Your search keyword '"Ulrike Philippar"' showing total 47 results

1. Bleximenib, the novel menin-KMT2A inhibitor JNJ-75276617, impairs long-term proliferation and immune evasion in acute myeloid leukemia

Author

Shanna M. Hogeling, Duy Minh Lê, Nikita La Rose, Min Chul Kwon, Albertus T.J. Wierenga, Fiona A.J. van den Heuvel, Vincent van den Boom, Anna Kuchnio, Ulrike Philippar, Gerwin Huls, and Jan Jacob Schuringa

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Acute myeloid leukemia (AML) remains challenging to treat, which in part relates to genetic heterogeneity of the disease, to the protective tumor microenvironment driving resistance to therapy, and also to immune evasion characteristics of leukemic cells. Targeting epigenetic programs in AML provides an attractive opportunity to impair long-term proliferation and induce differentiation. The novel inhibitor JNJ- 75276617 (bleximenib) targets the menin-KMT2A interaction and provides preclinical efficacy in AML (Kwon et al1). Here, we provide mechanistic insight in how JNJ- 75276617 impairs proliferation and drives differentiation of primary AML patient cells. A large-scale drug screen was set up in which genetic alterations and quantitative proteomics were compared with drug sensitivity in a preclinical setting, which revealed that granulocyte macrophage progenitor (GMP)-like AMLs display the greatest sensitivity. Furthermore, we identified that NPM1c/DNMT3Amut AMLs are sensitive, and some NPM1wt AML subtypes without KMT2A-MLLT3 rearrangements benefit from menin-KMT2A inhibition. Genome-wide ChIP-seq studies revealed patient-specific epigenetic alterations upon JNJ-75276617 treatment, uncovering a striking upregulation of MHC class I and class II expression as a consequence of epigenetic changes upon menin-KMT2A inhibition, independent of MEIS1 loss but involving CIITA activation. Functionally, this results in enhanced sensitivity of leukemic blasts to T cell-mediated cytotoxicity in allogeneic and autologous settings. Our data indicate that JNJ-75276617 provides a potential therapeutic approach whereby not only proliferation is impaired and differentiation is induced, but whereby therapeutic benefit might also be achieved by reactivating the antigen presentation machinery.

Published

2024

2. The methyltransferase domain of DNMT1 is an essential domain in acute myeloid leukemia independent of DNMT3A mutation

Author

Balpreet Bhogal, Barbara A. Weir, Ramona Crescenzo, Ann Marien, Min Chul Kwon, Ulrike Philippar, and Glenn S. Cowley

Subjects

Biology (General), QH301-705.5

Abstract

The methyltransferase domain of DNA methyltransferase protein 1 is an essential functional domain in acute myeloid leukemia, which is independent of DNMT3A mutation.

Published

2022

3. P624: PHASE 1 STUDY OF JNJ-67856633, A FIRST-IN-HUMAN HIGHLY SELECTIVE MALT1 INHIBITOR, IN RELAPSED/REFRACTORY (R/R) B-CELL NON-HODGKIN LYMPHOMA (B-NHL) AND CHRONIC LYMPHOCYTIC LEUKEMIA (CLL)

Author

Matko Kalac, Mark Hertzberg, Chan Cheah, Vincent Ribrag, Pablo Abrisquet Acosta, Stephen Opat, Emmanuel Bachy, Loïc Ysebaert, Lihua Qiu, Shuhua Yi, Noriko Nishimura, Charlotte Lemech, Jacqueline Bussolari, Changchun Deng, Tianbao Lu, Liang Xiu, Sandy Van Hemelryck, Ulrike Philippar, Yue Guo, Virginie Soete, Isabel Soriano, Nele Fourneau, John Gerecitano, and Franck Morschhauser

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2023

4. Predictive genes in adjacent normal tissue are preferentially altered by sCNV during tumorigenesis in liver cancer and may rate limiting.

Author

John R Lamb, Chunsheng Zhang, Tao Xie, Kai Wang, Bin Zhang, Ke Hao, Eugene Chudin, Hunter B Fraser, Joshua Millstein, Mark Ferguson, Christine Suver, Irena Ivanovska, Martin Scott, Ulrike Philippar, Dimple Bansal, Zhan Zhang, Julja Burchard, Ryan Smith, Danielle Greenawalt, Michele Cleary, Jonathan Derry, Andrey Loboda, James Watters, Ronnie T P Poon, Sheung T Fan, Chun Yeung, Nikki P Y Lee, Justin Guinney, Cliona Molony, Valur Emilsson, Carolyn Buser-Doepner, Jun Zhu, Stephen Friend, Mao Mao, Peter M Shaw, Hongyue Dai, John M Luk, and Eric E Schadt

Subjects

Medicine, Science

Abstract

BackgroundIn hepatocellular carcinoma (HCC) genes predictive of survival have been found in both adjacent normal (AN) and tumor (TU) tissues. The relationships between these two sets of predictive genes and the general process of tumorigenesis and disease progression remains unclear.Methodology/principal findingsHere we have investigated HCC tumorigenesis by comparing gene expression, DNA copy number variation and survival using ∼250 AN and TU samples representing, respectively, the pre-cancer state, and the result of tumorigenesis. Genes that participate in tumorigenesis were defined using a gene-gene correlation meta-analysis procedure that compared AN versus TU tissues. Genes predictive of survival in AN (AN-survival genes) were found to be enriched in the differential gene-gene correlation gene set indicating that they directly participate in the process of tumorigenesis. Additionally the AN-survival genes were mostly not predictive after tumorigenesis in TU tissue and this transition was associated with and could largely be explained by the effect of somatic DNA copy number variation (sCNV) in cis and in trans. The data was consistent with the variance of AN-survival genes being rate-limiting steps in tumorigenesis and this was confirmed using a treatment that promotes HCC tumorigenesis that selectively altered AN-survival genes and genes differentially correlated between AN and TU.Conclusions/significanceThis suggests that the process of tumor evolution involves rate-limiting steps related to the background from which the tumor evolved where these were frequently predictive of clinical outcome. Additionally treatments that alter the likelihood of tumorigenesis occurring may act by altering AN-survival genes, suggesting that the process can be manipulated. Further sCNV explains a substantial fraction of tumor specific expression and may therefore be a causal driver of tumor evolution in HCC and perhaps many solid tumor types.

Published

2011

5. Gene signatures derived from a c-MET-driven liver cancer mouse model predict survival of patients with hepatocellular carcinoma.

Author

Irena Ivanovska, Chunsheng Zhang, Angela M Liu, Kwong F Wong, Nikki P Lee, Patrick Lewis, Ulrike Philippar, Dimple Bansal, Carolyn Buser, Martin Scott, Mao Mao, Ronnie T P Poon, Sheung Tat Fan, Michele A Cleary, John M Luk, and Hongyue Dai

Subjects

Medicine, Science

Abstract

Biomarkers derived from gene expression profiling data may have a high false-positive rate and must be rigorously validated using independent clinical data sets, which are not always available. Although animal model systems could provide alternative data sets to formulate hypotheses and limit the number of signatures to be tested in clinical samples, the predictive power of such an approach is not yet proven. The present study aims to analyze the molecular signatures of liver cancer in a c-MET-transgenic mouse model and investigate its prognostic relevance to human hepatocellular carcinoma (HCC). Tissue samples were obtained from tumor (TU), adjacent non-tumor (AN) and distant normal (DN) liver in Tet-operator regulated (TRE) human c-MET transgenic mice (n = 21) as well as from a Chinese cohort of 272 HBV- and 9 HCV-associated HCC patients. Whole genome microarray expression profiling was conducted in Affymetrix gene expression chips, and prognostic significances of gene expression signatures were evaluated across the two species. Our data revealed parallels between mouse and human liver tumors, including down-regulation of metabolic pathways and up-regulation of cell cycle processes. The mouse tumors were most similar to a subset of patient samples characterized by activation of the Wnt pathway, but distinctive in the p53 pathway signals. Of potential clinical utility, we identified a set of genes that were down regulated in both mouse tumors and human HCC having significant predictive power on overall and disease-free survival, which were highly enriched for metabolic functions. In conclusions, this study provides evidence that a disease model can serve as a possible platform for generating hypotheses to be tested in human tissues and highlights an efficient method for generating biomarker signatures before extensive clinical trials have been initiated.

Published

2011

6. Discovery of JNJ-64264681: A Potent and Selective Covalent Inhibitor of Bruton’s Tyrosine Kinase

Author

Mark S. Tichenor, John J. M. Wiener, Navin L. Rao, Genesis M. Bacani, Jianmei Wei, Charlotte Pooley Deckhut, J. Kent Barbay, Kevin D. Kreutter, Leon Chang, Kathleen W. Clancy, Heather E. Murrey, Weixue Wang, Kay Ahn, Michael Huber, Elizabeth Rex, Kevin J. Coe, Jiejun Wu, Haopeng Rui, Kia Sepassi, Marcello Gaudiano, Mariette Bekkers, Ivo Cornelissen, Kathryn Packman, Mark Seierstad, Christos Xiouras, Scott D. Bembenek, Richard Alexander, Cynthia Milligan, Sriram Balasubramanian, Alec D. Lebsack, Jennifer D. Venable, Ulrike Philippar, James P. Edwards, and Gavin Hirst

Subjects

Arthritis, Rheumatoid, Drug Discovery, Agammaglobulinaemia Tyrosine Kinase, Humans, Lupus Erythematosus, Systemic, Molecular Medicine, Protein Kinase Inhibitors, Autoimmune Diseases

Abstract

Bruton's tyrosine kinase (BTK) is a Tec family kinase that plays an essential role in B-cell receptor (BCR) signaling as well as Fcγ receptor signaling in leukocytes. Pharmacological inhibition of BTK has been shown to be effective in treating hematological malignancies and is hypothesized to provide an effective strategy for the treatment of autoimmune diseases such as rheumatoid arthritis and systemic lupus erythematosus. We report the discovery and preclinical properties of JNJ-64264681 (

Published

2022

7. Data from BCL10 Mutations Define Distinct Dependencies Guiding Precision Therapy for DLBCL

Author

Ari M. Melnick, Hao Wu, Lorena Fontan, Ulrike Philippar, Tianbao Lu, Leandro Cerchietti, Nahuel Zamponi, Kojo S.J. Elenitoba-Johnson, Ozlem Onder, Ryan D. Morin, David W. Scott, Graham W. Slack, Andrew Lytle, Cem Meydan, Xiang Wang, Johana Gutierrez, Matt Teater, Liron David, and Min Xia

Abstract

Activated B cell–like diffuse large B-cell lymphomas (ABC-DLBCL) have unfavorable outcomes and chronic activation of CARD11–BCL10–MALT1 (CBM) signal amplification complexes that form due to polymerization of BCL10 subunits, which is affected by recurrent somatic mutations in ABC-DLBCLs. Herein, we show that BCL10 mutants fall into at least two functionally distinct classes: missense mutations of the BCL10 CARD domain and truncation of its C-terminal tail. Truncating mutations abrogated a motif through which MALT1 inhibits BCL10 polymerization, trapping MALT1 in its activated filament-bound state. CARD missense mutations enhanced BCL10 filament formation, forming glutamine network structures that stabilize BCL10 filaments. Mutant forms of BCL10 were less dependent on upstream CARD11 activation and thus manifested resistance to BTK inhibitors, whereas BCL10 truncating but not CARD mutants were hypersensitive to MALT1 inhibitors. Therefore, BCL10 mutations are potential biomarkers for BTK inhibitor resistance in ABC-DLBCL, and further precision can be achieved by selecting therapy based on specific biochemical effects of distinct mutation classes.Significance:ABC-DLBCLs feature frequent mutations of signaling mediators that converge on the CBM complex. We use structure–function approaches to reveal that BCL10 mutations fall into two distinct biochemical classes. Both classes confer resistance to BTK inhibitors, whereas BCL10 truncations confer hyperresponsiveness to MALT1 inhibitors, providing a road map for precision therapies in ABC-DLBCLs.See related commentary by Phelan and Oellerich, p. 1844.This article is highlighted in the In This Issue feature, p. 1825

Published

2023

8. Supplementary Figure from BCL10 Mutations Define Distinct Dependencies Guiding Precision Therapy for DLBCL

Author

Ari M. Melnick, Hao Wu, Lorena Fontan, Ulrike Philippar, Tianbao Lu, Leandro Cerchietti, Nahuel Zamponi, Kojo S.J. Elenitoba-Johnson, Ozlem Onder, Ryan D. Morin, David W. Scott, Graham W. Slack, Andrew Lytle, Cem Meydan, Xiang Wang, Johana Gutierrez, Matt Teater, Liron David, and Min Xia

Abstract

Supplementary Figure from BCL10 Mutations Define Distinct Dependencies Guiding Precision Therapy for DLBCL

Published

2023

9. Supplementary Data from BCL10 Mutations Define Distinct Dependencies Guiding Precision Therapy for DLBCL

Author

Ari M. Melnick, Hao Wu, Lorena Fontan, Ulrike Philippar, Tianbao Lu, Leandro Cerchietti, Nahuel Zamponi, Kojo S.J. Elenitoba-Johnson, Ozlem Onder, Ryan D. Morin, David W. Scott, Graham W. Slack, Andrew Lytle, Cem Meydan, Xiang Wang, Johana Gutierrez, Matt Teater, Liron David, and Min Xia

Abstract

Supplementary Data from BCL10 Mutations Define Distinct Dependencies Guiding Precision Therapy for DLBCL

Published

2023

10. Supplementary Figures from Discovery of a Novel ERK Inhibitor with Activity in Models of Acquired Resistance to BRAF and MEK Inhibitors

Author

Ahmed A. Samatar, Stephen Fawell, Leigh Zawel, Lata Jayaraman, D. Gary Gilliland, Daniel Hicklin, W. Robert Bishop, Paul Kirschmeier, David Witter, Phieng Siliphaivanh, Ulrike Philippar, Marc R. Pelletier, Bart A. Lutterbach, Ling Zhang, Pierre Daublain, Liang Zhu, Boga Sobhana Babu, Xiaolei Gao, Sunil Paliwal, Joe Kelly, James Wang, Alan Hruza, Gerald Shipps, Li Xiao, Jagdish Desai, Elaine M. Pinheiro, Minilik H. Angagaw, Shuxia Zhao, Rumin Zhang, William Windsor, Edward DiNunzio, Jenny Liu, Brian Long, Stuart Black, Weihong Jin, Yongi Deng, Donna Carr, Alan Cooper, Hugh Zhu, Priya Dayananth, Clifford R. Restaino, Sharda Jha, and Erick J. Morris

