Your search keyword '"John Bertin"' showing total 143 results

1. Data from Elesclomol induces cancer cell apoptosis through oxidative stress

Author

John Bertin, James Barsoum, Zhenjian Du, Mei Zhang, Chin-Yu Yang, Jane Kepros, Vishwasenani Balasubramanyam, Suqin He, and Jessica R. Kirshner

Abstract

Elesclomol (formerly STA-4783) is a novel small molecule undergoing clinical evaluation in a pivotal phase III melanoma trial (SYMMETRY). In a phase II randomized, double-blinded, controlled, multi-center trial in 81 patients with stage IV metastatic melanoma, treatment with elesclomol plus paclitaxel showed a statistically significant doubling of progression-free survival time compared with treatment with paclitaxel alone. Although elesclomol displays significant therapeutic activity in the clinic, the mechanism underlying its anticancer activity has not been defined previously. Here, we show that elesclomol induces apoptosis in cancer cells through the induction of oxidative stress. Treatment of cancer cells in vitro with elesclomol resulted in the rapid generation of reactive oxygen species (ROS) and the induction of a transcriptional gene profile characteristic of an oxidative stress response. Inhibition of oxidative stress by the antioxidant N-acetylcysteine blocked the induction of gene transcription by elesclomol. In addition, N-acetylcysteine blocked drug-induced apoptosis, indicating that ROS generation is the primary mechanism responsible for the proapoptotic activity of elesclomol. Excessive ROS production and elevated levels of oxidative stress are critical biochemical alterations that contribute to cancer cell growth. Thus, the induction of oxidative stress by elesclomol exploits this unique characteristic of cancer cells by increasing ROS levels beyond a threshold that triggers cell death. [Mol Cancer Ther 2008;7(8):2319–27]

Published

2023

2. Supplementary Table S1 from Elesclomol induces cancer cell apoptosis through oxidative stress

Author

John Bertin, James Barsoum, Zhenjian Du, Mei Zhang, Chin-Yu Yang, Jane Kepros, Vishwasenani Balasubramanyam, Suqin He, and Jessica R. Kirshner

Abstract

Supplementary Table S1 from Elesclomol induces cancer cell apoptosis through oxidative stress

Published

2023

3. Ubiquitylation of MLKL at lysine 219 positively regulates necroptosis-induced tissue injury and pathogen clearance

Author

Ioannis Roxanis, Laura Ramos Garcia, James M. Murphy, Sidonie Wicky John, Isabelle S Lucet, Andrew J. Kueh, Allison M. Beal, K. Aurelia Ball, Jyoti S. Choudhary, Cheree Fitzgibbon, Richard Newman, Jason W. Upton, Martin Sims, Lu Yu, George Ward, Gianmaria Liccardi, Winnie Fernando, Patrycja Gazinska, Naomi Guppy, Brad J. Geddes, Hyojin Kim, Samuel N. Young, Rachel O. Haich, Pascal Meier, Lung-Yu Liang, Mercedes Pardo, Tomoko Smyth, John Bertin, Tencho Tenev, and Alessandro Annibaldi

Subjects

0301 basic medicine, Muromegalovirus, Programmed cell death, Ubiquitylation, Necroptosis, Science, General Physics and Astronomy, Article, General Biochemistry, Genetics and Molecular Biology, Cell Line, Mice, Necrosis, 03 medical and health sciences, RIPK1, 0302 clinical medicine, Ubiquitin, Animals, Humans, Cells, Cultured, Skin, Mice, Knockout, Multidisciplinary, biology, Chemistry, Lysine, HEK 293 cells, Ubiquitination, Herpesviridae Infections, General Chemistry, Cell biology, Mice, Inbred C57BL, HEK293 Cells, 030104 developmental biology, Lytic cycle, Apoptosis, NIH 3T3 Cells, biology.protein, Phosphorylation, HT29 Cells, Protein Kinases, 030217 neurology & neurosurgery

