded by a transient myeloproliferative disorder during the neonatal period. Intensification of current treatment protocols is not feasible due to already high treatment‐related morbidity and mortality. Instead, more targeted therapies with less severe side effects are highly needed. Procedure To identify potential novel therapeutic targets for myeloid disorders in children, including DS‐AMKL and non‐DS‐AML, we performed an unbiased compound screen of 80 small molecules targeting epigenetic regulators in three pediatric AML cell lines that are representative for different subtypes of pediatric AML. Three candidate compounds were validated and further evaluated in normal myeloid precursor cells during neutrophil differentiation and in (pre‐)leukemic pediatric patient cells. Results Candidate drugs LMK235, NSC3852, and bromosporine were effective in all tested pediatric AML cell lines with antiproliferative, proapoptotic, and differentiation effects. Out of these three compounds, the pan‐histone deacetylase inhibitor NSC3852 specifically induced growth arrest and apoptosis in pediatric AML cells, without disrupting normal neutrophil differentiation. Conclusion NSC3852 is a potential candidate drug for further preclinical testing in pediatric AML and DS‐AMKL.

Published

2019

17. Intra-tumour diversification in colorectal cancer at the single-cell level

Author

Nobuo Sasaki, Niels Smakman, Joost van Gorp, Howard Lightfoot, Sebastian Grossmann, Marc van de Wetering, Matthew D. Young, Ludmil B. Alexandrov, Henry Lee-Six, David A. Egan, Hans Clevers, Stephen J. Gamble, Michael R. Stratton, Sam Behjati, Apollo Pronk, Thomas J. Mitchell, Peter J. Campbell, Sophie F. Roerink, Elizabeth Anderson, Chris Alder, Mitchell, Thomas [0000-0003-0761-9503], Apollo - University of Cambridge Repository, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

0301 basic medicine, Evolution, Colorectal cancer, DNA Mutational Analysis, Antineoplastic Agents, Biology, medicine.disease_cause, Evolution, Molecular, 03 medical and health sciences, Germline mutation, Single-cell analysis, Mutation Rate, medicine, Humans, Intestinal Mucosa, General, Cell Proliferation, Neoplastic, Mutation, Multidisciplinary, Molecular, Cancer, Colorectal Neoplasms/drug therapy, DNA Methylation, medicine.disease, Clone Cells, Gene Expression Regulation, Neoplastic, Intestines, Organoids, Clone Cells/drug effects, 030104 developmental biology, Gene Expression Regulation, Cancer cell, DNA methylation, Cancer research, Neoplastic cell, Organoids/cytology, Single-Cell Analysis, Colorectal Neoplasms, Transcriptome, Antineoplastic Agents/pharmacology, Intestinal Mucosa/metabolism, Intestines/cytology

Abstract

Every cancer originates from a single cell. During expansion of the neoplastic cell population, individual cells acquire genetic and phenotypic differences from each other. Here, to investigate the nature and extent of intra-tumour diversification, we characterized organoids derived from multiple single cells from three colorectal cancers as well as from adjacent normal intestinal crypts. Colorectal cancer cells showed extensive mutational diversification and carried several times more somatic mutations than normal colorectal cells. Most mutations were acquired during the final dominant clonal expansion of the cancer and resulted from mutational processes that are absent from normal colorectal cells. Intra-tumour diversification of DNA methylation and transcriptome states also occurred; these alterations were cell-autonomous, stable, and followed the phylogenetic tree of each cancer. There were marked differences in responses to anticancer drugs between even closely related cells of the same tumour. The results indicate that colorectal cancer cells experience substantial increases in somatic mutation rate compared to normal colorectal cells, and that genetic diversification of each cancer is accompanied by pervasive, stable and inherited differences in the biological states of individual cancer cells.

Published

2018

18. A Living Biobank of Breast Cancer Organoids Captures Disease Heterogeneity

Author

Harry Begthel, Fleur Weeber, Lodewyk F. A. Wessels, Marieke van der Ven, Robert G.J. Vries, Jeroen Korving, Karin Wind, Alexandra A. Duarte, Robert F Ernst, Anjali Vanita Balgobind, Isaac J. Nijman, Ruben van Boxtel, Sylvia F. Boj, Edwin Cuppen, Gergana Bounova, Sven Rottenberg, Arne Van Hoeck, Paul J. van Diest, Francis Blokzijl, Daphne Lelieveld, David A. Egan, Vittoria Zinzalla, Ana Gracanin, Emile E. Voest, Joep de Ligt, Oded Kopper, Hans Clevers, Marlous Hoogstraat, Ewa Gogola, Norman Sachs, Jürgen Moll, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

0301 basic medicine, medicine.medical_specialty, precision medicine, Disease, Biology, Biochemistry, General Biochemistry, Genetics and Molecular Biology, triple negative, 03 medical and health sciences, Breast cancer, breast cancer, basal, medicine, Organoid, Journal Article, Copy-number variation, 610 Medicine & health, organoids, luminal, 630 Agriculture, Genetic heterogeneity, Biochemistry, Genetics and Molecular Biology(all), medicine.disease, Biobank, biobank, 030104 developmental biology, Drug development, Cancer research, 570 Life sciences, biology, Histopathology, Genetics and Molecular Biology(all)

Abstract

Breast cancer (BC) comprises multiple distinct subtypes that differ genetically, pathologically, and clinically. Here, we describe a robust protocol for long-term culturing of human mammary epithelial organoids. Using this protocol, >100 primary and metastatic BC organoid lines were generated, broadly recapitulating the diversity of the disease. BC organoid morphologies typically matched the histopathology, hormone receptor status, and HER2 status of the original tumor. DNA copy number variations as well as sequence changes were consistent within tumor-organoid pairs and largely retained even after extended passaging. BC organoids furthermore populated all major gene-expression-based classification groups and allowed in vitro drug screens that were consistent with in vivo xeno-transplantations and patient response. This study describes a representative collection of well-characterized BC organoids available for cancer research and drug development, as well as a strategy to assess in vitro drug response in a personalized fashion. The heterogeneity of breast cancer subtypes can be captured using organoid cultures that can facilitate drug screens that corroborate with patient responses.

Published

2018

19. A novel microscopy-based high-throughput screening method to identify proteins that regulate global histone modification levels

Author

David A. Egan, Bas Castelijns, Michiel Vermeulen, Daphne Lelieveld, Hetty A.A.M. van Teeffelen, H. Th. Marc Timmers, F. M. van Schaik, Petra de Graaf, Philip Lijnzaad, and Roy Baas

Subjects

Histone-modifying enzymes, Biology, Methylation, Biochemistry, Chromatin remodeling, Cell Line, Epigenesis, Genetic, Analytical Chemistry, Histones, Histone H2A, Humans, Histone code, ChIA-PET, Epigenomics, Genetics, Microscopy, Proteomics and Chromatin Biology, Lysine, Proteins, Chromatin, High-Throughput Screening Assays, Cell biology, ChIP-sequencing, Molecular Medicine, Protein Processing, Post-Translational, Protein Binding, Biotechnology

Abstract

Posttranslational modifications of histones play an important role in the regulation of gene expression and chromatin structure in eukaryotes. The balance between chromatin factors depositing (writers) and removing (erasers) histone marks regulates the steady-state levels of chromatin modifications. Here we describe a novel microscopy-based screening method to identify proteins that regulate histone modification levels in a high-throughput fashion. We named our method CROSS, for Chromatin Regulation Ontology SiRNA Screening. CROSS is based on an siRNA library targeting the expression of 529 proteins involved in chromatin regulation. As a proof of principle, we used CROSS to identify chromatin factors involved in histone H3 methylation on either lysine-4 or lysine-27. Furthermore, we show that CROSS can be used to identify chromatin factors that affect growth in cancer cell lines. Taken together, CROSS is a powerful method to identify the writers and erasers of novel and known chromatin marks and facilitates the identification of drugs targeting epigenetic modifications.