Abstract

Supplementary Figures - PDF file 1385K, File contains Supplementary figures of resistant cell lines, proliferation assay of a panel of cell lines, TdF binding assay transcriptional out and kinome selectivity

Published

2023

11. Pharmacological Characterization of JNJ-75276617, a Menin-KMT2A Inhibitor, As Targeted Treatment for KMT2A-Altered and NPM1-Mutant Acute Leukemia

Author

Min Chul Kwon, Olivier Querolle, Xuedong Dai, Jan Willem Thuring, Tinne Verhulst, Ann Marien, Dries Goffin, Wei Cai, Vikki Keersmaekers, Filmon Eyassu, Karin Verstraeten, Sara El Ashkar, Shanna M Hogeling, Frank Jacob, Petra Vinken, Nicolas Darville, Vineet Pande, Daniel Krosky, Gregor Urbanietz, Bie Verbist, Lucille A. Ferrante, Christina Diane Drenberg, David Wilson, Ricardo M. Attar, Jan Jacob Schuringa, Nikki Daskalakis, Kathryn Packman, Christine Pietsch, Yusri Elsayed, and Ulrike Philippar

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

12. Characterization of JNJ-80948543, a Novel CD79bxCD20xCD3 Trispecific T-Cell Redirecting Antibody for the Treatment of B-Cell Non-Hodgkin Lymphoma

Author

Anna Kuchnio, Danlin Yang, Nele Vloemans, Cassandra Lowenstein, Ivo Cornelissen, Ricardo Amorim, Chao Han, Siddharth Sukumaran, Lut Janssen, Toon Suls, Mariette Bekkers, Elena Lasorsa, Lorena Fontana, Nicole Medeiros, Bingyuan Wu, Jun Chen, Michael Feldkamp, Sheng-Jiun Wu, Habtom Habte, John Krayer, Cam Holland, M. Phillip Deyoung, Yusri A Elsayed, and Ulrike Philippar

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

13. BCL10 Mutations Define Distinct Dependencies Guiding Precision Therapy for DLBCL

Author

Min Xia, Liron David, Matt Teater, Johana Gutierrez, Xiang Wang, Cem Meydan, Andrew Lytle, Graham W. Slack, David W. Scott, Ryan D. Morin, Ozlem Onder, Kojo S.J. Elenitoba-Johnson, Nahuel Zamponi, Leandro Cerchietti, Tianbao Lu, Ulrike Philippar, Lorena Fontan, Hao Wu, and Ari M. Melnick

Subjects

CARD Signaling Adaptor Proteins, Oncology, Carcinogenesis, Guanylate Cyclase, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, Mutation, NF-kappa B, Humans, Lymphoma, Large B-Cell, Diffuse, Precision Medicine, B-Cell CLL-Lymphoma 10 Protein, Article, Signal Transduction

Abstract

Activated B cell–like diffuse large B-cell lymphomas (ABC-DLBCL) have unfavorable outcomes and chronic activation of CARD11–BCL10–MALT1 (CBM) signal amplification complexes that form due to polymerization of BCL10 subunits, which is affected by recurrent somatic mutations in ABC-DLBCLs. Herein, we show that BCL10 mutants fall into at least two functionally distinct classes: missense mutations of the BCL10 CARD domain and truncation of its C-terminal tail. Truncating mutations abrogated a motif through which MALT1 inhibits BCL10 polymerization, trapping MALT1 in its activated filament-bound state. CARD missense mutations enhanced BCL10 filament formation, forming glutamine network structures that stabilize BCL10 filaments. Mutant forms of BCL10 were less dependent on upstream CARD11 activation and thus manifested resistance to BTK inhibitors, whereas BCL10 truncating but not CARD mutants were hypersensitive to MALT1 inhibitors. Therefore, BCL10 mutations are potential biomarkers for BTK inhibitor resistance in ABC-DLBCL, and further precision can be achieved by selecting therapy based on specific biochemical effects of distinct mutation classes. Significance: ABC-DLBCLs feature frequent mutations of signaling mediators that converge on the CBM complex. We use structure–function approaches to reveal that BCL10 mutations fall into two distinct biochemical classes. Both classes confer resistance to BTK inhibitors, whereas BCL10 truncations confer hyperresponsiveness to MALT1 inhibitors, providing a road map for precision therapies in ABC-DLBCLs.

Published

2021

14. The methyltransferase domain of DNMT1 is an essential domain in acute myeloid leukemia independent of DNMT3A mutation

Author

Balpreet Bhogal, Barbara A. Weir, Ramona Crescenzo, Ann Marien, Min Chul Kwon, Ulrike Philippar, and Glenn S. Cowley

Subjects

Leukemia, Myeloid, Acute, Mutation, Medicine (miscellaneous), Humans, Methyltransferases, DNA (Cytosine-5-)-Methyltransferases, DNA, General Agricultural and Biological Sciences, General Biochemistry, Genetics and Molecular Biology, DNA Methyltransferase 3A

Abstract

Aberrant DNA methylation patterns are a prominent feature of cancer. Methylation of DNA is mediated by the DNA methyltransferase (DNMT) protein family, which regulates de novo (DNMT3A and DNMT3B) and maintenance (DNMT1) methylation. Mutations in DNMT3A are observed in approximately 22% of acute myeloid leukemia (AML). We hypothesized that DNMT1 or DNMT3B could function as a synthetic lethal therapeutic strategy for DNMT3A-mutant AML. CRISPR-Cas9 tiling screens were performed to identify functional domains within DNMT1/DNMT3B that exhibited greater dependencies in DNMT3A mutant versus wild-type cell lines. Although increased sensitivity to DNMT1 mutation was observed in some DNMT3A mutant cellular models tested, the subtlety of these results prevents us from basing any conclusions on a synthetic lethal relationship between DNMT1 and DNMT3A. Our data suggests that a therapeutic window for DNMT1 methyltransferase inhibition in DNMT3A-driven AML may exist, but validation in more biologically relevant models is required.

Published

2021

15. Influence of the bispecific antibody IgG subclass on T cell redirection

Author

Ulrike Philippar, Erna Cleiren, Julien Häsler, Ricardo Attar, Mark L. Chiu, and Stephanie Kapelski

Subjects

CD3 Complex, bispecific antibody structure, T-Lymphocytes, T cell, Antigens, CD19, Immunology, Cell Line, T cell redirection, Immunological synapse, Immunoglobulin Fab Fragments, 03 medical and health sciences, 0302 clinical medicine, Antigen, Report, Antibodies, Bispecific, medicine, Humans, Immunology and Allergy, Bovine serum albumin, 030304 developmental biology, Antibody-dependent cell-mediated cytotoxicity, 0303 health sciences, antibody engineering, biology, Chemistry, Cell sorting, Molecular biology, Immunoglobulin Fc Fragments, medicine.anatomical_structure, CD19xCD3, Immunoglobulin G, 030220 oncology & carcinogenesis, Mutation, biology.protein, Ethanesulfonic acid, Fetal bovine serum

Abstract

T cell redirection mediated by bispecific antibodies (BsAbs) is a promising cancer therapy. Dual antigen binding is necessary for potent T cell redirection and is influenced by the structural characteristics of a BsAb, which are dependent on its IgG subclass. In this study, model BsAbs targeting CD19xCD3 were generated in variants of IgG1, IgG2, and IgG4 carrying Fc mutations that reduce FcγR interaction, and two chimeric IgG subclasses termed IgG1:2 and IgG4:2, in which the IgG1- or IgG4-F(ab)2 are grafted on an IgG2 Fc. Molecules containing an IgG2 or IgG4-F(ab)2 domain were confirmed to be the most structurally compact molecules. All BsAbs were shown to bind both of their target proteins (and corresponding cells) equally well. However, CD19xCD3 IgG2 did not bind both antigens simultaneously as measured by the absence of cellular clustering of T cells with target cells. This translated to a reduced potency of IgG2 BsAbs in T-cell redirection assays. The activity of IgG2 BsAbs was fully restored in the chimeric subclasses IgG4:2 and IgG1:2. This confirmed the major contribution of the F(ab)2 region to the BsAb’s functional activity and demonstrated that function of BsAbs can be modulated by engineering molecules combining different Fc and F(ab)2 domains. Abbreviations: ADCC: Antibody-dependent cellular cytotoxicity; AlphaScreenTM: Amplified Luminescent Proximity Homogeneous Assay Screening; ANOVA: Analysis of variance; BiTE: bispecific T-cell engager; BSA: bovine serum albumin; BsAb: bispecific antibody; cFAE: controlled Fab-arm exchange; CDC: complement-dependent cellular cytotoxicity; CIEX: cation-exchange; CIR: chimeric immune receptor; DPBS: Dulbecco’s phosphate-buffered saline; EC50 value: effective concentration to reach half-maximum effect; EGFR: epidermal growth factor receptor; EI: expansion index (RAt=x/RAt=0); FACS: fluorescence-activated cell sorting; FVD: fixable viability dye; HI-HPLC: hydrophobic interaction HPLC; HI-FBS: heat-inactivated fetal bovine serum; HPLC: high-pressure liquid chromatography; IC50 value: effective concentration to reach half-maximum inhibition; IQ: Inhibition Quotient; IS: immunological synapse; MES: 2-(N-morpholino)ethanesulfonic acid; R-PE: recombinant phycoerythrin; RA: red area in μm2/well; RD: receptor density; RFP: red fluorescent protein; Rg: radius of gyration; RSV: respiratory syncytial virus; SAXS: small-angle x-ray scattering; scFv: single-chain variable fragment; SD: standard deviation; SPR: surface plasmon resonance; WT: wild-type

Published

2019

16. Discovery of Highly Potent and Selective IRAK1 Degraders to Probe Scaffolding Functions of IRAK1 in ABC DLBCL

Author

Paul Gavine, Tu Wangyang, Dai Xuedong, Ricardo Attar, Yingtao Liu, Jing Zhang, Wenqian Wang, Liu Qian, Xu Yanping, Linglong Kong, Fu Liqiang, Ulrike Philippar, Xiaotao Wang, Na Cheng, James P. Edwards, Bin Shen, Jennifer Yang, Jennifer D. Venable, Mingxuan Xia, Xin Cai, and Tianyuan Zhou

Subjects

Cell Survival, Antineoplastic Agents, medicine.disease_cause, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, medicine, Humans, Kinase activity, Protein Kinase Inhibitors, Cell Proliferation, Mutation, Dose-Response Relationship, Drug, Molecular Structure, Kinase, Chemistry, IRAK1, medicine.disease, MYD88 Gene Mutation, Lymphoma, Interleukin-1 Receptor-Associated Kinases, Essential gene, Cancer research, Molecular Medicine, Lymphoma, Large B-Cell, Diffuse, Drug Screening Assays, Antitumor, Function (biology)

Abstract

MyD88 gene mutation has been identified as one of the most prevalent driver mutations in the activated B-cell-like diffuse large B-cell lymphoma (ABC DLBCL). The published literature suggests that interleukin-1 receptor-associated kinase 1 (IRAK1) is an essential gene for ABC DLBCL harboring MyD88 mutation. Importantly, the scaffolding function of IRAK1, rather than its kinase activity, is required for tumor cell survival. Herein, we present our design, synthesis, and biological evaluation of a novel series of potent and selective IRAK1 degraders. One of the most potent compounds, Degrader-3 (JNJ-1013), effectively degraded cellular IRAK1 protein with a DC50 of 3 nM in HBL-1 cells. Furthermore, JNJ-1013 potently inhibited IRAK1 downstream signaling pathways and demonstrated strong anti-proliferative effects in ABC DLBCL cells with MyD88 mutation. This work suggests that IRAK1 degraders have the potential for treating cancers that are dependent on the IRAK1 scaffolding function.

Published

2021

17. Discovery and Pharmacological Characterization of JNJ-64619178, a Novel Small-Molecule Inhibitor of PRMT5 with Potent Antitumor Activity

Author

Tinne Verhulst, Lieven Meerpoel, Emmanuel Gustin, Weimei Sun, Matthew V. Lorenzi, Junchen Gu, Longen Zhou, Wim Bert Griet Schepens, Hillary Millar, Tongfei Wu, Viellevoye Marcel, Vineet Pande, Petra Vinken, Desiree De Lange, An Boeckx, Christopher Moy, Friederike Pastore, Geert Mannens, Sylvie Laquerre, Ulrike Philippar, Vipul Bhargava, Gaston Stanislas Marcella Diels, Thomas Nys, Kathryn Packman, Jan Willem Thuring, Erika van Heerde, Bie Verbist, Sumit Rai, Lijs Beke, Pegah Safabakhsh, Timothy A. Graubert, Yue Fan, Angelique N Gilbert, Dirk Brehmer, Vikki Keersmaekers, Barbara Morschhäuser, Danilo Fiore, David Walker, Amy J. Johnson, Brehmer, D., Beke, L., Wu, T., Millar, H. J., Moy, C., Sun, W., Mannens, G., Pande, V., Boeckx, A., van Heerde, E., Nys, T., Gustin, E. M., Verbist, B., Zhou, L., Fan, Y., Bhargava, V., Safabakhsh, P., Vinken, P., Verhulst, T., Gilbert, A., Rai, S., Graubert, T. A., Pastore, F., Fiore, D., Gu, J., Johnson, A., Philippar, U., Morschhauser, B., Walker, D., de Lange, D., Keersmaekers, V., Viellevoye, M., Diels, G., Schepens, W., Thuring, J. W., Meerpoel, L., Packman, K., Lorenzi, M. V., and Laquerre, S.