Abstract

Necroptosis is a lytic, inflammatory form of cell death that not only contributes to pathogen clearance but can also lead to disease pathogenesis. Necroptosis is triggered by RIPK3-mediated phosphorylation of MLKL, which is thought to initiate MLKL oligomerisation, membrane translocation and membrane rupture, although the precise mechanism is incompletely understood. Here, we show that K63-linked ubiquitin chains are attached to MLKL during necroptosis and that ubiquitylation of MLKL at K219 significantly contributes to the cytotoxic potential of phosphorylated MLKL. The K219R MLKL mutation protects animals from necroptosis-induced skin damage and renders cells resistant to pathogen-induced necroptosis. Mechanistically, we show that ubiquitylation of MLKL at K219 is required for higher-order assembly of MLKL at membranes, facilitating its rupture and necroptosis. We demonstrate that K219 ubiquitylation licenses MLKL activity to induce lytic cell death, suggesting that necroptotic clearance of pathogens as well as MLKL-dependent pathologies are influenced by the ubiquitin-signalling system., Necroptosis is a form of cell death characterized by membrane rupture via MLKL oligomerization, although mechanistic details remain unclear. Here, the authors show that MLKL ubiquitylation of K219 facilitates high-order membrane assembly and subsequent rupture, promoting cytotoxicity.

Published

2021

4. RIPK1 kinase-dependent inflammation and cell death contribute to the pathogenesis of COPD

Author

Hannelore P. Van Eeckhoutte, Chantal Donovan, Richard Y. Kim, Thomas M. Conlon, Meshal Ansari, Haroon Khan, Ranjith Jayaraman, Nicole G. Hansbro, Yves Dondelinger, Tom Delanghe, Allison M. Beal, Brad Geddes, John Bertin, Tom Vanden Berghe, Joyceline De Volder, Tania Maes, Peter Vandenabeele, Bart M. Vanaudenaerde, Dieter Deforce, Sonja Škevin, Filip Van Nieuwerburgh, Fien M. Verhamme, Guy F. Joos, Sobia Idrees, Herbert B. Schiller, Ali Önder Yildirim, Alen Faiz, Mathieu J.M. Bertrand, Guy G. Brusselle, Philip M. Hansbro, and Ken R. Bracke

Subjects

Pulmonary and Respiratory Medicine, 11 Medical and Health Sciences, 1116 Medical Physiology, Respiratory System

Abstract

BackgroundReceptor-interacting protein kinase 1 (RIPK1) is a key mediator of regulated cell death (including apoptosis and necroptosis) and inflammation, both drivers of COPD pathogenesis. We aimed to define the contribution of RIPK1 kinase-dependent cell death and inflammation in the pathogenesis of COPD.MethodsWe assessedRIPK1expression in single-cell RNA sequencing (RNA-seq) data from human and mouse lungs, and validated RIPK1 levels in lung tissue of COPD patientsviaimmunohistochemistry. Next, we assessed the consequences of genetic and pharmacological inhibition of RIPK1 kinase activity in experimental COPD, usingRipk1S25D/S25Dkinase-deficient mice and the RIPK1 kinase inhibitor GSK′547.ResultsRIPK1expression increased in alveolar type 1 (AT1), AT2, ciliated and neuroendocrine cells in human COPD. RIPK1 protein levels were significantly increased in airway epithelium of COPD patients compared with never-smokers and smokers without airflow limitation. In mice, exposure to cigarette smoke (CS) increasedRipk1expression similarly in AT2 cells, and further in alveolar macrophages and T-cells. Genetic and/or pharmacological inhibition of RIPK1 kinase activity significantly attenuated airway inflammation upon acute and subacute CS exposure, as well as airway remodelling, emphysema, and apoptotic and necroptotic cell death upon chronic CS exposure. Similarly, pharmacological RIPK1 kinase inhibition significantly attenuated elastase-induced emphysema and lung function decline. Finally, RNA-seq on lung tissue of CS-exposed mice revealed downregulation of cell death and inflammatory pathways upon pharmacological RIPK1 kinase inhibition.ConclusionsRIPK1 kinase inhibition is protective in experimental models of COPD and may represent a novel promising therapeutic approach.