Published

2014

20. HTS-IA

Author

Judith Klumperman, Wienand A. Omta, Marco Spruit, David A. Egan, and Sjaak Brinkkemper

Subjects

Information Systems and Management, Database, business.industry, Relational database, Process (engineering), Computer science, Information architecture, Method engineering, Interoperability, Medicine (miscellaneous), computer.software_genre, Interchangeability, Management information systems, business, Software engineering, computer, Throughput (business), Information Systems

Abstract

This paper describes a high throughput screening architecture for functional genomics screens that use high content methods. Case studies were performed using the Yin case study approach. Additionally a detailed process model is provided using a Method Engineering approach. This study shows that current information architecture lacks interchangeability and functionality. Data enrichment is carried out manually, and software is still deficient in term of interoperability so as to be able to successfully gather data from various external sources. This begs for the growing need of a real integrated laboratory information management system both in academia as well as small-to-medium-sized commercial organizations. Current solutions are designed primarily for clinical samples and lack functionality for larger libraries. A solution should give users the ability to create data pipelines that allow processes to be easily reflected in a relational database.

Published

2013

21. Targeting mutant RAS in patient-derived colorectal cancer organoids by combinatorial drug screening

Author

Hugo J. Snippert, Marc van de Wetering, Johannes L. Bos, Marieke van der Ven, René M. Overmeer, Jarno Drost, David A. Egan, Bastiaan van Gerwen, Hans Clevers, Carla S Verissimo, René Bernards, Sander Mertens, Ingrid Verlaan-Klink, Bas Ponsioen, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

0301 basic medicine, Colorectal cancer, QH301-705.5, medicine.medical_treatment, Science, Drug Evaluation, Preclinical, Antineoplastic Agents, colorectal cancer, Biology, Bioinformatics, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Targeted therapy, 03 medical and health sciences, Genome editing, Organoid, medicine, Journal Article, KRAS, Humans, Clustered Regularly Interspaced Short Palindromic Repeats, Biology (General), organoids, Cancer Biology, Recombination, Genetic, General Immunology and Microbiology, General Neuroscience, Cancer, General Medicine, medicine.disease, targeted therapy, 030104 developmental biology, Developmental Biology and Stem Cells, Cancer cell, ras Proteins, Medicine, Mutant Proteins, Stem cell, Colorectal Neoplasms, Research Article, Human

Abstract

Colorectal cancer (CRC) organoids can be derived from almost all CRC patients and therefore capture the genetic diversity of this disease. We assembled a panel of CRC organoids carrying either wild-type or mutant RAS, as well as normal organoids and tumor organoids with a CRISPR-introduced oncogenic KRAS mutation. Using this panel, we evaluated RAS pathway inhibitors and drug combinations that are currently in clinical trial for RAS mutant cancers. Presence of mutant RAS correlated strongly with resistance to these targeted therapies. This was observed in tumorigenic as well as in normal organoids. Moreover, dual inhibition of the EGFR-MEK-ERK pathway in RAS mutant organoids induced a transient cell-cycle arrest rather than cell death. In vivo drug response of xenotransplanted RAS mutant organoids confirmed this growth arrest upon pan-HER/MEK combination therapy. Altogether, our studies demonstrate the potential of patient-derived CRC organoid libraries in evaluating inhibitors and drug combinations in a preclinical setting. DOI: http://dx.doi.org/10.7554/eLife.18489.001, eLife digest Recent technical advances mean that miniature replicas of many tissues can be grown in the laboratory. These so-called organoids provide scientists with model systems that are not as limited as simple, two-dimensional sheets of cells growing in a petri dish, and less labor and resource intensive than studies using laboratory animals. In particular, organoids grown from tumor cells from cancer patients have been suggested as having numerous advantages over both laboratory-grown cancer cells and mice when it comes to testing potential new anticancer drugs. Mutations in a gene called KRAS are common in many types of cancer including colon cancer. Tumors with these mutations are difficult to treat and so far virtually all attempts to generate compounds that selectively interfere with the KRAS protein encoded by the mutant gene have failed. Instead, drugs that indirectly inhibit this protein’s effects by targeting other proteins in the same signaling pathway are currently being tested on patients. However, there is still a need for better ways to pre-test whether these drugs will be effective in humans without having to expose the patient to side effects or an ineffective drug. Now, Verissimo, Overmeer, Ponsioen et al. have tested clinically-used KRAS pathway inhibitors and drug combinations against normal colon organoids and colon cancer organoids derived from patients with colon cancer. Gene editing techniques were used to introduce KRAS mutations into some of the normal organoids grown from healthy tissue, and into cancer organoids grown from tumors that had a normal copy of the KRAS gene. In all cases, only those organoids with mutant forms of the KRAS gene were resistant to the treatments. Furthermore, when organoids with the KRAS mutation were treated with some combination therapies that are currently being tested in clinical trials, the tumors stopped growing but the tumor cells failed to die. Similar drug treatments on mice carrying human colon cancer organoids confirmed these results, which is in line with previous studies where tumor tissue from human patients was transplanted into mice. These findings show that collections of tumor organoids from multiple patients could help researchers to quickly identify and optimize targeted anticancer therapies before they are incorporated into clinical trials. In the future, clinical studies are needed to verify how accurately the testing of cancer drugs on organoids predicts whether the drug will or will not work in patients. DOI: http://dx.doi.org/10.7554/eLife.18489.002

Published

2016

22. Author response: Targeting mutant RAS in patient-derived colorectal cancer organoids by combinatorial drug screening

Author

Ingrid Verlaan-Klink, Sander Mertens, Bastiaan van Gerwen, René M. Overmeer, Marc van de Wetering, Marieke van der Ven, Johannes L. Bos, Hugo J. Snippert, Jarno Drost, David A. Egan, Bas Ponsioen, Carla S Verissimo, Hans Clevers, and René Bernards

Subjects

Drug, business.industry, Colorectal cancer, media_common.quotation_subject, Mutant RAS, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Organoid, Cancer research, Medicine, In patient, business, 030215 immunology, media_common

Published

2016

23. Screening of a Library of FDA-Approved Drugs Identifies Several Enterovirus Replication Inhibitors That Target Viral Protein 2C

Author

Wienand A. Omta, Bruno Canard, Lonneke van der Linden, David A. Egan, Rachel Ulferts, Bruno Coutard, Maria J. Maté, Frank J. M. van Kuppeveld, S. Matthijn de Boer, Daphne Lelieveld, Julie Lichière, Heyrhyoung Lyoo, Lisa Bauer, Architecture et fonction des macromolécules biologiques (AFMB), Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU)-Institut National de la Recherche Agronomique (INRA), Institut National de la Recherche Agronomique (INRA)-Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS), AII - Amsterdam institute for Infection and Immunity, and Medical Microbiology and Infection Prevention

Subjects

0301 basic medicine, Rhinovirus, Viral protein, viruses, Carbazoles, Dibucaine, Viral Nonstructural Proteins, medicine.disease_cause, Virus Replication, Antiviral Agents, Chemical library, 03 medical and health sciences, chemistry.chemical_compound, Viral Proteins, Fluoxetine, Formoterol Fumarate, medicine, Journal Article, Humans, Pharmacology (medical), ComputingMilieux_MISCELLANEOUS, Enterovirus, Pharmacology, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], business.industry, Pirlindole, virus diseases, Clopenthixol, Virology, [SDV.BIBS]Life Sciences [q-bio]/Quantitative Methods [q-bio.QM], In vitro, 3. Good health, Zuclopenthixol, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biomolecules [q-bio.BM], 030104 developmental biology, Infectious Diseases, chemistry, Formoterol, business, Carrier Proteins, medicine.drug, HeLa Cells

Abstract

Enteroviruses (EVs) represent many important pathogens of humans. Unfortunately, no antiviral compounds currently exist to treat infections with these viruses. We screened the Prestwick Chemical Library, a library of approved drugs, for inhibitors of coxsackievirus B3, identified pirlindole as a potent novel inhibitor, and confirmed the inhibitory action of dibucaine, zuclopenthixol, fluoxetine, and formoterol. Upon testing of viruses of several EV species, we found that dibucaine and pirlindole inhibited EV-B and EV-D and that dibucaine also inhibited EV-A, but none of them inhibited EV-C or rhinoviruses (RVs). In contrast, formoterol inhibited all enteroviruses and rhinoviruses tested. All compounds acted through the inhibition of genome replication. Mutations in the coding sequence of the coxsackievirus B3 (CV-B3) 2C protein conferred resistance to dibucaine, pirlindole, and zuclopenthixol but not formoterol, suggesting that 2C is the target for this set of compounds. Importantly, dibucaine bound to CV-B3 protein 2C in vitro , whereas binding to a 2C protein carrying the resistance mutations was reduced, providing an explanation for how resistance is acquired.