Subjects

Cancer Research, Protein-Arginine N-Methyltransferases, Lung Neoplasms, PROTEIN, Splicing factor, Mice, In vivo, REVEALS, medicine, Animals, Humans, Pyrroles, Enzyme Inhibitors, Lung cancer, VULNERABILITY, Science & Technology, business.industry, Protein arginine methyltransferase 5, PRE-MESSENGER-RNA, METHYLATION, Myeloid leukemia, SELECTIVE INHIBITOR, medicine.disease, Lymphoma, Disease Models, Animal, Pyrimidines, Oncology, Cancer research, ARGININE METHYLTRANSFERASE PRMT5, Signal transduction, business, Life Sciences & Biomedicine, Ex vivo

Abstract

The protein arginine methyltransferase 5 (PRMT5) methylates a variety of proteins involved in splicing, multiple signal transduction pathways, epigenetic control of gene expression, and mechanisms leading to protein expression required for cellular proliferation. Dysregulation of PRMT5 is associated with clinical features of several cancers, including lymphomas, lung cancer, and breast cancer. Here, we describe the characterization of JNJ-64619178, a novel, selective, and potent PRMT5 inhibitor, currently in clinical trials for patients with advanced solid tumors, non-Hodgkin's lymphoma, and lower-risk myelodysplastic syndrome. JNJ-64619178 demonstrated a prolonged inhibition of PRMT5 and potent antiproliferative activity in subsets of cancer cell lines derived from various histologies, including lung, breast, pancreatic, and hematological malignancies. In primary acute myelogenous leukemia samples, the presence of splicing factor mutations correlated with a higher ex vivo sensitivity to JNJ-64619178. Furthermore, the potent and unique mechanism of inhibition of JNJ-64619178, combined with highly optimized pharmacological properties, led to efficient tumor growth inhibition and regression in several xenograft models in vivo, with once-daily or intermittent oral-dosing schedules. An increase in splicing burden was observed upon JNJ-64619178 treatment. Overall, these observations support the continued clinical evaluation of JNJ-64619178 in patients with aberrant PRMT5 activity-driven tumors. ispartof: MOLECULAR CANCER THERAPEUTICS vol:20 issue:12 pages:2317-2328 ispartof: location:United States status: published

Published

2021

18. Abstract 2133: In pursuit of MCL-1 inhibitors with improved therapeutic window for the treatment of hematological malignancies: Discovery of JNJ-4355

Author

Frederik J. Rombouts, Lento William, Ingrid Velter, Ann Vos, Aldo Peschiulli, Reuillon Tristan, Maria Dominguez Blanco, Matthieu Jouffroy, Lisa McQueen, Helena Steyvers, Mariette Bekkers, Cristina Altrocchi, Beth Pietrak, Seong Joo Koo, Lawrence Szewczuk, David Walker, Kathryn Packman, Ruud Bueters, Petra Vinken, Amy Johnson, Ricardo Attar, and Ulrike Philippar

Subjects

Cancer Research, Oncology

Abstract

Appropriate control of cell death is a fundamental biological process which is frequently dysregulated during tumor development and therapeutic resistance. Apoptosis is a form of regulated cell death initiated by either the extracellular environment (extrinsic) or following internal cellular damage (intrinsic). It is controlled by the BCL-2 family which includes anti-apoptotic regulators like BCL-2, BCL-XL and MCL-1 that bind and sequester various pro-apoptotic BH3-only proteins (BIM, BAD, BID, NOXA, PUMA, etc.), and the pro-apoptotic effectors (BAK, BAX, etc.) responsible for mitochondrial pore formation and MOMP (mitochondrial outer membrane permeabilization). MOMP results in intermembrane space protein release, leading to caspase activation in an irreversible path to programmed cell death. Of the anti-apoptotic regulators, MCL-1 is one of the most frequently and highly amplified genes in human cancers such as myeloid leukemia making it a compelling therapeutic target. Since BCL-2 proteins interact through protein-protein interactions, they have long been elusive targets. The success of selective BCL-2 protein inhibitor Venetoclax in the treatment of various hematological cancers, however spurred interest in MCL-1 as an oncology target. Using structure-based drug design, major breakthroughs were made in the development of MCL-1 inhibitors, with several candidates entering clinical studies in the past five years. JNJ-4355, a highly potent 1,4-indolyl macrocycle (MCL-1 Ki = 18 pM, Cell (MOLP8) AC50 = 8.7 nM) was optimized to address shortcomings from first generation MCL-1 inhibitors: it has improved physicochemical properties (CHI LogD7.4 = 2.35, EPSA = 151 Å2), resulting in greatly improved equilibrium solubility (3.14 mM in buffer pH 7) and reduced protein binding (99.93%). JNJ-4355 showed promising in vitro potency data in cancer cell lines and AML patient-derived samples (cell killing AC50 0.29-75 nM in 25/27 evaluable samples). In vivo MCL-1:BAK complex disruption was confirmed in a mouse MOLM13 (AML) xenograft. Efficacy was demonstrated in a mouse MOLP8 (multiple myeloma) xenograft resulting in complete tumor regression after a single IV dose of JNJ-4355. Citation Format: Frederik J. Rombouts, Lento William, Ingrid Velter, Ann Vos, Aldo Peschiulli, Reuillon Tristan, Maria Dominguez Blanco, Matthieu Jouffroy, Lisa McQueen, Helena Steyvers, Mariette Bekkers, Cristina Altrocchi, Beth Pietrak, Seong Joo Koo, Lawrence Szewczuk, David Walker, Kathryn Packman, Ruud Bueters, Petra Vinken, Amy Johnson, Ricardo Attar, Ulrike Philippar. In pursuit of MCL-1 inhibitors with improved therapeutic window for the treatment of hematological malignancies: Discovery of JNJ-4355 [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 2133.

Published

2022

19. Assessing IRAK4 Functions in ABC DLBCL by IRAK4 Kinase Inhibition and Protein Degradation

Author

Amanda Del Rosario, Tianyuan Zhou, Zhuming Zhang, Kay Ahn, James P. Edwards, Linglong Kong, Ricardo Attar, Dai Xuedong, Yingtao Liu, Jennifer Yang, Jing Zhang, Bin Shen, Fu Liqiang, Wenqian Wang, Liu Qian, Ying-Nan P. Chen, Paul Gavine, Ulrike Philippar, Ryan Meng, Xu Yanping, Yilin Yan, Xin Cai, Zhao-Kui Wan, and Xiaotao Wang

Subjects

Programmed cell death, Clinical Biochemistry, Biology, Protein degradation, 01 natural sciences, Biochemistry, Serine, chemistry.chemical_compound, Cell Line, Tumor, Drug Discovery, medicine, Humans, Molecular Biology, Protein Kinase Inhibitors, Pharmacology, Innate immune system, 010405 organic chemistry, Kinase, IRAK4, medicine.disease, 0104 chemical sciences, Interleukin-1 Receptor-Associated Kinases, chemistry, Drug Design, Proteolysis, Cancer research, Molecular Medicine, Lymphoma, Large B-Cell, Diffuse, Growth inhibition, Diffuse large B-cell lymphoma

Abstract

The interleukin-1 receptor-activated kinase 4 (IRAK4) belongs to the IRAK family of serine/threonine kinases and plays a central role in the innate immune response. However, the function of IRAK4 in tumor growth and progression remains elusive. Here we sought to determine the enzymatic and scaffolding functions of IRAK4 in activated B-cell-like diffuse large B cell lymphoma (ABC DLBCL). We chose a highly selective IRAK4 kinase inhibitor to probe the biological effects of kinase inhibition and developed a series of IRAK4 degraders to evaluate the effects of protein degradation in ABC DLBCL cells. Interestingly, the results demonstrated that neither IRAK4 kinase inhibition nor protein degradation led to cell death or growth inhibition, suggesting a redundant role for IRAK4 in ABC DLBCL cell survival. IRAK4 degraders characterized in this study provide useful tools for understanding IRAK4 protein scaffolding function, which was previously unachievable using pharmacological perturbation.

Published

2020

20. Discovery and optimization of a series of small-molecule allosteric inhibitors of MALT1 protease

Author

Weimei Sun, James P. Edwards, Ricardo Attar, Tianbao Lu, Nigel Austin, Lieven Meerpoel, Ann Cai, Luc Gys, Ulrike Philippar, Maxwell D. Cummings, Kent Barbay, Peter J. Connolly, Luc Van Nuffel, Mariette Bekkers, and Shen Fang

Subjects

chemistry.chemical_classification, Protease, medicine.medical_treatment, RELB, Organic Chemistry, Clinical Biochemistry, Allosteric regulation, Assay, Pharmaceutical Science, Biochemistry, Small molecule, Jurkat cells, Enzyme, chemistry, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, Cell Line, Tumor, Drug Discovery, medicine, Molecular Medicine, Humans, Molecular Biology, IC50

Abstract

We describe a series of potent and highly selective small-molecule MALT1 inhibitors, optimized from a High-Throughput Screening hit. Advanced analogues such as compound 40 show high potency (IC50: 0.01 µM) in a biochemical assay measuring MALT1 enzymatic activity, as well as in cellular assays: Jurkat T cell activation (0.05 µM) and IL6/10 secretion (IC50: 0.10/0.06 µM) in the TMD8 B-cell lymphoma line. Compound 40 also inhibited cleavage of the MALT1 substrate RelB (IC50: 0.10 µM). Mechanistic enzymology results suggest that these compounds bind to the known allosteric site of the protease.

Published

2019

21. Abstract 1256: JNJ-74856665, a novel DHODH inhibitor, mediates potent anti-leukemic activity and differentiation in vitro and in vivo

Author

Kathryn Packman, Scott D. Kuduk, Xiaochun Zhang, Ulrike Philippar, Yusri Elsayed, Andrew Steele, Jacqueline Bussolari, Weixue Wang, Gilles Bignan, Lindsey G. DeRatt, Kathryn Bradford, Ricardo Attar, Friedericke Pastore, Zhuming Zhang, Nikki Daskalakis, Edgar Jacoby, Christine Pietsch, Tony Greway, James P. Edwards, Aaron N. Patrick, Bush Tammy, and Faraz Kazmi

Subjects

Cancer Research, Myeloid, business.industry, HL60, Azacitidine, Myeloid leukemia, chemistry.chemical_compound, medicine.anatomical_structure, Oncology, chemistry, Differentiation therapy, Apoptosis, In vivo, Cancer research, medicine, Dihydroorotate dehydrogenase, business, medicine.drug

Abstract

Acute myeloid leukemia (AML) is a heterogeneous disease characterized by uncontrolled clonal expansion of hematopoietic progenitor cells (myeloid blasts). Disease remission can be achieved with standard induction chemotherapy, but refractory and relapsed disease remains a challenge with a 5-year overall survival rate of approximately 25%. Induction of differentiation is an alternative approach to AML therapy. Dihydroorotate dehydrogenase (DHODH) catalyzes the ubiquinone-mediated oxidation of dihydroorotate (DHO) to orotate in the de novo pyrimidine synthesis pathway. Pre-clinical findings demonstrated that DHODH is a metabolic vulnerability in AML and a new target for differentiation therapy. Given the genetic complexity of myeloid malignancies, future use of DHODH inhibitors in combination with selected antineoplastic agents (e.g., azacitidine) with nonoverlapping mechanisms of action may address specific aspects of the complex pathogenesis of AML and MDS (myelodysplastic syndrome), ultimately improving patients' outcomes.JNJ74856665 is an orally available, potent and selective DHODH inhibitor. JNJ-74856665 inhibited the biochemical activity of human DHODH with a 50% inhibitory concentration (IC50) in the subnanomolar range and in vitro inhibited proliferation of MOLM-13, OCI-AML3, HL60 and THP-1 AML cell lines with low nanomolar IC50 values. Mechanism of action studies using these four cell lines demonstrated induction of CD11b and CD14 differentiation marker mRNA levels. Differentiation was accompanied by cell cycle arrest and apoptosis induction. Importantly, addition of excess uridine to the tissue culture conditions abrogated the anti-proliferative, differentiation and apoptosis inducing activity of JNJ-74856665, indicating on target activity. In vivo, JNJ-74856665 mediated significant activity in decreasing leukemic burden and increasing life span across subcutaneous (MOLM-13 and OCI-AML3) and disseminated (MOLM-13) xenografts, respectively. Pharmacodynamic investigations demonstrated target engagement as evidenced by upregulation of the DHODH substrate dihydroorotate in plasma and induction of differentiation markers in tumor. Combination of JNJ-74856665 with azacitidine in vivo demonstrated lack of antagonism in the anti-leukemic activity.The results described herein demonstrate that JNJ-74856665 exerts potent anti-leukemic activity in vitro and in vivo and warrant further investigation. To that end, a phase 1 clinical trial assessing the safety and efficacy of JNJ-74856665 in patients with AML and MDS is planned to initiate shortly. Citation Format: Christine Pietsch, Scott Kuduk, Xiaochun Zhang, Tammy Bush, Faraz Kazmi, Edgar Jacoby, Zhuming Zhang, Lindsey DeRatt, Weixue Wang, Aaron Patrick, Andrew Steele, Friedericke Pastore, Tony Greway, Nikki Daskalakis, Kathryn Bradford, Kathryn Packman, Gilles Bignan, James Edwards, Ricardo Attar, Yusri Elsayed, Jacqueline Bussolari, Ulrike Philippar. JNJ-74856665, a novel DHODH inhibitor, mediates potent anti-leukemic activity and differentiation in vitro and in vivo [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1256.