Published

2022

5. Inhibiting RIPK1 Kinase Activity Is Protective in Experimental Models of COPD

Author

Hannelore P. Van Eeckhoutte, Chantal Donovan, Richard Kim, Haroon Khan, Ranjith Jayaraman, Yves Dondelinger, Tom Delanghe, Allison Beal, Brad Geddes, John Bertin, Tom Vanden Berghe, Peter Vandenabeele, Bart Vanaudenaerde, Dieter Deforce, Sonja Skevin, Filip Van Nieuwerburgh, Fien Verhamme, Guy Joos, Guy Brusselle, Mathieu Bertrand, Philip Hansbro, and Ken Bracke

Published

2022

6. RIP1 Kinase Drives Macrophage-Mediated Adaptive Immune Tolerance in Pancreatic Cancer

Author

Juan A. Kochen Rossi, Ankita Mishra, Berk Aykut, Mautin Hundeyin, Deirdre Jill Cohen, Ece Bagdatlioglu, Atsuo Ochi, Wenyu Su, Joshua Leinwand, Pamela Nassau, Narendra Verma, Mohammed Khan, Jacqueline I. Kim, Nan Wu, Michael Reilly, James H. Thorpe, Aarif Ahsan, Fei Li, Varshini Vasudevaraja, George Miller, Allison M. Beal, Ting Chen, Wei Wang, John D. Lich, Pardeep S. Taunk, Mukesh K. Mahajan, Inedouye Yaboh, Dennis Adeegbe, Jingjing Wu, Philip A. Harris, John Bertin, Johana Gutierrez, Kwok-Kin Wong, Brian Diskin, Emma Kurz, Yue Wu, Christina Almonte, J. Mosley, Michael Glacken, Jill M. Marinis, and Shivraj Savadkar

Subjects

0301 basic medicine, Cancer Research, Macrophage polarization, Biology, Lymphocyte Activation, Article, Immune tolerance, Mice, 03 medical and health sciences, L Cells, Downregulation and upregulation, Cell Line, Tumor, Pancreatic cancer, Immune Tolerance, medicine, Animals, Humans, Macrophage, Cytotoxic T cell, Protein kinase A, Mice, Knockout, Kinase, Macrophages, Cell Biology, Th1 Cells, medicine.disease, Mice, Inbred C57BL, Pancreatic Neoplasms, STAT1 Transcription Factor, 030104 developmental biology, Oncology, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, Th17 Cells, Carcinoma, Pancreatic Ductal, T-Lymphocytes, Cytotoxic

Abstract

Summary Pancreatic ductal adenocarcinoma (PDA) is characterized by immune tolerance and immunotherapeutic resistance. We discovered upregulation of receptor-interacting serine/threonine protein kinase 1 (RIP1) in tumor-associated macrophages (TAMs) in PDA. To study its role in oncogenic progression, we developed a selective small-molecule RIP1 inhibitor with high in vivo exposure. Targeting RIP1 reprogrammed TAMs toward an MHCIIhiTNFα+IFNγ+ immunogenic phenotype in a STAT1-dependent manner. RIP1 inhibition in TAMs resulted in cytotoxic T cell activation and T helper cell differentiation toward a mixed Th1/Th17 phenotype, leading to tumor immunity in mice and in organotypic models of human PDA. Targeting RIP1 synergized with PD1-and inducible co-stimulator-based immunotherapies. Tumor-promoting effects of RIP1 were independent of its co-association with RIP3. Collectively, our work describes RIP1 as a checkpoint kinase governing tumor immunity.

Published

2020

7. Understanding Pharmacokinetic Disconnect in Preclinical Species for 4-Aminoquinolines: Consequences of Low Permeability and High P-glycoprotein Efflux Ratio on Rat and Dog Oral Pharmacokinetics

Author

Bartholomew J. Votta, Michael Reilly, Linda N. Casillas, Robert W. Marquis, Rakesh Nagilla, Mukesh K. Mahajan, Demartino Michael P, John Bertin, Helen H. Sun, Elizabeth J. Rivera, and Pamela A. Haile

Subjects

Drug, ATP Binding Cassette Transporter, Subfamily B, media_common.quotation_subject, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, Pharmacology, 030226 pharmacology & pharmacy, Permeability, 03 medical and health sciences, Dogs, 0302 clinical medicine, Pharmacokinetics, Oral administration, Animals, Medicine, media_common, P-glycoprotein, Gastrointestinal tract, biology, business.industry, Biological Transport, Transporter, 021001 nanoscience & nanotechnology, Rats, Bioavailability, Aminoquinolines, biology.protein, Efflux, 0210 nano-technology, business