Published

2016

24. Identification of F-box only protein 7 as a negative regulator of NF-kappaB signalling

Author

Roderick L. Beijersbergen, Hendrik J. Kuiken, David A. Egan, Annette M.G. Dirac, Heike Laman, René Bernards, Laman, Heike [0000-0002-6089-171X], and Apollo - University of Cambridge Repository

Subjects

Immunoblotting, NF-κB signalling, Biology, Ubiquitin-conjugating enzyme, F-box protein, Inhibitor of Apoptosis Proteins, RNA interference, Ubiquitin, Humans, Immunoprecipitation, RNA, Small Interfering, FBXO7, regulatory ubiquitination, Transcription factor, Adaptor Proteins, Signal Transducing, Tumor Necrosis Factor-alpha, F-Box Proteins, NF-kappa B, Ubiquitination, RNA-Binding Proteins, Signal transducing adaptor protein, Original Articles, Cell Biology, NFKB1, Molecular biology, Cell biology, cIAP1, Nuclear Pore Complex Proteins, HEK293 Cells, Gene Expression Regulation, siRNA, biology.protein, Molecular Medicine, Signal transduction, Cullin, Signal Transduction

Abstract

The nuclear factor κB (NF-κB) signalling pathway controls important cellular events such as cell proliferation, differentiation, apoptosis and immune responses. Pathway activation occurs rapidly upon TNFα stimulation and is highly dependent on ubiquitination events. Using cytoplasmic to nuclear translocation of the NF-κB transcription factor family member p65 as a read-out, we screened a synthetic siRNA library targeting enzymes involved in ubiquitin conjugation and de-conjugation for modifiers of regulatory ubiquitination events in NF-κB signalling. We identified F-box protein only 7 (FBXO7), a component of Skp, Cullin, F-box (SCF)-ubiquitin ligase complexes, as a negative regulator of NF-κB signalling. F-box protein only 7 binds to, and mediates ubiquitin conjugation to cIAP1 and TRAF2, resulting in decreased RIP1 ubiquitination and lowered NF-κB signalling activity.

Published

2012

25. A Genome-wide multidimensional RNAi screen reveals pathways controlling MHC class II antigen presentation

Author

Tineke van den Hoorn, Rutger Hengeveld, Lennert Janssen, Mark J. Bakker, David A. Egan, Huib Ovaa, Peter Cresswell, Coenraad Kuijl, Roderick L. Beijersbergen, Petra Paul, Marieke van Ham, Marlieke L.M. Jongsma, Jacques Neefjes, Anja ten Brinke, Laboratory for General Clinical Chemistry, Landsteiner Laboratory, AII - Inflammatory diseases, and AII - Infectious diseases

Subjects

MHC class II, Antigen Presentation, biology, Antigen processing, Effector, Biochemistry, Genetics and Molecular Biology(all), Antigen presentation, Histocompatibility Antigens Class II, Autoimmunity, chemical and pharmacologic phenomena, Dendritic Cells, Myosins, Actin cytoskeleton, General Biochemistry, Genetics and Molecular Biology, Actins, Cell biology, MHC class II antigen, Immune system, Myosin, biology.protein, Humans, RNA Interference, Genome-Wide Association Study

Abstract

SummaryMHC class II molecules (MHC-II) present peptides to T helper cells to facilitate immune responses and are strongly linked to autoimmune diseases. To unravel processes controlling MHC-II antigen presentation, we performed a genome-wide flow cytometry-based RNAi screen detecting MHC-II expression and peptide loading followed by additional high-throughput assays. All data sets were integrated to answer two fundamental questions: what regulates tissue-specific MHC-II transcription, and what controls MHC-II transport in dendritic cells? MHC-II transcription was controlled by nine regulators acting in feedback networks with higher-order control by signaling pathways, including TGFβ. MHC-II transport was controlled by the GTPase ARL14/ARF7, which recruits the motor myosin 1E via an effector protein ARF7EP. This complex controls movement of MHC-II vesicles along the actin cytoskeleton in human dendritic cells (DCs). These genome-wide systems analyses have thus identified factors and pathways controlling MHC-II transcription and transport, defining targets for manipulation of MHC-II antigen presentation in infection and autoimmunity.

Published

2011

26. Abstract 2630: Preclinical identification of Venetoclax combination strategies with Idasanutlin, CUDC-907, Prexasertib or Talazoparib for neuroblastoma treatment

Author

Bianca Koopmans, Lindy Vernooij, Laurel T. Bate-Eya, Jan J. Molenaar, M. Emmy M. Dolman, Ronald W. Stam, Daphne Lelieveld, Mark Kerstjens, Anke H. W. Essing, Huib N. Caron, David A. Egan, and Lindy K. Alles

Subjects

Cancer Research, Combination therapy, biology, Venetoclax, business.industry, Cancer, medicine.disease, chemistry.chemical_compound, Oncology, chemistry, In vivo, Neuroblastoma, medicine, biology.protein, Cancer research, Mdm2, Talazoparib, business, B-cell lymphoma

Abstract

BACKGROUND: The anti-apoptotic protein B cell lymphoma/leukaemia 2 (BCL-2) is highly expressed in the majority of all neuroblastomas. In previous preclinical studies, we have shown that treatment of BCL-2-dependent neuroblastoma with BCL-2 inhibitors leads to programmed cell death. These results have contributed to the initiation of a phase I trial to study the safety and pharmacokinetics of Venetoclax in children with relapsed or refractory neuroblastoma. AIM: The current study aims to identify and validate targeted combination strategies to prevent or overcome neuroblastoma resistance to Venetoclax. METHODS: Targeted drug candidates for combination treatment with Venetoclax were identified by high-throughput drug screening of non-resistant and Venetoclax-resistant BCL-2-dependent neuroblastoma cell lines. Top hits were subsequently tested more extensively in vitro and in vivo to validate the screening results. RESULTS: High-throughput drug screens identified the MDM2 inhibitor Idasanutlin as one of the strongest re-sensitizers for Venetoclax in Venetoclax-resistant BCL-2-dependent neuroblastoma cells with wild-type p53. Subsequent in vitro validation showed that Idasanutlin induced cyclin dependent kinase inhibitor 1 (p21)-mediated growth arrest in non-resistant neuroblastoma cells, but induced a BCL-2-associated X protein (BAX)-mediated apoptotic response in Venetoclax-resistant neuroblastoma cells in the presence of Venetoclax. In vivo combination of Venetoclax with Idasanultin resulted in a remarkably improved anticancer effect compared to single agent therapy, with very good partial and complete responses in BCL-2-dependent neuroblastoma xenografts. Combination screens additionally revealed that the clinically studied targeted inhibitors CUDC-907 (PI3K/HDAC), Prexasertib (CHK1) and Talazoparib (PARP1/2) improved the efficacy of Venetoclax more potently than ALK inhibitors in BCL-2-dependent neuroblastoma cells harboring ALK mutations. CONCLUSION: Our findings suggest that the clinical use of Venetoclax for the treatment of children with BCL-2-dependent neuroblastoma tumors can be improved by combination therapy with targeted inhibitors. The presence of additional neuroblastoma driving genomic events is not always predictive of the optimal combination strategy for BCL-2-dependent neuroblastoma subgroups. These findings should guide the design of combination Phase 2 trials of Venetoclax with other targeted compounds such as Idasanutlin, CUDC-907, Prexasertib and Talazoparib. Citation Format: M. Emmy M. Dolman, Laurel T. Bate-Eya, Lindy Vernooij, Bianca Koopmans, Lindy K. Alles, Anke H. Essing, Daphne Lelieveld, David A. Egan, Mark Kerstjens, Ronald W. Stam, Huib N. Caron, Jan J. Molenaar. Preclinical identification of Venetoclax combination strategies with Idasanutlin, CUDC-907, Prexasertib or Talazoparib for neuroblastoma treatment [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 2630.