Published

2021

22. Abstract 1267: Combination therapy of JNJ-67856633, a novel, first-in-class MALT1 protease inhibitor, and JNJ-64264681, a novel BTK inhibitor, for the treatment of B-cell lymphomas

Author

Ulrike Philippar, Lorena Fontan, Ivo Cornelissen, Haopeng Rui, Sriram Balasubramanian, Marcello Gaudiano, Mariette Bekkers, Luc Van Nuffel, Tianbao Lu, John Wiener, Mark Tichenor, Tony Greway, Kathryn Packman, Bie Verbist, Yusri Elsayed, Ricardo Attar, Jacqueline Bussolari, and John Gerecitano

Subjects

Cancer Research, biology, Combination therapy, CD3, breakpoint cluster region, medicine.disease, Lymphoma, chemistry.chemical_compound, medicine.anatomical_structure, Oncology, chemistry, hemic and lymphatic diseases, biology.protein, medicine, Cancer research, Bruton's tyrosine kinase, Growth inhibition, Tyrosine kinase, B cell

Abstract

Background: Constitutive activation of the classical nuclear factor kappa-light-chain-enhancer of activated B-cells (NF-κB) pathway is a clear driver of B-cell non-Hodgkin lymphomas (NHL). Bruton's Tyrosine Kinase (BTK) and Mucosa-associated lymphoid tissue lymphoma translocation protein 1 (MALT1), which lies downstream of BTK, are key mediators of the classical NF-κB signaling pathway activated by BCR and TCR receptors. JNJ-67856633 is a first-in-class MALT1 protease inhibitor. JNJ-64264681 is a BTK inhibitor with improved selectivity against BTK. Blocking the BCR pathway at multiple points using these two orally bioavailable compounds could enhance clinical activity in B-cell lymphoma patients. Methods: JNJ-67856633 and JNJ-64264681 are currently being evaluated in phase 1 clinical trials designed to establish safety, PK, PD and the Recommended Phase 2 Dose (RP2D) of each agent. Results: JNJ-67856633 is a potent, selective, orally bioavailable, allosteric inhibitor of MALT1 protease activity. The compound inhibits proliferation of activated B-cell diffuse large B-cell lymphoma (ABC-DLBCL) cell lines bearing CD79b or CARD11 mutations as well as models mimicking resistance to covalent BTK inhibitors. JNJ-67856633 exhibits potent tumor growth inhibition in two human DLBCL xenograft models, OCI-Ly3 and OCI-Ly10, and mutation selected patient derived DLBCL xenografts. Furthermore, treatment with JNJ-67856633 leads to dose dependent inhibition of the generation of Tregs (CD4+CD25+FoxP3+) following CD3/28 stimulation in vitro, suggesting a potential immune modulatory role of MALT1 inhibition. JNJ-64264681 is an orally active small molecule that is a potent, selective, and irreversible covalent BTK inhibitor. JNJ-64264681 inhibits the growth of CD79b-mutant DLBCL cell lines in vitro and potently inhibits tumor growth in xenograft- or patient-derived DLBCL models in vivo. Treatment with JNJ-64264681 and JNJ-67856633 administered together demonstrated statistically significant tumor growth inhibition compared with vehicle control in two CD79b mutant mouse lymphoma models, one based on a DLBCL cell line (OCI-Ly10) and one based on a patient-derived DLBCL model (LY2298). In both models, the combination showed increased growth inhibition compared with single agents and tumor regression in the combination arm. Synergistic anti-proliferative activity was observed in three DLBCL cell lines carrying CD79b mutations and one MCL cell line. Conclusions: Taken together, the in vitro and in vivo data for JNJ-67856633 and JNJ-64264681 suggest that combination therapy can increase the anti-tumor effect of the monotherapies and provide a more sustained response, offering strong support for clinical investigation of the combination of these two novel agents. A phase 1b combination study is scheduled to initiate. Citation Format: Ulrike Philippar, Lorena Fontan, Ivo Cornelissen, Haopeng Rui, Sriram Balasubramanian, Marcello Gaudiano, Mariette Bekkers, Luc Van Nuffel, Tianbao Lu, Tianbao Lu, John Wiener, Mark Tichenor, Tony Greway, Kathryn Packman, Bie Verbist, Yusri Elsayed, Ricardo Attar, Jacqueline Bussolari, John Gerecitano. Combination therapy of JNJ-67856633, a novel, first-in-class MALT1 protease inhibitor, and JNJ-64264681, a novel BTK inhibitor, for the treatment of B-cell lymphomas [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1267.

Published

2021

23. Discovery of 1-(1H-Pyrazolo[4,3-c]pyridin-6-yl)urea Inhibitors of Extracellular Signal-Regulated Kinase (ERK) for the Treatment of Cancers

Author

Marlene C. Hinton, Hua Zhou, Dongyu Sun, Ulrike Philippar, Peter Spacciapoli, Hongmin Chen, Shruti D. Raut, G. Naumov, Joey L. Methot, Alessia Petrocchi, Alan Hruza, My Sam Mansueto, Jongwon Lim, Joon Jung, Elizabeth Helen Kelley, Susan E. Hill, Phieng Siliphaivanh, and John Maclean

Subjects

Models, Molecular, 0301 basic medicine, MAPK/ERK pathway, Pyridines, Antineoplastic Agents, Crystallography, X-Ray, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Urea, Structure–activity relationship, Extracellular Signal-Regulated MAP Kinases, Protein Kinase Inhibitors, Cell Proliferation, Dose-Response Relationship, Drug, Molecular Structure, Drug discovery, Chemistry, Melanoma, Neoplasms, Experimental, medicine.disease, Dose–response relationship, 030104 developmental biology, Biochemistry, Cell culture, Cancer research, Molecular Medicine, Experimental pathology, Drug Screening Assays, Antitumor

Abstract

The ERK/MAPK pathway plays a central role in the regulation of critical cellular processes and is activated in more than 30% of human cancers. Specific BRAF and MEK inhibitors have shown clinical efficacy in patients for the treatment of BRAF-mutant melanoma. However, the majority of responses are transient, and resistance is often associated with pathway reactivation of the ERK signal pathway. Acquired resistance to these agents has led to greater interest in ERK, a downstream target of the MAPK pathway. De novo design efforts of a novel scaffold derived from SCH772984 by employing hydrogen bond interactions specific for ERK in the binding pocket identified 1-(1H-pyrazolo[4,3-c]pyridin-6-yl)ureas as a viable lead series. Sequential SAR studies led to the identification of highly potent and selective ERK inhibitors with low molecular weight and high LE. Compound 21 exhibited potent target engagement and strong tumor regression in the BRAF(V600E) xenograft model.

Published

2016

24. Abstract PO-49: Discovery of JNJ-67856633: A novel, first-in-class MALT1 protease inhibitor for the treatment of B-cell lymphomas

Author

Yann Abraham, Bart Petrus Anna Maria Jozef Medaer, Weimei Sun, Greet Vanhoof, Haopeng Rui, Yusri Elsayed, Sriram Balasubramanian, Ulrike Philippar, Marcello Gaudiano, Jan Willem Thuring, Jenna D. Goldberg, Tianbao Lu, Jennifer Smit, Peter J. Connolly, James P. Edwards, Max Cummings, Emanuele Trella, John Gerecitano, Nele Vloemans, Ricardo Attar, Tony Greway, Katarzyna Wnuk-Lipinska, Jan Linders, Kristof Kimpe, Amy J. Johnson, Jaqueline Bussolari, Bas-jan van der Leede, Luc Van Nuffel, Mariette Bekkers, and Katie Amssoms

Subjects

0301 basic medicine, biology, Chemistry, CD3, General Medicine, medicine.disease, BCL10, Lymphoma, 03 medical and health sciences, Interleukin 10, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, biology.protein, Cancer research, medicine, Bruton's tyrosine kinase, IL-2 receptor, Tyrosine kinase, B cell

Abstract

Introduction: Constitutive activation of the classical nuclear factor kappa-light-chain-enhancer of activated B cells (NF κB) pathway is a clear driver of B-cell lymphomas, especially the aggressive activated B-cell (ABC) subtype of diffuse large B-cell lymphoma (DLBCL). Mucosa-associated lymphoid tissue lymphoma translocation protein 1 (MALT1) is a key mediator of the classical NF-κB signaling pathway downstream of B-cell receptor and T-cell receptor. MALT1 possesses two functions: a scaffolding function to recruit NF-κB signaling proteins and a protease function to cleave and inactivate inhibitors of the NF-κB signaling pathway. Methods: Using a high-throughput screen followed by iterative structure-activity relationship (SAR) analyses, the MALT1 inhibitor JNJ-67856633 was identified. JNJ-67856633 was evaluated using biochemical, cellular in vitro, in vivo tumor efficacy and safety models. Results: JNJ-67856633 is a potent, selective, allosteric inhibitor of MALT1 protease activity as measured by biochemical assays or downstream cellular cytokine readouts (IL6/10) or direct MALT1 substrate cleavage (RelB, BCL10). The compound inhibits proliferation of activated B-cell diffuse large B-cell lymphoma (ABC-DLBCL) cell lines bearing CD79b or CARD11 mutations as well as models mimicking resistance to covalent Bruton's tyrosine kinase (BTK) inhibitors. Furthermore, combination effects were observed in CD79b cellular ABC-DLBCL models when JNJ-67856633 was combined with a BTK inhibitor. JNJ-67856633 showed activity in organoid cultures derived from ABC-DLBCL patients. JNJ-67856633 leads to potent in vivo pharmacodynamic shutdown in CD79b- as well as CARD11-mutant ABC-DLBCL models as measured by serum IL10 or uncleaved BCL10 levels in tumors. JNJ-67856633 exhibits potent tumor growth inhibition in two human DLBCL xenograft models, OCI Ly3 and OCI Ly10. In addition, >5 patient-derived DLBCL xenografts were evaluated and activity in mutation selected models was observed. To address the role of MALT1 inhibition in T cells, primary human T cells derived from normal healthy volunteers were treated with JNJ-67856633 in vitro. Dose-dependent inhibition of the generation of Tregs (CD4+CD25+FoxP3+) following CD3/28 stimulation was observed upon treatment with JNJ-67856633, suggesting a potential immune-modulatory role of MALT1 inhibition. Conclusions: Phase 1 clinical trials assessing the safety and efficacy of JNJ-67856633 initiated in 2019. JNJ-67856633 is a combination partner for BTK inhibitors and a promising treatment option for BTKi-resistant tumors, with demonstrated preclinical activity in CARD11 mutant tumors. In addition to ABC-DLBCL, a MALT1 inhibitor is a promising treatment option for patients with CLL, MCL, WM, and FL whose tumors have been shown to be sensitive to inhibition of BTK. MALT lymphomas, characterized by MALT1 and BCL10 translocation, represent another attractive target for MALT1 inhibition. Citation Format: Ulrike Philippar, Tianbao Lu, Lorena Fontan, Nele Vloemans, Mariette Bekkers, Luc van Nuffel, Marcello Gaudiano, Katarzyna Wnuk-Lipinska, Bas-Jan Van Der Leede, Katie Amssoms, Kristof Kimpe, Bart Medaer, Tony Greway, Yann Abraham, Max Cummings, Emanuele Trella, Greet Vanhoof, Weimei Sun, Jan Willem Thuring, Peter Connolly, Haopeng Rui, Sriram Balasubramanian, John Gerecitano, Ari Melnick, Ricardo Attar. Discovery of JNJ-67856633: A novel, first-in-class MALT1 protease inhibitor for the treatment of B-cell lymphomas [abstract]. In: Proceedings of the AACR Virtual Meeting: Advances in Malignant Lymphoma; 2020 Aug 17-19. Philadelphia (PA): AACR; Blood Cancer Discov 2020;1(3_Suppl):Abstract nr PO-49.

Published

2020

25. Abstract 5690: Discovery of JNJ-67856633: A novel, first-in-class MALT1 protease inhibitor for the treatment of B cell lymphomas

Author

Ulrike Philippar, Tianbao Lu, Nele Vloemans, Mariette Bekkers, Luc Van Nuffel, Marcello Gaudiano, Katarzyna Wnuk-Lipinska, Bas-jan Van Der Leede, Katie Amssoms, Kristof Kimpe, Bart Medaer, Tony Greway, Yann Abraham, Max Cummings, Emanuele Trella, Greet Vanhoof, Weimei Sun, Jan Willem Thuring, Peter Connolly, Jan Linders, Haopeng Rui, Sriram Balasubramanian, Amy Johnson, John Gerecitano, Jenna Goldberg, James P. Edwards, Yusri Elsayed, Jennifer Smit, Jaqueline Bussolari, and Ricardo Attar

Subjects

Cancer Research, Oncology

Abstract

Introduction: Constitutive activation of the classical nuclear factor kappa-light-chain-enhancer of activated B-cells (NF-κB) pathway is a clear driver of B-cell lymphomas, especially the aggressive activated B-cell (ABC) subtype of diffuse large B-cell lymphoma (DLBCL). Mucosa-associated lymphoid tissue lymphoma translocation protein 1 (MALT1) is a key mediator of the classical NF-κB signaling pathway downstream of B-cell receptor and T-cell receptor. MALT1 possesses 2 functions: a scaffolding function to recruit NF-κB signaling proteins and a protease function to cleave and inactivate inhibitors of the NF-κB signaling pathway. Methods: Using a high-throughput screen followed by iterative structure-activity relationship (SAR) analyses, the MALT1 inhibitor JNJ-67856633 was identified. The lead compound was evaluated using biochemical, in vitro cellular and in vivo tumor efficacy and safety models. Results: JNJ-67856633 is a potent, selective, allosteric inhibitor of MALT1 protease activity as measured by biochemical assays or downstream cellular cytokine readouts (IL 6/10) or direct MALT1 substrate cleavage (RelB, BCL10). The compound inhibits proliferation of activated B-cell diffuse large B-cell lymphoma (ABC-DLBCL) cell lines bearing CD79b or CARD11 mutations as well as models mimicking resistance to covalent Bruton's Tyrosine Kinase (BTK) inhibitors. Furthermore, combination effects were observed in CD79b cellular ABC-DLBCL models when JNJ-67856633 was combined with a BTK inhibitor. JNJ-67856633 leads to potent in vivo pharmacodynamic shutdown in CD79b- as well as CARD11-mutant ABC-DLBCL models as measured by serum IL10 or uncleaved BCL10 levels in tumors. JNJ-67856633 exhibits potent tumor growth inhibition in two human DLBCL xenograft models, OCI Ly3 and OCI Ly10, and mutation selection patient derived DLBCL xenografts. To address the role of MALT1 inhibition in T cells, primary human T cells derived from normal healthy volunteers were treated with JNJ-67856633 in vitro. Dose dependent inhibition of the generation of Tregs (CD4+CD25+FoxP3+) following CD3/28 stimulation was observed upon treatment with JNJ-67856633 suggesting a potential immune modulatory role of MALT1 inhibition. Conclusions: Phase 1 clinical trials assessing the safety and efficacy of JNJ-67856633 initiated in 2019. JNJ-67856633 is a combination partner for BTK inhibitors and a promising treatment option for BTKi-resistant tumors, with demonstrated preclinical activity in CARD11 mutant tumors. In addition to ABC-DLBCL, a MALT1 inhibitor is a promising treatment option for patients with CLL, MCL, WM, and FL whose tumors have been shown to be sensitive to inhibition of BTK. MALT lymphomas, characterized by MALT1 and BCL10 translocation, represent another attractive target for MALT1 inhibition. Citation Format: Ulrike Philippar, Tianbao Lu, Nele Vloemans, Mariette Bekkers, Luc Van Nuffel, Marcello Gaudiano, Katarzyna Wnuk-Lipinska, Bas-jan Van Der Leede, Katie Amssoms, Kristof Kimpe, Bart Medaer, Tony Greway, Yann Abraham, Max Cummings, Emanuele Trella, Greet Vanhoof, Weimei Sun, Jan Willem Thuring, Peter Connolly, Jan Linders, Haopeng Rui, Sriram Balasubramanian, Amy Johnson, John Gerecitano, Jenna Goldberg, James P. Edwards, Yusri Elsayed, Jennifer Smit, Jaqueline Bussolari, Jaqueline Bussolari, Ricardo Attar. Discovery of JNJ-67856633: A novel, first-in-class MALT1 protease inhibitor for the treatment of B cell lymphomas [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 5690.