Abstract

Receptor Interacting Protein 2 (RIP2) kinase inhibitors have been reported for therapeutic opportunities in inflammatory bowel diseases such as Ulcerative Colitis and Crohn's disease. During lead optimization, team identified 4-aminoquinoline series and several compounds from this series were investigated in rat and dog pharmacokinetic studies. While compounds such as GSKA and GSKB demonstrated acceptable pharmacokinetics in rat and dog, further progression of these compounds was halted due to adverse findings in advanced safety studies. Structurally similar analogues incorporating polarity at C-7 position of 4-aminoquinoline resulted in identification of GSKC - GSKF. Interestingly, following oral administration to rat at similar low dose, GSKC - GSKF demonstrated significantly low systemic drug exposure compared to GSKA and GSKB (3-17-fold difference). However, in dog, dose normalized oral systemic exposure for GSKC - GSKF was comparable to GSKA and GSKB (within 2-fold). A series of studies were conducted to understand the disconnect which highlighted that an intrinsic reduction in permeability and high P-glycoprotein (P-gp) efflux ratio for C-7 substituted analogues were driving pharmacokinetic disconnect between rat and dog. Oral absorption was minimally impacted in dog by P-gp mediated efflux compared to rat because the leakier gastrointestinal tract in dog likely overcomes this effect.

Published

2020

8. An intestinal organoid–based platform that recreates susceptibility to T-cell–mediated tissue injury

Author

Eugene Rudensky, Jennifer Tsai, Sandra J. Hoffman, Victor J. Torres, David Hudesman, Chen Liu, John Bertin, Ken Cadwell, Thomas Heaney, Brad J. Geddes, Marcel R.M. van den Brink, Jordan E. Axelrad, Yu Matsuzawa-Ishimoto, Xiaomin Yao, Allison M. Beal, Frank Yeung, P'ng Loke, Yusuke Shono, Ashley M. Hine, Jessica A Neil, Samantha L. Schuster, Michael Cammer, Ying-Han Chen, Amina Lazrak, Erin E Zwack, M. Zahidunnabi Dewan, and Katherine B Nichols

Subjects

0301 basic medicine, business.industry, Necroptosis, T cell, Immunology, Cell Biology, Hematology, medicine.disease, Biochemistry, Transplantation, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Graft-versus-host disease, medicine.anatomical_structure, Interferon, 030220 oncology & carcinogenesis, medicine, Organoid, Cancer research, business, ATG16L1, Ex vivo, medicine.drug

Abstract

A goal in precision medicine is to use patient-derived material to predict disease course and intervention outcomes. Here, we use mechanistic observations in a preclinical animal model to design an ex vivo platform that recreates genetic susceptibility to T-cell–mediated damage. Intestinal graft-versus-host disease (GVHD) is a life-threatening complication of allogeneic hematopoietic cell transplantation. We found that intestinal GVHD in mice deficient in Atg16L1, an autophagy gene that is polymorphic in humans, is reversed by inhibiting necroptosis. We further show that cocultured allogeneic T cells kill Atg16L1-mutant intestinal organoids from mice, which was associated with an aberrant epithelial interferon signature. Using this information, we demonstrate that pharmacologically inhibiting necroptosis or interferon signaling protects human organoids derived from individuals harboring a common ATG16L1 variant from allogeneic T-cell attack. Our study provides a roadmap for applying findings in animal models to individualized therapy that targets affected tissues.