Published

2018

27. Discovery and Optimization of Boronic Acid Based Inhibitors of Autotaxin

Author

Laurens A. van Meeteren, Wouter H. Moolenaar, Erica W. van Tilburg, David A. Egan, Huib Ovaa, and Harald M. H. G. Albers

Subjects

Magnetic Resonance Spectroscopy, Mass Spectrometry, Cell Line, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, Multienzyme Complexes, Drug Discovery, Lysophosphatidic acid, Humans, Structure–activity relationship, Enzyme Inhibitors, Pyrophosphatases, Threonine, chemistry.chemical_classification, Phosphoric Diester Hydrolases, Lysophosphatidylcholines, Lipid signaling, Boronic Acids, Small molecule, Enzyme, chemistry, Biochemistry, Phosphodiesterase I, Molecular Medicine, Thiazolidinediones, lipids (amino acids, peptides, and proteins), Autotaxin, Boronic acid, Signal Transduction

Abstract

Autotaxin (ATX) is an extracellular enzyme that hydrolyzes lysophosphatidylcholine (LPC) to produce the lipid mediator lysophosphatidic acid (LPA). The ATX-LPA signaling axis has been implicated in diverse physiological and pathological processes, including vascular development, inflammation, fibrotic disease, and tumor progression. Therefore, targeting ATX with small molecule inhibitors is an attractive therapeutic strategy. We recently reported that 2,4-thiazolidinediones inhibit ATX activity in the micromolar range. Interestingly, inhibitory potency was dramatically increased by introduction of a boronic acid moiety, designed to target the active site threonine in ATX. Here we report on the discovery and further optimization of boronic acid based ATX inhibitors. The most potent of these compounds inhibits ATX-mediated LPC hydrolysis in the nanomolar range (IC(50) = 6 nM). The finding that ATX can be targeted by boronic acids may aid the development of ATX inhibitors for therapeutic use.

Published

2010

28. An image-based miRNA screen identifies miRNA-135s as regulators of CNS axon growth and regeneration by targeting krüppel-like factor 4

Author

Alwin A.H.A. Derijck, Daphne Lelieveld, Youri Adolfs, Giuliano Giuliani, R. Jeroen Pasterkamp, Eoghan O'Duibhir, Marieke G. Verhagen, Toshihide Yamashita, Yuki Fujita, Roel Q.J. Schaapveld, Eljo Y. van Battum, David A. Egan, Vamshidhar R. Vangoor, and Thijs de Gunst

Subjects

0301 basic medicine, Male, Retinal Ganglion Cells, Neuroscience(all), Central nervous system, Kruppel-Like Transcription Factors, Biology, 03 medical and health sciences, Kruppel-Like Factor 4, Mice, microRNA, medicine, Gene silencing, Animals, Humans, Regeneration, Axon, Research Articles, General Neuroscience, Regeneration (biology), Nerve injury, KLF4, Axons, Nerve Regeneration, Axon growth, Mice, Inbred C57BL, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Retinal ganglion cell, Gene Expression Regulation, nervous system, Intrinsic, Female, medicine.symptom, Neuroscience

Abstract

During embryonic development, axons extend over long distances to establish functional connections. In contrast, axon regeneration in the adult mammalian CNS is limited in part by a reduced intrinsic capacity for axon growth. Therefore, insight into the intrinsic control of axon growth may provide new avenues for enhancing CNS regeneration. Here, we performed one of the first miRNome-wide functional miRNA screens to identify miRNAs with robust effects on axon growth. High-content screening identified miR-135a and miR-135b as potent stimulators of axon growth and cortical neuron migrationin vitroandin vivoin male and female mice. Intriguingly, both of these developmental effects of miR-135s relied in part on silencing of Krüppel-like factor 4 (KLF4), a well known intrinsic inhibitor of axon growth and regeneration. These results prompted us to test the effect of miR-135s on axon regeneration after injury. Our results show that intravitreal application of miR-135s facilitates retinal ganglion cell (RGC) axon regeneration after optic nerve injury in adult mice in part by repressing KLF4. In contrast, depletion of miR-135s further reduced RGC axon regeneration. Together, these data identify a novel neuronal role for miR-135s and the miR-135–KLF4 pathway and highlight the potential of miRNAs as tools for enhancing CNS axon regeneration.SIGNIFICANCE STATEMENTAxon regeneration in the adult mammalian CNS is limited in part by a reduced intrinsic capacity for axon growth. Therefore, insight into the intrinsic control of axon growth may provide new avenues for enhancing regeneration. By performing an miRNome-wide functional screen, our studies identify miR-135s as stimulators of axon growth and neuron migration and show that intravitreal application of these miRNAs facilitates CNS axon regeneration after nerve injury in adult mice. Intriguingly, these developmental and regeneration-promoting effects rely in part on silencing of Krüppel-like factor 4 (KLF4), a well known intrinsic inhibitor of axon regeneration. Our data identify a novel neuronal role for the miR-135–KLF4 pathway and support the idea that miRNAs can be used for enhancing CNS axon regeneration.

Published

2018

29. EDS as a method of manufacturing diamond tools

Author

Seamus Melody and David Patrick Egan

Subjects

Materials science, Mechanical Engineering, Metallurgy, Aerospace Engineering, Diamond, Sintering, High density, engineering.material, Iron powder, Mechanics of Materials, Automotive Engineering, engineering, General Materials Science, Electrical conductor

Abstract

This paper details the use of electro discharge sintering (EDS) to sinter diamond containing segments to high density and strength from standard iron powders using a split mould with insulating sides and conductive punches. Additional segments were made from iron powder and diamond manufactured in strip form and cut to shape …

Published

2009

30. The microRNAs miR-373 and miR-520c promote tumour invasion and metastasis

Author

Kiranmai Gumireddy, George Coukos, le Sage C, Reuven Agami, Dionyssios Katsaros, Mariette Schrier, David A. Egan, Phyllis A. Gimotty, Andres J. Klein-Szanto, Nair S, Remco Nagel, Guanghua Huang, Lin Zhang, Puré E, Qihong Huang, and Anping Li

Subjects

Male, Transplantation, Heterologous, Breast Neoplasms, Mice, SCID, Biology, Metastasis, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Cell Movement, In vivo, Cell Line, Tumor, microRNA, medicine, Animals, Humans, Neoplasm Invasiveness, Neoplasm Metastasis, 030304 developmental biology, 0303 health sciences, CD44, Prostatic Neoplasms, Cell Biology, medicine.disease, Phenotype, 3. Good health, Cell biology, MicroRNAs, Hyaluronan Receptors, Cell culture, Lymphatic Metastasis, 030220 oncology & carcinogenesis, Colonic Neoplasms, biology.protein, Female, Cell Migration Assays, Neoplasm Transplantation, Genetic screen

Abstract

MicroRNAs (miRNAs) are single-stranded, noncoding RNAs that are important in many biological processes1,2. Although the oncogenic and tumour-suppressive functions of several miRNAs have been characterized, the role of miRNAs in mediating tumour metastasis was addressed only recently3 and still remains largely unexplored4,5. To identify potential metastasis-promoting miRNAs, we set up a genetic screen using a non-metastatic, human breast tumour cell line that was transduced with a miRNA-expression library and subjected to a trans-well migration assay. We found that human miR-373 and miR-520c stimulated cancer cell migration and invasion in vitro and in vivo, and that certain cancer cell lines depend on endogenous miR-373 activity to migrate efficiently. Mechanistically, the migration phenotype of miR-373 and miR-520c can be explained by suppression of CD44. We found significant upregulation of miR-373 in clinical breast cancer metastasis samples that correlated inversely with CD44 expression. Taken together, our findings indicate that miRNAs are involved in tumour migration and invasion, and implicate miR-373 and miR-520c as metastasis-promoting miRNAs.