Published

2020

26. Specific covalent inhibition of MALT1 paracaspase suppresses B cell lymphoma growth

Author

Matthew Durant, Natalia Bilchuk, Giuseppe Palladino, Qi Qiao, David A. Scott, Matt Teater, Lorena Fontan, Hao Wu, Ari Melnick, Nathanael S. Gray, Guangyan Du, Min Xia, Giorgio Inghirami, Spandan Chennamadhavuni, Ilkay Us, John M. Hatcher, Gabriella Casalena, and Ulrike Philippar

Subjects

0301 basic medicine, Male, B-cell receptor, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Drug Delivery Systems, Mice, Inbred NOD, Catalytic Domain, Cell Line, Tumor, medicine, Cytotoxic T cell, Animals, Humans, B-cell lymphoma, B cell, Chemistry, General Medicine, Paracaspase, medicine.disease, Caspase Inhibitors, Neoplasm Proteins, MALT1, 030104 developmental biology, medicine.anatomical_structure, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, 030220 oncology & carcinogenesis, Cancer research, Female, Lymphoma, Large B-Cell, Diffuse, Diffuse large B-cell lymphoma, Signal Transduction, Research Article

Abstract

The paracaspase MALT1 plays an essential role in activated B cell-like diffuse large B cell lymphoma (ABC DLBCL) downstream of B cell and TLR pathway genes mutated in these tumors. Although MALT1 is considered a compelling therapeutic target, the development of tractable and specific MALT1 protease inhibitors has thus far been elusive. Here, we developed a target engagement assay that provides a quantitative readout for specific MALT1-inhibitory effects in living cells. This enabled a structure-guided medicinal chemistry effort culminating in the discovery of pharmacologically tractable, irreversible substrate-mimetic compounds that bind the MALT1 active site. We confirmed that MALT1 targeting with compound 3 is effective at suppressing ABC DLBCL cells in vitro and in vivo. We show that a reduction in serum IL-10 levels exquisitely correlates with the drug pharmacokinetics and degree of MALT1 inhibition in vitro and in vivo and could constitute a useful pharmacodynamic biomarker to evaluate these compounds in clinical trials. Compound 3 revealed insights into the biology of MALT1 in ABC DLBCL, such as the role of MALT1 in driving JAK/STAT signaling and suppressing the type I IFN response and MHC class II expression, suggesting that MALT1 inhibition could prime lymphomas for immune recognition by cytotoxic immune cells.

Published

2017

27. Abstract 950: In vivo efficacy and pharmacodynamic modulation of JNJ-64619178, a selective PRMT5 inhibitor, in human lung and hematologic preclinical models

Author

Tinne Verhulst, Tongfei Wu, An Boeckx, Nahor Haddish-Berhane, Erika van Heerde, Joseph Portale, Dirk Brehmer, Tony Greway, Kathryn Packman, Hillary Millar, Dana Gaffney, Sylvie Laquerre, Thomas Nys, and Ulrike Philippar

Subjects

0301 basic medicine, Cancer Research, Methyltransferase, business.industry, Cell growth, Protein arginine methyltransferase 5, Phases of clinical research, Cancer, Myeloid leukemia, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, In vivo, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Medicine, business

Abstract

Protein arginine methyltransferase 5 (PRMT5), a type II methyltransferase, is responsible for symmetric arginine di-methylation of multiple cellular proteins involved in the regulation of cellular transcription. PRMT5 is involved in cellular processes such as survival, proliferation, and apoptosis, and an elevated tumor PRMT5 protein level has recently been correlated with poor survival of cancer patients. JNJ-64619178, a selective PRMT5 inhibitor, showed inhibition of cellular growth in several cell lines representing multiple cancer histologies in vitro. From this, a broad selection of xenograft models was chosen to demonstrate potent anti-tumor efficacy. Xenograft models representing small cell lung cancer (SCLC), non-small cell lung cancer (NSCLC), acute myeloid leukemia (AML), and non-Hodgkin lymphoma were chosen to demonstrate anti-tumor efficacy. Biologically significant tumor growth inhibition up to 99% was observed in both solid and hematological xenograft models, including an aggressive disseminated model of AML, with oral doses of 1 to 10 mg/kg, once daily. Importantly, continued inhibition of tumor growth was observed for several weeks following dosing cessation. Dosing of JNJ-64619178 results in inhibition of Sym-Arg di-methylation of SMD1/3 proteins, core components of the spliceosome in the tumor, and general Sym-Arg di-methylation of serum proteins. These serve as pharmacodynamic markers of PRMT5 inhibition in xenograft models. Potent and prolonged inhibition of SMD1/3 di-methylation was observed in the SCLC model, during and after the dosing period. This has led to the exploration of alternative dosing regimens preclinically. PRMT5 inhibitor JNJ-64619178 is currently being investigated in a Phase I clinical trial, based on its high selectivity and potency, favorable pharmacokinetics and safety properties, and strong preclinical efficacy and pharmacodynamic data. Citation Format: Hillary J. Millar, Dirk Brehmer, Tinne Verhulst, Nahor Haddish-Berhane, Tony Greway, Dana Gaffney, An Boeckx, Erika Van Heerde, Thomas Nys, Joseph Portale, Ulrike Philippar, Tongfei Wu, Sylvie Laquerre, Kathryn Packman. In vivo efficacy and pharmacodynamic modulation of JNJ-64619178, a selective PRMT5 inhibitor, in human lung and hematologic preclinical models [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 950.

Published

2019

28. DISCOVERY OF A NOVEL, POTENTIAL FIRST-IN-CLASS MALT1 PROTEASE INHIBITOR FOR THE TREATMENT OF B CELL LYMPHOMAS

Author

Ricardo Attar, Weimei Sun, Peter J. Connolly, Yann Abraham, Joannes T. M. Linders, Bart Petrus Anna Maria Jozef Medaer, Jenna D. Goldberg, L. van Nuffel, Kristof Kimpe, Marcello Gaudiano, Greet Vanhoof, Johannes Wilhelmus John F. Thuring, James P. Edwards, Nele Vloemans, Mariette Bekkers, Yusri Elsayed, John Gerecitano, Katie Amssoms, B.M. van der Leede, Tony Greway, E. Trella, Ulrike Philippar, K. Wnuk-Lipinska, Jennifer Smit, Maxwell D. Cummings, Tianbao Lu, and Jacqueline Bussolari

Subjects

Cancer Research, Class (set theory), medicine.anatomical_structure, Oncology, MALT1 protease, business.industry, medicine, Cancer research, Hematology, General Medicine, business, B cell

Published

2019

29. Discovery of a Novel ERK Inhibitor with Activity in Models of Acquired Resistance to BRAF and MEK Inhibitors

Author

Shuxia Zhao, Paul Kirschmeier, Ulrike Philippar, Li Xiao, Wang James J-S, Boga Sobhana Babu, Pierre Daublain, Phieng Siliphaivanh, Priya Dayananth, Clifford Restaino, Donna Carr, Lata Jayaraman, Xiaolei Gao, Marc Pelletier, Ling Zhang, Bart Lutterbach, Erick J. Morris, Stuart Black, Rumin Zhang, Weihong Jin, Ahmed A. Samatar, Joe Kelly, Daniel J. Hicklin, Alan B. Cooper, Leigh Zawel, Liang Zhu, Brian Long, Elaine M. Pinheiro, Hugh Y. Zhu, Sharda Jha, Stephen Fawell, Sunil Paliwal, D. Gary Gilliland, Jenny Liu, William T. Windsor, David J. Witter, Edward DiNunzio, Yongi Deng, W. Robert Bishop, Minilik Angagaw, Desai Jagdish A, Alan Hruza, and Gerald W. Shipps

Subjects

Proto-Oncogene Proteins B-raf, MAPK/ERK pathway, Neuroblastoma RAS viral oncogene homolog, Pharmacology, medicine.disease_cause, Cell Line, Tumor, Neoplasms, medicine, Humans, Extracellular Signal-Regulated MAP Kinases, Protein kinase A, Protein Kinase Inhibitors, neoplasms, Cell Proliferation, Kinase, Cell growth, Chemistry, Melanoma, MAP Kinase Kinase Kinases, medicine.disease, Oncology, Drug Resistance, Neoplasm, Mutation, KRAS, Signal transduction, Signal Transduction

Abstract

The high frequency of activating RAS or BRAF mutations in cancer provides strong rationale for targeting the mitogen-activated protein kinase (MAPK) pathway. Selective BRAF and MAP-ERK kinase (MEK) inhibitors have shown clinical efficacy in patients with melanoma. However, the majority of responses are transient, and resistance is often associated with pathway reactivation of the extracellular signal-regulated kinase (ERK) signaling pathway. Here, we describe the identification and characterization of SCH772984, a novel and selective inhibitor of ERK1/2 that displays behaviors of both type I and type II kinase inhibitors. SCH772984 has nanomolar cellular potency in tumor cells with mutations in BRAF, NRAS, or KRAS and induces tumor regressions in xenograft models at tolerated doses. Importantly, SCH772984 effectively inhibited MAPK signaling and cell proliferation in BRAF or MEK inhibitor–resistant models as well as in tumor cells resistant to concurrent treatment with BRAF and MEK inhibitors. These data support the clinical development of ERK inhibitors for tumors refractory to MAPK inhibitors. Significance: BRAF and MEK inhibitors have activity in MAPK-dependent cancers with BRAF or RAS mutations. However, resistance is associated with pathway alterations resulting in phospho-ERK reactivation. Here, we describe a novel ERK1/2 kinase inhibitor that has antitumor activity in MAPK inhibitor-naïve and MAPK inhibitor-resistant cells containing BRAF or RAS mutations. Cancer Discov; 3(7); 742–50. ©2013 AACR. See related commentary by Nissan et al., p. 719 This article is highlighted in the In This Issue feature, p. 705

Published

2013

30. DLK1-DIO3 Genomic Imprinted MicroRNA Cluster at 14q32.2 Defines a Stemlike Subtype of Hepatocellular Carcinoma Associated with Poor Survival

Author

Irena Ivanovska, Michele A. Cleary, Ulrike Philippar, Daniel G. Tenen, John M. Luk, Chuen-Neng Lee, Hongyue Dai, Angela M. Liu, Mao Mao, Sheung Tat Fan, Peter M. Shaw, Chunsheng Zhang, Felix H. Shek, Carolyn A. Buser, Julja Burchard, Nikki P. Lee, Ronnie T.P. Poon, and Kwong F. Wong

Subjects

Carcinoma, Hepatocellular, medicine.medical_treatment, Biology, Stem cell marker, Bioinformatics, Iodide Peroxidase, Biochemistry, Targeted therapy, Cohort Studies, microRNA, Biomarkers, Tumor, medicine, Humans, Tissue Distribution, CD90, Molecular Biology, Chromosomes, Human, Pair 14, Calcium-Binding Proteins, Liver Neoplasms, Membrane Proteins, Cancer, Molecular Bases of Disease, Cell Biology, Prognosis, medicine.disease, digestive system diseases, Up-Regulation, MicroRNAs, Treatment Outcome, Liver, Multigene Family, Hepatocellular carcinoma, Cancer research, Intercellular Signaling Peptides and Proteins, Genomic imprinting, Liver cancer

Abstract

Hepatocellular carcinoma (HCC) is a heterogeneous and highly aggressive malignancy, for which there are no effective cures. Identification of a malignant stemlike subtype of HCC may offer patients with a dismal prognosis a potential targeted therapy using c-MET and Wnt pathway inhibitors. MicroRNAs (miRNAs) show promise as diagnostic and prognostic tools for cancer detection and stratification. Using a TRE-c-Met-driven transgenic HCC mouse model, we identified a cluster of 23 miRNAs that is encoded within the Dlk1-Gtl2 imprinted region on chromosome 12qF1 overexpressed in all of the isolated liver tumors. Interestingly, this region is conserved among mammalian species and maps to the human DLK1-DIO3 region on chromosome 14q32.2. We thus examined the expression of the DLK1-DIO3 miRNA cluster in a cohort of 97 hepatitis B virus-associated HCC patients and identified a subgroup (n = 18) of patients showing strong coordinate overexpression of miRNAs in this cluster but not in other cancer types (breast, lung, kidney, stomach, and colon) that were tested. Expression levels of imprinted gene transcripts from neighboring loci in this 14q32.2 region and from a subset of other imprinted sites were concomitantly elevated in human HCC. Interestingly, overexpression of the DLK1-DIO3 miRNA cluster was positively correlated with HCC stem cell markers (CD133, CD90, EpCAM, Nestin) and associated with a high level of serum α-fetoprotein, a conventional biomarker for liver cancer, and poor survival rate in HCC patients. In conclusion, our findings suggest that coordinate up-regulation of the DLK1-DIO3 miRNA cluster at 14q32.2 may define a novel molecular (stem cell-like) subtype of HCC associated with poor prognosis.

Published

2011

31. Abstract 1383: A CRISPR-Cas9 tiling screen to identify functional domains within DNMT1 and/or DNMT3B that can be targeted for therapeutic intervention in AML

Author

Min Chul Kwon, Glenn S. Cowley, Ramona Crescenzo, Ricardo Attar, Balpreet Bhogal, Barbara A. Weir, David Pocalyko, and Ulrike Philippar

Subjects

Cancer Research, Oncology, embryonic structures, DNA methylation, DNMT3B, DNMT1, Mutagenesis (molecular biology technique), CRISPR, Methylation, Computational biology, Biology, Genomic imprinting, DNA methyltransferase

Abstract

DNA methylation is an epigenetic mechanism that regulates gene expression during many stages of development, including genomic imprinting, stem cell regulation, and X-chromosome inactivation. Moreover, aberrant DNA methylation patterns, characterized by genome-wide hypomethylation and promoter-specific hypermethylation, are a prominent feature of cancer. Methylation of DNA at the 5-position of cytosines is mediated by the DNA methyltransferase (DNMT) protein family, which regulates both maintenance methylation (DNMT1) and de novo methylation (DNMT3A and DNMT3B). Loss-of-function mutations of DNMT3A have been identified in hematological malignancies including acute myeloid leukemia (AML), where DNMT3A is mutated in approximately 25% of known cases. Published reports suggest the existence of a synthetic lethal interaction between DNMT3A and DNMT1/3B. To further study this potential genetic interaction, we are performing a CRISPR-Cas9 tiling screen to identify functional domains within DNMT1 and/or DNMT3B that are synthetic lethal with DNMT3A. We generated a lentiviral library containing 777 and 421 single guide RNAs (sgRNAs) that tile the coding region of DNMT1 and DNMT3B, respectively and performed viability screens in AML cell lines that are either wild-type or mutant for DNMT3A. This screen was designed to identify in-frame alterations within functional domains that lead to effects on cell viability. Next generation sequencing of sgRNAs identified three functional domains of DNMT1 which, when mutated, leads to decreases in cell viability. Current efforts are focused on verifying the essentiality of these functional domains using CRISPR-Cas9-based approaches as well as mutagenesis by integrated tiles (MITE)-seq analyses. Citation Format: Balpreet Bhogal, Barbara Weir, Ramona Crescenzo, Min Chul Kwon, Ulrike Philippar, Ricardo Attar, Glenn Cowley, David Pocalyko. A CRISPR-Cas9 tiling screen to identify functional domains within DNMT1 and/or DNMT3B that can be targeted for therapeutic intervention in AML [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 1383.