Published

2008

31. A potent erythropoietin-mimicking human antibody interacts through a novel binding site

Author

Susan E. Lacy, David A. Egan, Robert L Simmer, Nancy Xie, Edward B. Reilly, Devries Peter J, Richard R. Lesniewski, Zhihong Liu, Clarissa G. Jakob, John E. Harlan, and Vincent S. Stoll

Subjects

Models, Molecular, Genetically modified mouse, Immunology, Pure red cell aplasia, Biology, Crystallography, X-Ray, Biochemistry, Antibodies, Cell Line, law.invention, Mice, law, hemic and lymphatic diseases, Receptors, Erythropoietin, medicine, Animals, Humans, Erythropoiesis, Binding site, Protein Structure, Quaternary, Erythropoietin, Mice, Knockout, Binding Sites, Activator (genetics), Molecular Mimicry, food and beverages, Cell Biology, Hematology, medicine.disease, Molecular biology, Protein Structure, Tertiary, Erythropoietin receptor, Hematocrit, Structural Homology, Protein, biology.protein, Recombinant DNA, Cancer research, Antibody, medicine.drug

Abstract

Recombinant human erythropoietin (rHu-EPO) is used to treat anemia by activating the erythropoietin receptor (EPOR) in erythroid progenitor cells, leading to proliferation and differentiation into mature red blood cells. To allow less frequent dosing, a hyperglycosylated version of EPO has been developed with a longer half-life. In principle, an agonistic antibody targeting EPOR would offer an even longer half-life, support robust monthly dosing, and, unlike EPO products, reduce the risk of pure red cell aplasia. The efficiency of signaling and corresponding potency of previously reported antibody mimics are generally suboptimal compared with EPO and not suitable for clinical use. Here we describe a potent, fully human, agonistic antibody (ABT007) targeting EPOR that supports potent, more sustained, and less pulsatile elevation of hematocrit in a human EPOR–expressing transgenic mouse model compared with standard doses of rHu-EPO while requiring less frequent dosing. Resolution of the crystal structure of the EPOR extracellular domain (ECD) complexed to the ABT007 Fab fragment, determined at 0.32 nm, identifies a binding site that is consistent with a novel mechanism of receptor activation based on a unique antibody-imposed conformational change. These results demonstrate that a symmetric molecule can serve as a potent activator of the EPOR.

Published

2007

32. The glucocorticoid mometasone furoate is a novel FXR ligand that decreases inflammatory but not metabolic gene expression

Author

Alexandra Milona, Chiara Guercini, Ingrid T. G. W. Bijsmans, José M. Ramos Pittol, Antimo Gioiello, David A. Egan, Saskia W.C. van Mil, Roberto Pellicciari, Daphne Lelieveld, and Wienand A. Omta

Subjects

Models, Molecular, Anti-Inflammatory Agents, Molecular Conformation, Gene Expression, Receptors, Cytoplasmic and Nuclear, FXR, mometasone furoate, molecular mechanism, gene regulation, metabolic desease, inflammation, Biology, Research Support, Ligands, Article, Mice, Transactivation, Glucocorticoid receptor, metabolic desease, Genes, Reporter, medicine, Journal Article, Animals, Humans, Non-U.S. Gov't, Promoter Regions, Genetic, Receptor, General, Transrepression, Inflammation, Regulation of gene expression, Multidisciplinary, Tumor Necrosis Factor-alpha, Research Support, Non-U.S. Gov't, NF-kappa B, Transcription Factor RelA, Hep G2 Cells, NFKB1, Cell biology, Molecular Docking Simulation, FXR, Gene Expression Regulation, Biochemistry, Farnesoid X receptor, molecular mechanism, gene regulation, Mometasone Furoate, Glucocorticoid, Protein Binding, medicine.drug

Abstract

The Farnesoid X receptor (FXR) regulates bile salt, glucose and cholesterol homeostasis by binding to DNA response elements, thereby activating gene expression (direct transactivation). FXR also inhibits the immune response via tethering to NF-κB (tethering transrepression). FXR activation therefore has therapeutic potential for liver and intestinal inflammatory diseases. We aim to identify and develop gene-selective FXR modulators, which repress inflammation, but do not interfere with its metabolic capacity. In a high-throughput reporter-based screen, mometasone furoate (MF) was identified as a compound that reduced NF-κB reporter activity in an FXR-dependent manner. MF reduced mRNA expression of pro-inflammatory cytokines and induction of direct FXR target genes in HepG2-GFP-FXR cells and intestinal organoids was minor. Computational studies disclosed three putative binding modes of the compound within the ligand binding domain of the receptor. Interestingly, mutation of W469A residue within the FXR ligand binding domain abrogated the decrease in NF-κB activity. Finally, we show that MF-bound FXR inhibits NF-κB subunit p65 recruitment to the DNA of pro-inflammatory genes CXCL2 and IL8. Although MF is not suitable as selective anti-inflammatory FXR ligand due to nanomolar affinity for the glucocorticoid receptor, we show that separation between metabolic and anti-inflammatory functions of FXR can be achieved.

Published

2015

33. Signal Inhibitory Receptor on Leukocytes-1 Limits the Formation of Neutrophil Extracellular Traps, but Preserves Intracellular Bacterial Killing

Author

Paul H. Naccache, Maarten van der Linden, Kristof Van Avondt, David A. Egan, and Linde Meyaard

Subjects

0301 basic medicine, Cytoplasm, Staphylococcus aureus, Neutrophils, Phagocytosis, Immunology, Biology, Extracellular Traps, Microbiology, 03 medical and health sciences, Journal Article, Extracellular, Immunology and Allergy, Humans, Receptors, Immunologic, Receptor, Opsonin, chemistry.chemical_classification, Reactive oxygen species, NADPH Oxidases, Neutrophil extracellular traps, Kinetics, 030104 developmental biology, chemistry, Host-Pathogen Interactions, Signal transduction, Reactive Oxygen Species, Intracellular, Signal Transduction

Abstract

In response to microbial invasion, neutrophils release neutrophil extracellular traps (NETs) to trap and kill extracellular microbes. Alternatively, NET formation can result in tissue damage in inflammatory conditions and may perpetuate autoimmune disease. Intervention strategies that are aimed at modifying pathogenic NET formation should ideally preserve other neutrophil antimicrobial functions. We now show that signal inhibitory receptor on leukocytes-1 (SIRL-1) attenuates NET release by human neutrophils in response to distinct triggers, including opsonized Staphylococcus aureus and inflammatory danger signals. NET release has different kinetics depending on the stimulus, and rapid NET formation is independent of NADPH oxidase activity. In line with this, we show that NET release and reactive oxygen species production upon challenge with opsonized S. aureus require different signaling events. Importantly, engagement of SIRL-1 does not affect bacterially induced production of reactive oxygen species, and intracellular bacterial killing by neutrophils remains intact. Thus, our studies define SIRL-1 as an intervention point of benefit to suppress NET formation in disease while preserving intracellular antimicrobial defense.

Published

2015

34. Effects of Pelvic Asymmetry and Low Back Pain on Trunk Kinematics During Sitting: A Comparison With Standing

Author

Kevin J. Deluzio, Richard J. Wassersug, Einas Al-Eisa, and David A. Egan

Subjects

Adult, Male, medicine.medical_specialty, Posture, Kinematics, Sitting, Physical medicine and rehabilitation, Multivariate analysis of variance, medicine, Humans, Orthopedics and Sports Medicine, Prospective Studies, Range of Motion, Articular, Pelvic Bones, Back, business.industry, Middle Aged, Low back pain, Trunk kinematics, Trunk, Biomechanical Phenomena, body regions, Female, Neurology (clinical), medicine.symptom, Pelvic asymmetry, business, Range of motion, Low Back Pain

Abstract

STUDY DESIGN A prospective study was conducted on a group of patients with unilateral nonspecific low back pain (LBP) and healthy controls. OBJECTIVES To answer 3 questions: (1) Does pelvic asymmetry measured in standing affect the dynamics of motion performed in sitting? (2) Do patients with LBP perform trunk motions differently from non-LBP participants in sitting position? and (3) Do the kinematics of lateral flexion and axial rotation differ between sitting and standing positions? SUMMARY OF BACKGROUND DATA The effect of pelvic asymmetry on trunk motion while sitting remains unclear. LBP has been associated with altered trunk kinematics in standing; however, there is limited information available describing trunk kinematics in sitting position in comparison to standing. METHODS Pelvic asymmetry was measured in 54 patients with unilateral nonspecific LBP and 59 control subjects. A motion-analysis system was used to test the range and symmetry of lateral flexion and axial rotation in sitting and standing positions. Bivariate correlations, regression, multivariate analysis of variance, and paired sample t tests were used to test for associations between variables and differences between groups. RESULTS We found significant: (1) correlations between pelvic asymmetry and asymmetric trunk motion performed in sitting, (2) differences between the LBP and control groups in patterns of trunk motion performed in a sitting posture, and (3) differences between kinematics of motions performed in sitting versus standing postures. CONCLUSIONS This study shows a link between pelvic asymmetry and altered trunk motion in sitting position. We suggest that people with LBP may have a distinct compensatory mechanism, secondary to pelvic asymmetry, which puts the lumbar spine under higher stress. Movement asymmetry, rather than range of motion, may be a better indicator of disturbed function for people with LBP. Structural and functional asymmetries are factors that may be considered in the seating design and work environment.

Published

2006

35. Effects of Pelvic Skeletal Asymmetry on Trunk Movement

Author

Einas Al-Eisa, Kevin J. Deluzio, Richard J. Wassersug, and David A. Egan

Subjects

Adult, Male, musculoskeletal diseases, Pelvic tilt, medicine.medical_specialty, Movement, Thoracic Vertebrae, Lumbar, Physical medicine and rehabilitation, medicine, Humans, Orthopedics and Sports Medicine, Range of Motion, Articular, Pelvic Bones, Pelvis, Lumbar Vertebrae, Referred pain, business.industry, Middle Aged, Trunk, Low back pain, Biomechanical Phenomena, body regions, medicine.anatomical_structure, Multivariate Analysis, Laterality, Female, Neurology (clinical), medicine.symptom, Range of motion, business, Low Back Pain

Abstract

Study design Comparative analysis and correlational research design were used to investigate the association between anthropometry and biomechanical performance among asymptomatic subjects and patients with low back pain (LBP). Objectives To examine the association between pelvic asymmetry and patterns of trunk motion in asymptomatic and LBP subjects. Secondary objective was to investigate the association between restricted trunk motion, laterality of referred pain, and pelvic asymmetry. Summary of background data Subtle pelvic asymmetry (exhibited as either lateral pelvic tilt or iliac rotational asymmetry), which is common among normal individuals, has not been convincingly linked to abnormalities in back movements. Given the difficulty in diagnosing most LBP, a classification using pelvic asymmetry and patterns of movement could be helpful in establishing a rational treatment plan. Methods Fifty-nine subjects with no history of LBP and 54 patients with mechanical unilateral LBP were tested. An anthropometric frame was used to measure pelvic asymmetry in standing. Dynamic motion data, comprised of the principal and coupled movements, were collected using the Qualysis Motion Capture System. Results While the groups did not differ in the total range of lumbar movement, the LBP group exhibited significantly higher asymmetry in the principal motion. The groups differed significantly in the pattern of coupled rotation during lateral flexion. Asymmetry in lumbar lateral flexion was highly related to two types of pelvic asymmetry: lateral pelvic tilt (LPT) and iliac rotation asymmetry (IRA). Asymmetry in lumbar axial rotation was highly related to IRA but weakly related to LPT. Conclusions This study demonstrates objective differences in patterns of lumbar movement between asymptomatic subjects and patients with LBP. The study also demonstrates that subtle anatomic abnormality in the pelvis is associated with altered mechanics in the lumbar spine. We suggest that asymmetry of lumbar movement may be a better indicator of functional deficit than the absolute range of movement in LBP.

Published

2006

36. Association Between Lateral Pelvic Tilt and Asymmetry in Sitting Pressure Distribution

Author

Anne Fenety, Einas Al-Eisa, and David A. Egan

Subjects

Pelvic tilt, medicine.medical_specialty, business.industry, media_common.quotation_subject, Peak pressure, Sitting posture, Physical Therapy, Sports Therapy and Rehabilitation, Anthropometry, Sitting, Asymmetry, Surgery, Physical medicine and rehabilitation, Interface pressure, medicine, business, Association (psychology), media_common

Abstract

Physical therapists commonly associate lateral pelvic tilt (LPT) with a variety of musculoskeletal adaptations, syndromes and altered function. Such musculoskeletal adaptations have been suggested in many reports to cause unequal sitting pressure distribution (SPD) at the buttock/chair interface. However, those reports have failed to provide objective evidence to support that hypothesis. This study was conducted to examine the relationship between LPT and SPD in a sample of healthy female volunteers. Subjects were tested for pelvic symmetry using an anthropometric frame, then assigned to two groups: symmetrical (n = 36) and LPT (n = 9). SPD was measured in an upright sitting posture using an interface pressure mat. Although the results indicated that there were no significant differences between the two groups in the magnitude and position of the peak pressure, there was a greater variability among subjects in the LPT group than the symmetrical group. This observation is worth further investigatio...

Published

2004

37. Fluctuating asymmetry and low back pain

Author

David A. Egan, Einas Al-Eisa, and Richard J. Wassersug

Subjects

medicine.medical_specialty, media_common.quotation_subject, Experimental and Cognitive Psychology, Anatomy, Control subjects, Asymmetry, Low back pain, Asymptomatic, Fluctuating asymmetry, body regions, Physical medicine and rehabilitation, medicine.anatomical_structure, Arts and Humanities (miscellaneous), medicine, Fitness measure, medicine.symptom, Psychology, Pelvic asymmetry, Ecology, Evolution, Behavior and Systematics, Pelvis, media_common

Abstract

Fluctuating asymmetry (FA), a pattern of bilateral variation that is normally distributed around a mean of zero, appears to correlate inversely with fitness and health. In this study, we compared the FA of asymptomatic control subjects (n=51) and patients with low back pain (n=44). We measured eight traits, from the upper and lower limbs, and used them to obtain asymmetry indices for each subject. We also measured pelvic asymmetry in standing subjects. The low back pain (LBP) group showed significantly higher asymmetry in the pelvis, and in ulnar length and bistyloid breadth. Our results demonstrate a link between LBP and asymmetry not only in a weight-bearing trait (i.e., pelvic configuration), but in two traits that are not functionally related to the back (i.e., ulnar length and bistyloid breadth). We can now consider LBP as another health and fitness measure correlated with FA.

Published

2004

38. Human Daxx regulates Fas-induced apoptosis from nuclear PML oncogenic domains (PODs)

Author

John C. Reed, Seiji Torii, David A. Egan, and Ronald A. Evans

Subjects

Programmed cell death, Fluorescent Antibody Technique, Apoptosis, Promyelocytic Leukemia Protein, Transfection, Arsenicals, General Biochemistry, Genetics and Molecular Biology, Cell Line, Promyelocytic leukemia protein, Death-associated protein 6, Arsenic Trioxide, Yeasts, medicine, Humans, fas Receptor, Cloning, Molecular, Nuclear protein, Molecular Biology, Transcription factor, Caspase, Adaptor Proteins, Signal Transducing, Cell Nucleus, General Immunology and Microbiology, biology, Tumor Suppressor Proteins, General Neuroscience, Intracellular Signaling Peptides and Proteins, JNK Mitogen-Activated Protein Kinases, Nuclear Proteins, Oxides, Precipitin Tests, Molecular biology, Neoplasm Proteins, Cell biology, Enzyme Activation, Cell nucleus, medicine.anatomical_structure, Gene Expression Regulation, biology.protein, Mitogen-Activated Protein Kinases, Carrier Proteins, Co-Repressor Proteins, Research Article, Molecular Chaperones, Protein Binding, Transcription Factors

Abstract

Daxx was first identified as a protein that binds the cytosolic domain of Fas and links this receptor to an apoptosis pathway involving activation of Jun N-terminal kinase (JNK). We show here that cells overexpressing the human homolog of Daxx (hDaxx) display enhanced sensitivity to apoptosis induced by Fas but not by several other cell death stimuli. hDaxx-mediated enhancement of Fas-induced apoptosis was correlated with accelerated activation of caspases but not with JNK induction. Although specifically enhancing Fas function, hDaxx does not bind Fas and instead is found in the nucleus where it localizes to PML oncogenic domains (PODs). Moreover, the hDaxx protein also exhibits the ability to repress transcription. Mutagenesis studies demonstrated a correlation between the localization of hDaxx to PODs and its ability to enhance Fas-induced cell death. Arsenic trioxide (As(2)O(3)), an agent that accentuates POD formation, collaborated synergistically with overexpression of hDaxx to increase cellular sensitivity to Fas-induced apoptosis. Taken together, these findings argue that hDaxx promotes sensitivity to Fas from a nuclear location, probably by modulating the transcription of genes involved in Fas-induced caspase activation and apoptosis.