Published

2018

32. A Mena Invasion Isoform Potentiates EGF-Induced Carcinoma Cell Invasion and Metastasis

Author

Yarong Wang, John S. Condeelis, Douglas A. Lauffenburger, Evanthia T. Roussos, Erik Sahai, Matthew G. Oser, Jeffrey B. Wyckoff, Ulrike Philippar, Silvia Giampieri, Hyung-Do Kim, Hideki Yamaguchi, Frank B. Gertler, and Sumanta Goswami

Subjects

Lung Neoplasms, HUMDISEASE, Motility, macromolecular substances, Biology, Models, Biological, Article, General Biochemistry, Genetics and Molecular Biology, Metastasis, Mice, Downregulation and upregulation, Cell Movement, Epidermal growth factor, medicine, Animals, Humans, Protein Isoforms, Neoplasm Invasiveness, Neoplasm Metastasis, Molecular Biology, Actin, Epidermal Growth Factor, Macrophages, Carcinoma, Microfilament Proteins, Vasodilator-stimulated phosphoprotein, Cancer, Cell Biology, biochemical phenomena, metabolism, and nutrition, medicine.disease, Gene Expression Regulation, Neoplastic, Alternative Splicing, Lymphatic system, SIGNALING, Cancer research, CELLBIO, Neoplasm Transplantation, Developmental Biology

Abstract

The spread of cancer during metastatic disease requires that tumor cells subvert normal regulatory networks governing cell motility to invade surrounding tissues and migrate toward blood and lymphatic vessels. Enabled (Ena)/vasodilator-stimulated phosphoprotein (VASP) proteins regulate cell motility by controlling the geometry of assembling actin networks. Mena, an Ena/VASP protein, is upregulated in the invasive subpopulation of breast cancer cells. In addition, Mena is alternately spliced to produce an invasion isoform, Mena(INV). Here we show that Mena and Mena(INV) promote carcinoma cell motility and invasiveness in vivo and in vitro, and increase lung metastasis. Mena and Mena(INV) potentiate epidermal growth factor (EGF)-induced membrane protrusion and increase the matrix degradation activity of tumor cells. Interestingly, Mena(INV) is significantly more effective than Mena in driving metastases and sensitizing cells to EGF-dependent invasion and protrusion. Upregulation of Mena(INV) could therefore enable tumor cells to invade in response to otherwise benign EGF stimulus levels.

Published

2008

33. Identification of invasion specific splice variants of the cytoskeletal protein Mena present in mammary tumor cells during invasion in vivo

Author

Ulrike Philippar, Jacob Avraham, John S. Condeelis, Weigang Wang, Frank B. Gertler, Daqian Sun, Sumanta Goswami, Antonia Patsialou, Francesca Di Modugno, and Paola Nisticò

Subjects

Gene isoform, Cancer Research, Transplantation, Heterologous, Breast Neoplasms, Mice, SCID, macromolecular substances, Adenocarcinoma, Biology, Article, Metastasis, Mice, Gentamicin protection assay, In vivo, Gene expression, medicine, Animals, Humans, Protein Isoforms, Neoplasm Invasiveness, Neoplasm Metastasis, Mammary tumor, Chemotaxis, Microfilament Proteins, Mammary Neoplasms, Experimental, General Medicine, medicine.disease, Rats, Oncology, Cancer cell, Cancer research, Neoplasm Transplantation

Abstract

We have studied the gene expression pattern of invasive primary mammary tumor cells using a unique in vivo invasion assay that isolates the invasive tumor cells by chemotaxis. One of the genes upregulated in the invasive tumor cells is Mena, an actin binding protein involved in the regulation of cell motility. There are multiple known splice variants of Mena accounted for by four alternatively included exons, +, ++, +++ and 11a. Using the in vivo invasion assay in rats and mice with mammary tumors we observed that two isoforms of Mena, ++ and +++, are upregulated in the invasive tumor cells and one isoform, 11a, is downregulated. The Mena isoform switching pattern described here may provide a new biomarker for the presence of metastatic cancer cells and for prognosis.

Published

2008

34. Human Mena+11a Isoform Serves as a Marker of Epithelial Phenotype and Sensitivity to Epidermal Growth Factor Receptor Inhibition in Human Pancreatic Cancer Cell Lines

Author

Marcella Mottolese, Elisa Melucci, Francesca Di Modugno, Massimo Alessio, Frank B. Gertler, Michele Milella, Pier Giorgio Natali, David J. McConkey, Ulrike Philippar, Maria Simona Pino, Michele Balsamo, and Paola Nisticò

Subjects

Cancer Research, Pathology, medicine.medical_specialty, biology, Cell growth, Oncology, Growth factor receptor, Epidermal growth factor, Cancer research, biology.protein, medicine, Epidermal growth factor receptor, Erlotinib, Erlotinib Hydrochloride, Protein kinase B, medicine.drug, EGFR inhibitors

Abstract

Purpose: hMena, member of the enabled/vasodilator-stimulated phosphoprotein family, is a cytoskeletal protein that is involved in the regulation of cell motility and adhesion. The aim of this study was to determine whether or not the expression of hMena isoforms correlated with sensitivity to EGFR tyrosine kinase inhibitors and could serve as markers with potential clinical use. Experimental Design: Human pancreatic ductal adenocarcinoma cell lines were characterized for in vitro sensitivity to erlotinib, expression of HER family receptors, markers of epithelial to mesenchymal transition, and expression of hMena and its isoform hMena+11a. The effects of epidermal growth factor (EGF) and erlotinib on hMena expression as well as the effect of hMena knockdown on cell proliferation were also evaluated. Results: hMena was detected in all of the pancreatic tumor cell lines tested as well as in the majority of the human tumor samples [primary (92%) and metastatic (86%)]. Intriguingly, in vitro hMena+11a isoform was specifically associated with an epithelial phenotype, EGFR dependency, and sensitivity to erlotinib. In epithelial BxPC3 cells, epidermal growth factor up-regulated hMena/hMena+11a and erlotinib down-regulated expression. hMena knockdown reduced cell proliferation and mitogen-activated protein kinase and AKT activation in BxPC3 cells, and promoted the growth inhibitory effects of erlotinib. Conclusions: Collectively, our data indicate that the hMena+11a isoform is associated with an epithelial phenotype and identifies EGFR-dependent cell lines that are sensitive to the EGFR inhibitor erlotinib. The availability of anti-hMena+11a–specific probes may offer a new tool in pancreatic cancer management if these results can be verified prospectively in cancer patients.

Published

2008

35. Filopodia are required for cortical neurite initiation

Author

Erik W. Dent, Arthur S. Alberts, Craig Furman, Stephanie L. Gupton, Jiangyang Zhang, Susumu Mori, Leslie M. Mebane, Melanie Barzik, Douglas A. Rubinson, Adam V. Kwiatkowski, Frank B. Gertler, Ulrike Philippar, and J. Edward van Veen

Subjects

Nervous system, Neurite, macromolecular substances, Myosins, Microtubules, Mice, Laminin, Microtubule, Neurites, medicine, Animals, Pseudopodia, Cells, Cultured, Actin, Cerebral Cortex, Mice, Knockout, Myosin Type II, Neurons, biology, Microfilament Proteins, NADPH Dehydrogenase, Cell Biology, Phosphoproteins, Actins, Cell biology, Dendritic filopodia, DNA-Binding Proteins, medicine.anatomical_structure, nervous system, Mutation, biology.protein, Ectopic expression, Cell Adhesion Molecules, Microtubule-Associated Proteins, Filopodia

Abstract

Extension of neurites from a cell body is essential to form a functional nervous system; however, the mechanisms underlying neuritogenesis are poorly understood. Ena/VASP proteins regulate actin dynamics and modulate elaboration of cellular protrusions. We recently reported that cortical axon-tract formation is lost in Ena/VASP-null mice and Ena/VASP-null cortical neurons lack filopodia and fail to elaborate neurites. Here, we report that neuritogenesis in Ena/VASP-null neurons can be rescued by restoring filopodia formation through ectopic expression of the actin nucleating protein mDia2. Conversely, wild-type neurons in which filopodia formation is blocked fail to elaborate neurites. We also report that laminin, which promotes the formation of filopodia-like actin-rich protrusions, rescues neuritogenesis in Ena/VASP-deficient neurons. Therefore, filopodia formation is a key prerequisite for neuritogenesis in cortical neurons. Neurite initiation also requires microtubule extension into filopodia, suggesting that interactions between actin-filament bundles and dynamic microtubules within filopodia are crucial for neuritogenesis.

Published

2007

36. PTP1B-dependent regulation of receptor tyrosine kinase signaling by the actin-binding protein Mena

Author

Laila Ritsma, Jeff Wyckoff, Douglas A. Lauffenburger, Jason R. Neil, Frank B. Gertler, Eliza Vasile, Jacco van Rheenen, John S. Condeelis, Madeleine J. Oudin, Robert J. Eddy, Shannon K. Hughes, Ulrike Philippar, Jenny Tadros, Alisha Lussiez, Brian A. Joughin, Forest M. White, Amanda M. Del Rosario, Massachusetts Institute of Technology. Department of Biological Engineering, Massachusetts Institute of Technology. Department of Biology, Koch Institute for Integrative Cancer Research at MIT, Hughes, Shannon Kay, Oudin, Madeleine Julie, Tadros, Jenny, Neil, Jason Robert, Del Rosario, Amanda M., Joughin, Brian A., Vasile, Eliza, Philippar, Ulrike, Lussiez, Alisha, White, Forest M., Lauffenburger, Douglas A., Gertler, Frank, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

medicine.medical_treatment, Motility, Breast Neoplasms, Protein tyrosine phosphatase, macromolecular substances, Biology, Receptor tyrosine kinase, Cell Movement, Epidermal growth factor, Cell Adhesion, medicine, Humans, Protein Isoforms, Neoplasm Metastasis, Phosphorylation, Receptor, Molecular Biology, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Epidermal Growth Factor, Growth factor, Microfilament Proteins, Receptor Protein-Tyrosine Kinases, Articles, Cell Biology, Signaling, Actins, 3. Good health, Cell biology, ErbB Receptors, Cytoskeletal Proteins, biology.protein, Cancer research, Female, Signal transduction, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

During breast cancer progression, alternative mRNA splicing produces functionally distinct isoforms of Mena, an actin regulator with roles in cell migration and metastasis. Aggressive tumor cell subpopulations express Mena[superscript INV], which promotes tumor cell invasion by potentiating EGF responses. However, the mechanism by which this occurs is unknown. Here we report that Mena associates constitutively with the tyrosine phosphatase PTP1B and mediates a novel negative feedback mechanism that attenuates receptor tyrosine kinase signaling. On EGF stimulation, complexes containing Mena and PTP1B are recruited to the EGFR, causing receptor dephosphorylation and leading to decreased motility responses. Mena also interacts with the 5′ inositol phosphatase SHIP2, which is important for the recruitment of the Mena-PTP1B complex to the EGFR. When Mena[superscript INV] is expressed, PTP1B recruitment to the EGFR is impaired, providing a mechanism for growth factor sensitization to EGF, as well as HGF and IGF, and increased resistance to EGFR and Met inhibitors in signaling and motility assays. In sum, we demonstrate that Mena plays an important role in regulating growth factor–induced signaling. Disruption of this attenuation by Mena[superscript INV] sensitizes tumor cells to low–growth factor concentrations, thereby increasing the migration and invasion responses that contribute to aggressive, malignant cell phenotypes., Breast Cancer Research Program (U.S.) (Grant W81XWH-10-1-0040), Breast Cancer Research Program (U.S.) (Grant W81XWH-13-1-0031), National Institutes of Health (U.S.) (Grant U54-CA112967), National Institutes of Health (U.S.) (Grant GM58801), Virginia and D.K. Ludwig Fund for Cancer Research

Published

2015

37. The SRF Target Gene Fhl2 Antagonizes RhoA/MAL-Dependent Activation of SRF

Author

Alfred Nordheim, Judith M. Müller, Petra Galgoczy, Roland Schüle, Frank B. Gertler, Felix B. Engel, Ulrike Philippar, Martin Vingron, Christoph Dieterich, Gerhard Schratt, and Mark T. Keating

Subjects

Serum Response Factor, RHOA, genetic structures, Proteolipids, Recombinant Fusion Proteins, LIM-Homeodomain Proteins, Muscle Proteins, Mice, In vivo, Coactivator, Serum response factor, Animals, Gene, Molecular Biology, Homeodomain Proteins, biology, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Myelin and Lymphocyte-Associated Proteolipid Proteins, Stem Cells, Membrane Transport Proteins, Herpes Simplex Virus Protein Vmw65, Promoter, Cell Biology, musculoskeletal system, Precipitin Tests, Molecular biology, Chromatin, eye diseases, FHL2, Gene expression profiling, embryonic structures, NIH 3T3 Cells, cardiovascular system, biology.protein, rhoA GTP-Binding Protein, Myelin Proteins, Transcription Factors

Abstract

RhoA signaling regulates the activity of the transcription factor SRF (serum response factor) during muscle differentiation. How RhoA signaling is integrated at SRF target promoters to achieve muscle-lineage-specific expression is largely unknown. Using large-scale expression profiling combined with bioinformatic and biochemical approaches, we identified several SRF target genes, including Fhl2, encoding a transcriptional cofactor that is highly expressed in the heart. SRF binds the Fhl2 promoter in vivo and regulates Fhl2 expression in response to RhoA activation. FHL2 protein and SRF interact physically, and FHL2 binds the promoters of SRF-responsive smooth muscle (SM) genes, but not the promoters of immediate-early genes (IEGs), in response to RhoA. FHL2 antagonizes induction of SM genes, but not IEGs or cardiac genes, by competing with the coactivator MAL/MRTF-A for SRF binding. Our findings identify an autoregulatory mechanism to selectively regulate subsets of RhoA-activated SRF target genes.