Published

1999

39. Modulation of CREB binding protein function by the promyelocytic (PML) oncoprotein suggests a role for nuclear bodies in hormone signaling

Author

Marc Tini, Vassilis Doucas, David A. Egan, and Ronald M. Evans

Subjects

Transcriptional Activation, Acute promyelocytic leukemia, viruses, Promyelocytic Leukemia Protein, CREB, Promyelocytic leukemia protein, Leukemia, Promyelocytic, Acute, Enhancer binding, medicine, Humans, CREB-binding protein, Nuclear protein, Transcription factor, Cell Nucleus, Multidisciplinary, biology, Tumor Suppressor Proteins, virus diseases, Nuclear Proteins, Biological Sciences, medicine.disease, CREB-Binding Protein, Cell Compartmentation, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Cell nucleus, medicine.anatomical_structure, Trans-Activators, biology.protein, Cancer research, Transcription Factors

Abstract

Disaggregation of the spherical nuclear bodies termed promyelocytic (PML) oncogenic domains (PODs) is a characteristic of acute promyelocytic leukemia. Here, we demonstrate that the cAMP enhancer binding protein (CREB)-binding protein (CBP) associates with PML in vitro and is recruited to the PODs in vivo . Through its association with CBP, wild-type PML dramatically stimulates nuclear receptor transcriptional activity. These results demonstrate that a fraction of CBP is compartmentalized to the POD through its association with PML and thus suggest that PML and other POD-associated proteins may play an unexpectedly broad role in aspects of transcriptional regulation and human disease.

Published

1999

40. An Alternative Method for the Measurement of Pelvic Skeletal Asymmetry (PSA) Using an Asymmetry Ratio (AR)

Author

Joan H. Cole, David A. Egan, and Lance Twomey

Subjects

Alternative methods, business.industry, System of measurement, media_common.quotation_subject, Leg length, Physical Therapy, Sports Therapy and Rehabilitation, Pattern recognition, Anatomy, Asymmetry, Medicine, Artificial intelligence, Skeletal asymmetry, business, media_common

Abstract

This paper presents an alternative method for determining PSA. Frequently, physical therapists rely heavily on visual palpatory techniques for the assessment of pelvic skeletal asymmetry; however, a more objective approach using valid and reliable measurement systems is needed. This study shows how a relatively simple and non-invasive measurement system will provide accurate measurements of PSA. The asymmetry ratio, which is easily derived from these measurements, provides a quantitative measurement and a differentiation between two common types of PSA, leg length discrepancy (LLD) and iliac rotation asymmetry (IRA). A distinct advantage is that the AR provides normalized data that take into account the individual differences in pelvic width. Alternative measurement systems may also be used to estimate AR provided they give reliable measurements of the height and width differences of the pelvic bony landmarks.

Published

1999

41. Data Record 2: Secondary dsRNA screen data

Author

Andre F Maia, Marvin E Tanenbaum, Matilde Galli, Daphne Lelieveld, David A Egan, Reto Gassmann, Claudio Sunkel, Sander van den Heuvel, Rene H Medema, Andre F Maia, Marvin E Tanenbaum, Matilde Galli, Daphne Lelieveld, David A Egan, Reto Gassmann, Claudio Sunkel, Sander van den Heuvel, and Rene H Medema

Published

2015

42. Data Record 1: Primary dsRNA screen data

Author

Andre F Maia, Marvin E Tanenbaum, Matilde Galli, Daphne Lelieveld, David A Egan, Reto Gassmann, Claudio Sunkel, Sander van den Heuvel, Rene H Medema, Andre F Maia, Marvin E Tanenbaum, Matilde Galli, Daphne Lelieveld, David A Egan, Reto Gassmann, Claudio Sunkel, Sander van den Heuvel, and Rene H Medema

Published

2015

43. Domain structure analysis of elongation factor-3 fromsaccharomyces cerevisiaeby limited proteolysis and differential scanning calorimetry

Author

Robert C. Goldman, Seth W. Snyder, Tom Mcgonigal, Karl A. Walter, Uri S. Ladror, John O. Capobianco, Sarah A. Dorwin, Rohinton Edalji, David A. Egan, Thomas F. Holzman, Robert W. Johnson, and Aparna V. Sarthy

Subjects

Saccharomyces cerevisiae Proteins, Proteolysis, Molecular Sequence Data, Saccharomyces cerevisiae, Biology, Biochemistry, Fungal Proteins, Differential scanning calorimetry, medicine, Trypsin, Amino Acid Sequence, Molecular Biology, Peptide sequence, Chromatography, High Pressure Liquid, Fungal protein, Calorimetry, Differential Scanning, medicine.diagnostic_test, Peptide Elongation Factors, biology.organism_classification, Peptide Fragments, Elongation factor, Electrophoresis, Polyacrylamide Gel, Ultracentrifuge, Ultracentrifugation, Research Article, medicine.drug

Abstract

Elongation-factor-3 (EF-3) is an essential factor of the fungal protein synthesis machinery. In this communication the structure of EF-3 from Saccharomyces cerevisiae is characterized by differential scanning calorimetry (DSC), ultracentrifugation, and limited tryptic digestion. DSC shows a major transition at a relatively low temperature of 39 degrees C, and a minor transition at 58 degrees C. Ultracentrifugation shows that EF-3 is a monomer; thus, these transitions could not reflect the unfolding or dissociation of a multimeric structure. EF-3 forms small aggregates, however, when incubated at room temperature for an extended period of time. Limited proteolysis of EF-3 with trypsin produced the first cleavage at the N-side of Gln775, generating a 90-kDa N-terminal fragment and a 33-kDa C-terminal fragment. The N-terminal fragment slowly undergoes further digestion generating two major bands, one at approximately 75 kDa and the other at approximately 55 kDa. The latter was unusually resistant to further tryptic digestion. The 33-kDa C-terminal fragment was highly sensitive to tryptic digestion. A 30-min tryptic digest showed that the N-terminal 60% of EF-3 was relatively inaccessible to trypsin, whereas the C-terminal 40% was readily digested. These results suggest a tight structure of the N-terminus, which may give rise to the 58 degrees C transition, and a loose structure of the C-terminus, giving rise to the 39 degrees C transition. Three potentially functional domains of the protein were relatively resistant to proteolysis: the supposed S5-homologous domain (Lys102-Ile368), the N-terminal ATP-binding cassette (Gly463-Lys622), and the aminoacyl-tRNA-synthase homologous domain (Glu820-Gly865). Both the basal and ribosome-stimulated ATPase activities were inactivated by trypsin, but the ribosome-stimulated activity was inactivated faster.

Published

1998

44. [Untitled]

Author

Kathleen W. Scotto and David A. Egan

Subjects

Genetics, education.field_of_study, Cellular differentiation, Clinical Biochemistry, Population, Biomedical Engineering, Bioengineering, Cell Biology, Biology, Multiple drug resistance, Gene product, Gene expression, Transcriptional regulation, Cancer research, biology.protein, education, Gene, Biotechnology, P-glycoprotein

Abstract

The emergence of resistance in a tumor population is most often associated with a disregulation of gene expression, usually at the level of transcription. A major goal in the field of cancer chemotherapy is to define the mechanisms underlying transcriptional regulation of drug resistance genes in an effort to identify targets for therapeutic intervention. Recently, considerable progress has been made in identifying the molecular mechanisms involved in the transcriptional regulation of the P-glycoprotein (Pgp) gene. When overexpressed in tumor cells, Pgp confers resistance to a variety of chemotherapeutic agents; this resistance has been termed MDR (multidrug resistance). Moreover, Pgp is a normal component of a variety of highly differentiated cell types and, as such, is regulated by both internal and external environmental stimuli. In this review, we will discuss the current knowledge regarding the DNA elements and protein factors involved in both constitutive and inducible regulation of Pgp transcription in normal and tumor cells.