Published

2004

38. Serum response factor is crucial for actin cytoskeletal organization and focal adhesion assembly in embryonic stem cells

Author

Alfred Nordheim, Ulrike Philippar, Jürgen Berger, Gerhard Schratt, Olaf Heidenreich, and Heinz Schwarz

Subjects

Talin, Serum Response Factor, Stress fiber, Recombinant Fusion Proteins, Focal adhesion assembly, macromolecular substances, Article, Focal adhesion, Mice, Cell Movement, Serum response factor, Metalloproteins, Cell Adhesion, Animals, Cell adhesion, Cytoskeleton, Mice, Knockout, Focal Adhesions, biology, SRF, ES cells, actin cytoskeleton, focal adhesion, cell migration, Integrin beta1, Stem Cells, Herpes Simplex Virus Protein Vmw65, Cell Biology, Vinculin, Protein-Tyrosine Kinases, Actins, Zyxin, Cell biology, Enzyme Activation, Gene Expression Regulation, Focal Adhesion Kinase 1, Focal Adhesion Protein-Tyrosine Kinases, embryonic structures, biology.protein, sense organs, Lamellipodium, rhoA GTP-Binding Protein

Abstract

The activity of serum response factor (SRF), an essential transcription factor in mouse gastrulation, is regulated by changes in actin dynamics. Using Srf(−/−) embryonic stem (ES) cells, we demonstrate that SRF deficiency causes impairments in ES cell spreading, adhesion, and migration. These defects correlate with defective formation of cytoskeletal structures, namely actin stress fibers and focal adhesion (FA) plaques. The FA proteins FA kinase (FAK), β1-integrin, talin, zyxin, and vinculin were downregulated and/or mislocalized in ES cells lacking SRF, leading to inefficient activation of the FA signaling kinase FAK. Reduced overall actin expression levels in Srf(−/−) ES cells were accompanied by an offset treadmilling equilibrium, resulting in lowered F-actin levels. Expression of active RhoA-V14 rescued F-actin synthesis but not stress fiber formation. Introduction of constitutively active SRF-VP16 into Srf(−/−) ES cells, on the other hand, strongly induced expression of FA components and F-actin synthesis, leading to a dramatic reorganization of actin filaments into stress fibers and lamellipodia. Thus, using ES cell genetics, we demonstrate for the first time the importance of SRF for the formation of actin-directed cytoskeletal structures that determine cell spreading, adhesion, and migration. Our findings suggest an involvement of SRF in cell migratory processes in multicellular organisms.

Published

2002

39. Abstract LB-303: Substrate-mimetic covalent inhibitor of MALT1 is most effective against CARD11 mutant ABC-DLBCL

Author

Nathaniel Gray, Qi Qiao, Ulrike Philippar, Mariette Bekkers, Gabriella Casalena, David L. Scott, Hao Wu, Lorena Fontan, Matthew Durant, Ilkay Us, John M. Hatcher, Ari Melnick, and Spandan Chennamadhavuni

Subjects

Cancer Research, Mutation, biology, Chemistry, Kinase, breakpoint cluster region, Syk, Germinal center, medicine.disease_cause, medicine.disease, Oncology, immune system diseases, hemic and lymphatic diseases, Cancer research, medicine, biology.protein, Bruton's tyrosine kinase, Primary mediastinal B-cell lymphoma, PI3K/AKT/mTOR pathway

Abstract

Diffuse Large B-cell lymphoma is the most common subtype of B-cell non Hodgkin Lymphoma (B-NHL) representing 30% of all B-NHL. There are three molecular subtypes: germinal center B cell-like (GCB) DLBCL, activated B cell-like (ABC) DLBCL, and primary mediastinal B cell lymphoma (PMBL). Of those, Activated B-cell like Diffuse Large B-cell Lymphoma (ABC-DLBCL) represents a third of the patients and is characterized by constitutive NF-κB activity due to mutations in various proteins of the B-cell receptor (BCR) as well as Toll-like receptor (TLR) pathways. Mutations in the BCR pathway include: activating mutations of CD79A/B (20% of ABC-DLBCLs) and CARD11 (10%) and deletion or inactivating mutation of A20 (20-30%). In the TLR pathway, MYD88 is mutated in 37% of ABC-DLBCL patients. Given this scenario, numerous therapeutic strategies targeting proteins signaling downstream of the BCR pathway have been proposed for ABC-DLBCL -including inhibitors targeting kinases SYK, BTK, PI3K, PKC, MAPKs and AKT or the protease MALT1. MALT1 inhibition provides advantages to other targets because it is downstream of most of the BCR pathway mutations present in patients, including CARD11. Patients with CARD11 mutations do not respond to BTK inhibitors. However, none of the MALT1 inhibitors reported to date are good candidates for clinical use. Here we report a new class of substrate mimetic MALT1 inhibitors based on Z-VRPR-fmk. Our lead compound, SCM-02-138 displayed nanomolar potency in biochemical and cellular MALT1 protease reporter assays. Crystallography shows covalent binding of the compound to MALT1 active site Cys residue. SCM-02-138 was highly selective for MALT1 and showed over 100-fold differential killing in sensitive vs resistant cell lines. MALT1 inhibition was most effective in CARD11 mutant cells. SCM-02-138 was active in vivo, as assessed by hIL10 inhibition in xenografted models of ABC-DLBCL cell lines. Moreover it was effective against ABC-DLBCL xenografts and PDX DLBCL ex vivo. Combination of SCM-02-138 with other BCR inhibitors revealed PI3K delta inhibition as the most synergistic combination. Combination of SCM-02-138 and CAL-101 potentiated both proliferation inhibition and apoptosis. In summary, we have developed a new class of MALT1 peptidic inhibitor characterized by nanomolar potency, irreversibility and high specificity. This inhibitor will be particularly useful against CARD11 mutant ABC-DLBCL, which are resistant to BTK inhibitors. Citation Format: Lorena Fontan, David Scott, John Hatcher, Qi Qiao, Ilkay Us, Gabriella Casalena, Mariette Bekkers, Ulrike Philippar, Matthew Durant, Spandan Chennamadhavuni, Hao Wu, Nathaniel Gray, Ari Melnick. Substrate-mimetic covalent inhibitor of MALT1 is most effective against CARD11 mutant ABC-DLBCL [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr LB-303. doi:10.1158/1538-7445.AM2017-LB-303

Published

2017

40. Gene Signatures Derived from a c-MET-Driven Liver Cancer Mouse Model Predict Survival of Patients with Hepatocellular Carcinoma

Author

Dimple Bansal, Michele A. Cleary, Mao Mao, Kwong F. Wong, Chunsheng Zhang, Irena Ivanovska, Hongyue Dai, Ronnie T.P. Poon, Angela M. Liu, Ulrike Philippar, Carolyn A. Buser, Nikki P. Lee, Sheung Tat Fan, Martin L. Scott, John M. Luk, and Patrick Lewis

Subjects

Genetically modified mouse, Male, C-Met, Carcinoma, Hepatocellular, lcsh:Medicine, Mice, Transgenic, Gastroenterology and Hepatology, Biology, Bioinformatics, Transcriptome, Molecular Genetics, chemistry.chemical_compound, Mice, Gastrointestinal Cancers, medicine, Genetics, Cancer Genetics, Animals, Humans, Carcinoma, Hepatocellular - diagnosis - genetics - metabolism - pathology, lcsh:Science, Regulation of gene expression, Multidisciplinary, Proto-Oncogene Proteins c-met - genetics, lcsh:R, Liver Neoplasms, Wnt signaling pathway, Proto-Oncogene Proteins c-met, medicine.disease, Prognosis, Survival Analysis, Liver Neoplasms - diagnosis - genetics - metabolism - pathology, Gene expression profiling, Disease Models, Animal, chemistry, Liver, Liver - cytology - metabolism - pathology, Cancer research, Biomarker (medicine), Medicine, lcsh:Q, Female, Liver cancer, Research Article

Abstract

Biomarkers derived from gene expression profiling data may have a high false-positive rate and must be rigorously validated using independent clinical data sets, which are not always available. Although animal model systems could provide alternative data sets to formulate hypotheses and limit the number of signatures to be tested in clinical samples, the predictive power of such an approach is not yet proven. The present study aims to analyze the molecular signatures of liver cancer in a c-MET-transgenic mouse model and investigate its prognostic relevance to human hepatocellular carcinoma (HCC). Tissue samples were obtained from tumor (TU), adjacent non-tumor (AN) and distant normal (DN) liver in Tet-operator regulated (TRE) human c-MET transgenic mice (n = 21) as well as from a Chinese cohort of 272 HBV- and 9 HCV-associated HCC patients. Whole genome microarray expression profiling was conducted in Affymetrix gene expression chips, and prognostic significances of gene expression signatures were evaluated across the two species. Our data revealed parallels between mouse and human liver tumors, including down-regulation of metabolic pathways and up-regulation of cell cycle processes. The mouse tumors were most similar to a subset of patient samples characterized by activation of the Wnt pathway, but distinctive in the p53 pathway signals. Of potential clinical utility, we identified a set of genes that were down regulated in both mouse tumors and human HCC having significant predictive power on overall and disease-free survival, which were highly enriched for metabolic functions. In conclusions, this study provides evidence that a disease model can serve as a possible platform for generating hypotheses to be tested in human tissues and highlights an efficient method for generating biomarker signatures before extensive clinical trials have been initiated. © 2011 Ivanovska et al., published_or_final_version

Published

2011

41. Predictive genes in adjacent normal tissue are preferentially altered by sCNV during tumorigenesis in liver cancer and may rate limiting

Author

Hunter B. Fraser, Chunsheng Zhang, James Watters, Cliona Molony, Christine Suver, Zhan Zhang, John Lamb, Hongyue Dai, Danielle M. Greenawalt, C Yeung, Mao Mao, Ke Hao, Stephen H. Friend, Eugene Chudin, Bin Zhang, John M. Luk, Peter M. Shaw, Tao Xie, Michele A. Cleary, Sheung T. Fan, Ulrike Philippar, Carolyn A. Buser-Doepner, Jonathan M. J. Derry, Kai Wang, Julja Burchard, Ronnie T.P. Poon, Ryan Smith, Eric E. Schadt, Nikki P. Lee, Jun Zhu, Andrey Loboda, Mark D. Ferguson, Dimple Bansal, Martin L. Scott, Joshua Millstein, Justin Guinney, Valur Emilsson, and Irena Ivanovska

Subjects

Male, Somatic cell, Gene regulatory network, Genetic Networks, medicine.disease_cause, Mice, Gene expression, Basic Cancer Research, Liver - metabolism - pathology, Gene Regulatory Networks, Copy-number variation, Genome Evolution, Oligonucleotide Array Sequence Analysis, Genetics, Multidisciplinary, Systems Biology, Liver Neoplasms, Genomics, Middle Aged, Proto-Oncogene Proteins c-met, Genome Scans, Liver, Oncology, Chromosomes, Human, Pair 1, Regression Analysis, Medicine, Female, Research Article, Adult, Carcinoma, Hepatocellular, DNA Copy Number Variations, Gene prediction, Science, Mice, Transgenic, Gastroenterology and Hepatology, Biology, Genome Analysis Tools, Cell Line, Tumor, Gastrointestinal Tumors, medicine, Cancer Genetics, Animals, Humans, Gene Networks, Trait Locus Analysis, Gene, Aged, Models, Genetic, Gene Expression Profiling, Liver Neoplasms - genetics, Computational Biology, Cancers and Neoplasms, Hepatocellular Carcinoma, Carcinoma, Hepatocellular - genetics, Gene expression profiling, Genetics of Disease, Cancer research, Carcinogenesis, Genome Expression Analysis

Abstract

Background: In hepatocellular carcinoma (HCC) genes predictive of survival have been found in both adjacent normal (AN) and tumor (TU) tissues. The relationships between these two sets of predictive genes and the general process of tumorigenesis and disease progression remains unclear. Methodology/Principal Findings: Here we have investigated HCC tumorigenesis by comparing gene expression, DNA copy number variation and survival using ~250 AN and TU samples representing, respectively, the pre-cancer state, and the result of tumorigenesis. Genes that participate in tumorigenesis were defined using a gene-gene correlation meta-analysis procedure that compared AN versus TU tissues. Genes predictive of survival in AN (AN-survival genes) were found to be enriched in the differential gene-gene correlation gene set indicating that they directly participate in the process of tumorigenesis. Additionally the AN-survival genes were mostly not predictive after tumorigenesis in TU tissue and this transition was associated with and could largely be explained by the effect of somatic DNA copy number variation (sCNV) in cis and in trans. The data was consistent with the variance of AN-survival genes being rate-limiting steps in tumorigenesis and this was confirmed using a treatment that promotes HCC tumorigenesis that selectively altered AN-survival genes and genes differentially correlated between AN and TU. Conclusions/Significance: This suggests that the process of tumor evolution involves rate-limiting steps related to the background from which the tumor evolved where these were frequently predictive of clinical outcome. Additionally treatments that alter the likelihood of tumorigenesis occurring may act by altering AN-survival genes, suggesting that the process can be manipulated. Further sCNV explains a substantial fraction of tumor specific expression and may therefore be a causal driver of tumor evolution in HCC and perhaps many solid tumor types. © 2011 Lamb et al., published_or_final_version

Published

2011

42. Degeneration of the mouse retina upon dysregulated activity of serum response factor

Author

Jenny, Sandström, Peter, Heiduschka, Susanne C, Beck, Ulrike, Philippar, Matthias W, Seeliger, Ulrich, Schraermeyer, and Alfred, Nordheim