Published

1998

45. A Review of the Muscle Activation Patterns Associated with the Pelvic Tilt Exercise Used in the Treatment of Low Back Pain

Author

David A. Egan, Cheryl L. Hubley-Kozey, and M.Johanne Vezina

Subjects

Pelvic tilt, medicine.medical_specialty, business.industry, Physical Therapy, Sports Therapy and Rehabilitation, Muscle activation, Low back pain, Trunk, body regions, Physical medicine and rehabilitation, Abdominal muscles, Rehabilitation exercise, Motor unit recruitment, Physical therapy, Medicine, Emg biofeedback, medicine.symptom, business

Abstract

A survey of the literature was undertaken to review the evolution of the posterior pelvic tilt exercise (PPTE) and to evaluate the use of the PPTE in treatment programs for low back pain (LBP). The review then focused on electromyographic (EMG) evidence supporting the clinical claims of improved posture, abdominal muscle strength, trunk stability and decreased pain associated with the PPTE.The recruitment patterns and the level of activation during the PPTE for the abdominal and the trunk extensor muscles in different postures have not been clearly established for normal subjects or those with LBP. Minimal evidence supporting the role of the hip extensor muscles in performing the pelvic tilt was found. Claims that the PPTE activates the abdominal or hip extensor muscles to a level that would promote strengthening cannot be substantiated. It is suggested that EMG biofeedback could potentially assist in decisions to use the PPTE.

Published

1998

46. A polarization-based optical fibre vibrometer

Author

Stephen W. James, Ralph P. Tatam, and David A. Egan

Subjects

Materials science, Birefringence, Optical fiber, Laser diode, business.industry, Applied Mathematics, Polarization (waves), law.invention, Interferometry, Optics, Signal beam, law, Laser scanning vibrometry, business, Instrumentation, Engineering (miscellaneous), Laser Doppler vibrometer

Abstract

A fibre optic heterodyne vibrometer configuration based on the use of birefringent optical fibre components is demonstrated. The heterodyne processing is moved to the receiving section of the interferometer, reducing the optomechanical stability requirements of the system and enabling optimization of the reference to signal beam ratio intensity. The instrument can be configured to have minimum down lead sensitivity. The technique was demonstrated with a laser diode at 833 nm with a minimum detectable phase change of obtained at 5 kHz.

Published

1997

47. The Standing Forward Flexion Test: An Inaccurate Determinant of Sacroiliac Joint Dysfunction

Author

David A. Egan, Lance T. Twomey, and Joan H. Cole

Subjects

Sacroiliac joint, Orthodontics, medicine.medical_specialty, business.industry, Flexion Test, Physical Therapy, Sports Therapy and Rehabilitation, Anthropometry, Low back pain, Asymptomatic, medicine.anatomical_structure, Sacroiliac joint dysfunction, Statistical significance, medicine, Back pain, Physical therapy, medicine.symptom, business

Abstract

Summary Objective evidence which supports an association between the forward flexion test (FFT) and sacroiliac joint dysfunction is lacking. The purpose of this study was to investigate the occurrence of a positive FFT in a sample of young adults (N = 128), and to examine the association of factors such as low back pain, pelvic skeletal asymmetry, age, height, weight, and stance asymmetry. The history of back pain and the results of the FFT were recorded and measurements of height, weight, preferred stance angle and asymmetry ratio were taken. Descriptive statistics were used to present the anthropometric and FFT data, and t-tests were used to examine differences between females and males, and subjects with and without a positive FFT. The 0.05 level of significance was selected. Of the subjects tested 24% (n = 31) had a positive FFT and the highest occurrence of a positive FFT was in male subjects (n = 19). Nine asymptomatic subjects had a positive FFT. Statistically significant differences were observed between the positive and negative FFT groups for height, weight and asymmetry ratio (p > 0.05). It is concluded that factors other than sacroiliac joint dysfunction are likely to be the cause of a positive FFT.

Published

1996

48. Fibre optic based reference beam laser Doppler velocimetry

Author

Robert A. Lockey, Stephen W. James, Ralph P. Tatam, and David A. Egan

Subjects

Distributed feedback laser, Materials science, Laser diode, business.industry, Physics::Optics, Laser Doppler velocimetry, Laser, Beam parameter product, Atomic and Molecular Physics, and Optics, Electronic, Optical and Magnetic Materials, law.invention, Optics, law, Reference beam, Physics::Atomic Physics, Laser beam quality, Electrical and Electronic Engineering, Physical and Theoretical Chemistry, business, Laser Doppler vibrometer

Abstract

A compact reference beam laser Doppler velocimeter is described, constructed using semiconductor laser diodes, optical fibre components and semiconductor detectors. The design of the device overcomes many of the problems commonly associated with reference beam configurations. The system is demonstrated for the laser diode operating in cw and pulsed modes, to demonstrate its applicability to wavelength and time division multiplexing schemes for 3D laser Doppler velocimetry. The performance of the probe is investigated by measuring the velocity of a spinning disk in the range −20 m/s to +20 m/s.

Published

1995

49. High-content screening of peptide-based non-viral gene delivery systems

Author

Markus de Raad, Daphne Lelieveld, Enrico Mastrobattista, Erik A. Teunissen, and David A. Egan

Subjects

Cell Membrane Permeability, Cell Survival, viruses, High-throughput screening, Cell, Pharmaceutical Science, Cell Count, Computational biology, Biology, Gene delivery, Transfection, Peptide Library, High-Throughput Screening Assays, Chlorocebus aethiops, medicine, Animals, Peptide library, Cytotoxicity, Molecular biology, medicine.anatomical_structure, Microscopy, Fluorescence, High-content screening, embryonic structures, COS Cells, Peptides

Abstract

High-content screening (HCS) uses high-capacity automated fluorescence imaging for the quantitative analysis of single cells and cell populations. Here, we developed an HCS assay for rapid screening of non-viral gene delivery systems as exemplified by the screening of a small library of peptide-based transfectants. These peptides were simultaneously screened for transfection efficiency, cytotoxicity, induction of cell permeability and the capacity to transfect non-dividing cells. We demonstrated that HCS is a valuable extension to the already existing screening methods for the in vitro evaluation of non-viral gene delivery systems with the added value that multiple parameters can be screened in parallel thereby obtaining more information from a single screening event, which will accelerate the development of novel gene delivery systems.

Published

2011

50. Equilibrium denaturation of recombinant human FK binding protein in urea

Author

Edmund D. Matayoshi, Timothy M. Logan, David A. Egan, Heng Liang, Thomas F. Holzman, and Stephen W. Fesik

Subjects

Models, Molecular, Protein Denaturation, Magnetic Resonance Spectroscopy, Protein Conformation, Biochemistry, Tacrolimus, Tacrolimus Binding Proteins, chemistry.chemical_compound, Protein structure, Humans, Urea, Denaturation (biochemistry), Amino Acid Sequence, Peptidylprolyl isomerase, Circular Dichroism, Binding protein, digestive, oral, and skin physiology, Tryptophan, Recombinant Proteins, Kinetics, Spectrometry, Fluorescence, FKBP, chemistry, Biophysics, Spectrophotometry, Ultraviolet, Carrier Proteins, Heteronuclear single quantum coherence spectroscopy

Abstract

The equilibrium folding behavior of recombinant human FK-binding protein, a peptidyl-prolyl cis-trans-isomerase, was examined by urea-induced denaturation using probes of protein structure including intrinsic tryptophan fluorescence, second-derivative UV absorbance, CD, and NMR. All optical probes of protein structure indicate that FKBP is capable of folding reversibly. The second-derivative UV absorbance and CD probes of the structure exhibited urea denaturation transitions at approximately 4.3 M urea. The fluorescence of the single protein tryptophan is quenched in the folded state. During the unfolding-folding transition, the unquenching of tryptophan fluorescence occurs at a slightly lower urea concentration (3.9 M urea) than the changes observed for the other optical probes of folding. These probes of structure demonstrate little dependence on protein concentration in the range of 0.2- approximately 3 mg/mL across the urea-induced denaturation transition. The reversibility of the unfolding-folding transition was confirmed from two-dimensional 15N/1H heteronuclear single-quantum coherence (HSQC) spectra of [U-15N]FKBP. In addition, the native-denatured transitions for 57 individual amino acids were determined from an analysis of these spectra acquired at different urea concentrations. Analysis of the transitions for all clearly observable HSQC cross peaks for residues distributed throughout the protein and comparison to the optical folding transitions, indicate that FKBP global folding is consistent with a two-state process. Although direct measurement of FKBP catalytic activity in urea was complex, enzyme activity was observed up to the beginning of the FKBP urea-denaturation transition.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993