Subjects

Serum Response Factor, genetic structures, Recombinant Fusion Proteins, Retinal Degeneration, Gene Dosage, Gene Expression, Gene Expression Regulation, Developmental, Herpes Simplex Virus Protein Vmw65, Transfection, eye diseases, Mice, Mutant Strains, Retina, Disease Models, Animal, Mice, embryonic structures, cardiovascular system, Electroretinography, Animals, Eosine Yellowish-(YS), sense organs, Transgenes, Hematoxylin, Embryonic Stem Cells, Research Article

Abstract

Purpose Our aim was to generate and phenotypically characterize a transgenic mouse line expressing a constitutively active variant of the transcription regulatory protein serum response factor (SRF), namely the SRF-VP16 protein. This new mouse strain has been registered under the designation Gt(ROSA)26Sortm1(SRF-VP16)Antu. We found phenotypic changes upon ectopic expression of SRF-VP16, especially in the mouse retina. Methods Using homologous recombination, we integrated an SRF-VP16 conditional (i.e., “flox-STOP” repressed) expression transgene into the Rosa26 locus of murine embryonic stem (ES) cells. These engineered ES cells were used to derive the Gt(ROSA)26Sortm1(SRF-VP16)Antu mouse strain. Semiquantitative real-time PCR was used to determine expression of the SRF-VP16 transgene at the mRNA level, both in young (P20 and P30) and adult (six months old) Gt(ROSA)26Sortm1(SRF-VP16)Antu mice. We also investigated the transcript levels of endogenous Srf and several SRF target genes. Retinal function was tested by electroretinography in both young and adult mice. Morphological abnormalities could be visualized by hematoxylin and eosin staining of sectioned, paraffin-embedded eye tissue samples. Scanning-laser ophthalmoscopy was used to investigate retinal vascularization and degeneration in adult mice. Results We show that the SRF-VP16 mRNA is expressed to a low but significant degree in the retinas of young and adult animals of the Gt(ROSA)26Sortm1(SRF-VP16)Antu mouse strain, even in the absence of Cre-mediated deletion of the “flox-STOP” cassette. In the retinas of these transgenic mice, endogenous Srf displays elevated transcript levels. Ectopic retinal expression of constitutively active SRF-VP16 is correlated with the malfunction of retinal neurons in both heterozygous and homozygous animals of both age groups (P20 and adult). Additionally, mislamination of retinal cell layers and cellular rosette formations are found in retinas of both heterozygous and homozygous animals of young age. In homozygous individuals, however, the cellular rosettes are more widespread over the fundus. At adult age, retinas both from animals that are heterozygous and homozygous for the floxSTOP/SRF-VP16 transgene display severe degeneration, mainly of the photoreceptor cell layer. Wild-type age-matched littermates, however, do not show any degeneration. The severity of the observed effects correlates with dosage of the transgene. Conclusions This is the first report suggesting an influence of the transcription factor SRF on the development and function of the murine retina. Ectopic SRF-VP16 mRNA expression in the retinas of young animals is correlated with photoreceptor layer mislamination and impaired retinal function. At an advanced age of six months, degenerative processes are detected in SRF-VP16 transgenic retinas accompanied by impaired retinal function. The Gt(ROSA)26Sortm1(SRF-VP16)Antu mouse strain represents a genetic SRF gain-of-function mouse model that will complement the current SRF loss-of-function models. It promises to provide new insight into the hitherto poorly defined role of SRF in retinal development and function, including potential contributions to ophthalmologic disorders. Furthermore, using conditional Cre-mediated activation of SRF-VP16, the described mouse strain will enable assessment of the impact of dysregulated SRF activity on the physiologic functions of various other organs.

Published

2010

43. Simultaneous imaging of GFP, CFP and collagen in tumors in vivo using multiphoton microscopy

Author

Jeffrey Wyckoff, Jeffrey E. Segall, Ulrike Philippar, Erik Sahai, John S. Condeelis, Frank B. Gertler, Massachusetts Institute of Technology. Department of Biology, Philippar, Ulrike, and Gertler, Frank

Subjects

Cell type, lcsh:Biotechnology, Green Fluorescent Proteins, Cell, Biology, Green fluorescent protein, Cell membrane, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Genes, Reporter, In vivo, Neoplasms, lcsh:TP248.13-248.65, Microscopy, medicine, Animals, Neoplasm Metastasis, 030304 developmental biology, Mice, Inbred BALB C, Photons, 0303 health sciences, Methodology Article, Carcinoma, Cell Membrane, Resolution (electron density), Fluorescence, Rats, 3. Good health, Cell biology, Luminescent Proteins, Microscopy, Fluorescence, Multiphoton, medicine.anatomical_structure, Microscopy, Fluorescence, 030220 oncology & carcinogenesis, Collagen, Neoplasm Transplantation, Plasmids, Biotechnology

Abstract

Background: The development of multiphoton laser scanning microscopy has greatly facilitated the imaging of living tissues. However, the use of genetically encoded fluorescent proteins to distinguish different cell types in living animals has not been described at single cell resolution using multiphoton microscopy. Results: Here we describe a method for the simultaneous imaging, by multiphoton microscopy, of Green Fluorescent Protein, Cyan Fluorescent Protein and collagen in vivo in living tumors. This novel method enables: 1) the simultaneous visualization of overall cell shape and sub-cellular structures such as the plasma membrane or proteins of interest in cells inside living animals, 2) direct comparison of the behavior of single cells from different cell lines in the same microenvironment in vivo. Conclusion: Using this multi-fluor, multiphoton technique, we demonstrate that motility and metastatic differences between carcinoma cells of differing metastatic potential can be imaged in the same animal simultaneously at sub-cellular resolution., National Institutes of Health (U.S) ( grant CA100324), National Institutes of Health (U.S) ( grant GM58801), International Union against Cancer (Aventis Translational Cancer Research Fellowship)

Published

2005

44. Neuronal migration in the murine rostral migratory stream requires serum response factor

Author

Günther Schütz, Siegfried Alberti, Franziska F. Wiebel, Alfred Nordheim, Emilio Casanova, Ulrike Philippar, Heinz Schwarz, Sven M. Krause, Oliver Kretz, Thomas Lemberger, and Michael Frotscher

Subjects

Serum Response Factor, Rostral migratory stream, Subventricular zone, Mice, Transgenic, macromolecular substances, Biology, Mice, Prosencephalon, Cell Movement, Serum response factor, medicine, Animals, Sequence Deletion, Mice, Knockout, Neurons, Multidisciplinary, Brain, Cell migration, Cofilin, Biological Sciences, Actin cytoskeleton, Actins, Mice, Mutant Strains, Cell biology, medicine.anatomical_structure, nervous system, Forebrain, Immunology, Gelsolin

Abstract

The central nervous system is fundamentally dependent on guided cell migration, both during development and in adulthood. We report an absolute requirement of the transcription factor serum response factor (SRF) for neuronal migration in the mouse forebrain. Conditional, late-prenatal deletion of Srf causes neurons to accumulate ectopically at the subventricular zone (SVZ), a prime neurogenic region in the brain. SRF-deficient cells of the SVZ exhibit impaired tangential chain migration along the rostral migratory stream into the olfactory bulb. SVZ explants display retarded chain migration in vitro . Regarding target genes, SRF deficiency impairs expression of the β-actin and gelsolin genes, accompanied by reduced cytoskeletal actin fiber density. At the posttranslational level, cofilin, a key regulator of actin dynamics, displays dramatically elevated inhibitory phosphorylation at Ser-3. Our studies indicate that SRF-controlled gene expression directs both the structure and dynamics of the actin microfilament, thereby determining cell-autonomous neuronal migration.

Published

2005

45. SRF regulates Bcl-2 expression and promotes cell survival during murine embryonic development

Author

Ulrike Philippar, Heinz Schwarz, Dirk Hockemeyer, Siegfried Alberti, Alfred Nordheim, and Gerhard Schratt

Subjects

Serum Response Factor, genetic structures, Cell Survival, Cellular differentiation, Embryonic Development, Apoptosis, Embryoid body, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Mice, Transcription (biology), Depsipeptides, Serum response factor, Animals, Humans, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Cells, Cultured, Mice, Knockout, General Immunology and Microbiology, Base Sequence, General Neuroscience, Stem Cells, Gene Expression Regulation, Developmental, Cell Differentiation, musculoskeletal system, Embryo, Mammalian, Embryonic stem cell, Molecular biology, eye diseases, Cell biology, Proto-Oncogene Proteins c-bcl-2, embryonic structures, cardiovascular system, Stem cell

Abstract

The transcription factor serum response factor (SRF) controls the expression of genes involved in cellular proliferation and differentiation. Interestingly, SRF also promotes cell survival by regulating the expression of antiapoptotic genes. In in vitro differentiating murine embryonic stem (ES) cells, SRF deficiency leads to increased apoptosis. Loss of SRF correlates with impaired expression of the antiapoptotic Bcl-2 and Bcl-xl genes. SRF binds the Bcl-2 promoter in vivo and activates Bcl-2 transcription. Reconstituting Bcl-2 in Srf(−/−) ES cells rescues these cells from apoptosis, demonstrating that SRF-dependent Bcl-2 expression is critical for ES cell survival. At the multicellular level, SRF deficiency leads to impaired cavitation and reduced Bcl-2 expression in embryoid bodies (EBs) and inappropriate apoptosis in both EBs and pregastrulation mouse embryos. Thus, our data from genetic and cellular studies uncover SRF-regulated Bcl-2 expression as a novel mechanism that is important for cell survival during early murine embryogenesis.

Published

2003

46. Abstract 2343: A novel ERK inhibitor is active in models of acquired resistance to BRAF and MEK inhibitors

Author

Sharda Jha, Steve Fawell, Restaino R. Clifford, Lata Jayaraman, Bart Luttrerbach, Ahmed A. Samatar, Gary Gilliland, Ulrike Philippar, Marc Pelletier, Erick J. Morris, and Leigh Zawel

Subjects

Neuroblastoma RAS viral oncogene homolog, MAPK/ERK pathway, Trametinib, Cancer Research, business.industry, MEK inhibitor, Melanoma, Dabrafenib, medicine.disease_cause, medicine.disease, Oncology, Immunology, medicine, Cancer research, KRAS, Vemurafenib, business, medicine.drug

Abstract

The high frequency of activating BRAFV600E mutations in melanoma (40-70%), thyroid (50%) and colorectal cancer (10%), or KRAS/NRAS mutations in melanoma (20%), pancreatic (90%), colorectal (50%) and non-small cell lung cancer (30%), provides strong rationale for targeting the MAPK pathway as a therapeutic strategy 1-6. Vemurafenib (PLX4032) and dabrafenib (GSK2118436), selective BRAF inhibitors, and trametinib (GSK1120212), an allosteric MEK inhibitor, have shown robust clinical efficacy in melanoma patients 7-10. However, the majority of responses are transient and cellular resistance is often associated with pathway reactivation involving the downstream extracellular-signal-regulated kinases 1 and 2 (ERK1/2) (reviewed in 11). We hypothesized that pathway blockade at ERK, the last signaling node prior to MAPK transcriptional programming, would not only be efficacious in MAPK-activated tumors but would also have utility in BRAF or MEK inhibitor resistant settings. We therefore sought to identify small molecule inhibitors of ERK. This report describes the identification and characterization of SCH772984, a potent and selective ATP competitive inhibitor of ERK1/2 which displays behaviors of both type I and type II kinase inhibitors. SCH772984 has nanomolar cellular potency on tumor cells with mutations in BRAF, NRAS, or KRAS and induces tumor regressions in xenograft models at tolerated doses. Importantly, SCH772984 effectively inhibited MAPK signaling and cell proliferation in BRAF or MEK inhibitor resistant models as well as in the context of BRAF/MEK combination resistance. Together these data support the clinical development of ERK inhibitors, not only in patients with MAPK activated tumors, but also in patients who have developed acquired resistance to BRAF or MEK inhibitors or resistance to the recently described combination of these agents. Citation Format: Ahmed A. Samatar, Erick J. Morris, Sharda Jha, Restaino R. Clifford, Bart Luttrerbach, Marc Pelletier, Ulrike Philippar, Lata Jayaraman, Leigh Zawel, Steve Fawell, Gary Gilliland. A novel ERK inhibitor is active in models of acquired resistance to BRAF and MEK inhibitors. [abstract]. In: Proceedings of the 104th Annual Meeting of the American Association for Cancer Research; 2013 Apr 6-10; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2013;73(8 Suppl):Abstract nr 2343. doi:10.1158/1538-7445.AM2013-2343

Published

2013

47. Ena/VASP Is Required for Neuritogenesis in the Developing Cortex

Author

Frank B. Gertler, Adam V. Kwiatkowski, Ulrike Philippar, Jiangyang Zhang, Roderick T. Bronson, Leslie M. Mebane, Reinhard Fässler, Douglas A. Rubinson, Aurora A. Burds, Erik W. Dent, J. Edward van Veen, Susumu Mori, Jonathan D. Leslie, and Elaine M. Pinheiro

Subjects

Male, Neurite, Neuroscience(all), Growth Cones, DEVBIO, macromolecular substances, Biology, Nervous System Malformations, MOLNEURO, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Movement, Neural Pathways, medicine, Neurites, Animals, Pseudopodia, Axon, Cytoskeleton, Growth cone, Cells, Cultured, 030304 developmental biology, Body Patterning, Cerebral Cortex, Mice, Knockout, 0303 health sciences, Mice, Inbred BALB C, Chimera, General Neuroscience, Microfilament Proteins, Cell Differentiation, Actin cytoskeleton, Phosphoproteins, Cell biology, Mice, Inbred C57BL, Corticogenesis, Actin Cytoskeleton, medicine.anatomical_structure, nervous system, Mutation, Female, Neuroscience, Filopodia, Cell Adhesion Molecules, 030217 neurology & neurosurgery

Abstract

SummaryMammalian cortical development involves neuronal migration and neuritogenesis; this latter process forms the structural precursors to axons and dendrites. Elucidating the pathways that regulate the cytoskeleton to drive these processes is fundamental to our understanding of cortical development. Here we show that loss of all three murine Ena/VASP proteins, a family of actin regulatory proteins, causes neuronal ectopias, alters intralayer positioning in the cortical plate, and, surprisingly, blocks axon fiber tract formation during corticogenesis. Cortical fiber tract defects in the absence of Ena/VASP arise from a failure in neurite initiation, a prerequisite for axon formation. Neurite initiation defects in Ena/VASP-deficient neurons are preceded by a failure to form bundled actin filaments and filopodia. These findings provide insight into the regulation of neurite formation and the role of the actin cytoskeleton during cortical development.