Published

2020

9. Respiratory Syncytial Virus Infection Promotes Necroptosis and HMGB1 Release by Airway Epithelial Cells

Author

Yves Dondelinger, Gunter Hartel, Mark L. Everard, John Bertin, Vivian Zhang, John W. Upham, Peter J. Gough, Natasha Collinson, Antoon J. M. van Oosterhout, Rhiannon B. Werder, Mathieu J.M. Bertrand, Jennifer Simpson, Ashik Ullah, Zhixuan Loh, Kirsten Spann, Simon Phipps, Christopher C Blyth, and Jason P. Lynch

Subjects

GENETIC SUSCEPTIBILITY, CHILDREN, Critical Care and Intensive Care Medicine, Mice, 0302 clinical medicine, Medicine and Health Sciences, Medicine, Prospective Studies, 030212 general & internal medicine, HMGB1 Protein, biology, Respiratory infection, Pneumovirus, respiratory system, APOPTOSIS, DEFICIENCY, Child, Preschool, Necroptosis, Bronchiolitis, bronchiolitis, medicine.symptom, Viral load, MLKL, Pulmonary and Respiratory Medicine, PREDISPOSES, necroptosis, Inflammation, Respiratory Mucosa, Respiratory Syncytial Virus Infections, HMGB1, 03 medical and health sciences, INFLAMMATION, Animals, Humans, INNATE IMMUNE-RESPONSES, business.industry, Editorials, Biology and Life Sciences, Infant, Epithelial Cells, asthma, medicine.disease, 030228 respiratory system, Immunology, biology.protein, Respiratory epithelium, MEMBRANE, business

Abstract

Rationale: Respiratory syncytial virus (RSV) bronchiolitis causes significant infant mortality. Bronchiolitis is characterized by airway epithelial cell (AEC) death; however, the mode of death remains unknown. Objectives: To determine whether necroptosis contributes to RSV b r onchiolitis pathogenesis via HMGB1 (high mobility group box 1) release. Methods: Nasopharyngeal samples were collected from children presenting to the hospital with acute respiratory infection. Primary human AECs and neonatal mice were inoculated with RSV and murine Pneumovirus, respectively. Necroptosis was determined via viability assays and immunohistochemistry for RIPK1 (receptor-interacting protein kinase-1), MLKL (mixed lineage kinase domain-like pseudokinase) protein, and caspase-3. Necroptosis was blocked using pharmacological inhibitors and RIPK1 kinase-dead knockin mice. Measurements and Main Results: HMGB1 levels were elevated in nasopharyngeal samples of children with acute RSV infection. RSV-induced epithelial cell death was associated with increased phosphorylated RIPK1 and phosphorylated MLKL but not active caspase-3 expression. Inhibition of RIPK1 or MLKL attenuated RSV-induced HMGBI translocation and release, and lowered viral load. MLKL inhibition increased active caspase-3 expression in a caspase-8/9-dependent manner. In susceptible mice, Pneumovirus infection upregulated RIPK1 and MLKL expression in the airway epithelium at 8 to 10 days after infection, coinciding with AEC sloughing, HMGB1 release, and neutrophilic inflammation. Genetic or pharmacological inhibition of RIPK1 or MLKL attenuated these pathologies, lowered viral load, and prevented type 2 inflammation and airway remodeling. Necroptosis inhibition in early life ameliorated asthma progression induced by viral or allergen challenge in later life. Conclusions: Pneumovirus infection induces AEC necroptosis. Inhibition of necroptosis may be a viable strategy to limit the severity of viral bronchiolitis and break its nexus with asthma.

Published

2020

10. MALT1 Protease Plays a Dual Role in the Allergic Response by Acting in Both Mast Cells and Endothelial Cells

Author

Linda M. McAllister-Lucas, Tina L. Sumpter, Kevin Foley, Danielle N. Alfano, Peter J. Gough, John Bertin, Peter C. Lucas, Linda R. Klei, Matthew Trotta, and Hanna B. Klei

Subjects

medicine.medical_treatment, Immunology, Lymphocyte Activation, medicine.disease_cause, Cell Line, Proinflammatory cytokine, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Bone Marrow, Hypersensitivity, medicine, Animals, Humans, Immunology and Allergy, Mast Cells, Mast cell cytokine production, Inflammation, Protease, Receptors, IgE, Chemistry, FCER1, NF-kappa B, Degranulation, Endothelial Cells, Immunoglobulin E, Cell biology, Mice, Inbred C57BL, Cytokine, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, Allergic response, Cytokines, Female, Histamine, 030215 immunology

Abstract

The signaling protein MALT1 plays a key role in promoting NF-κB activation in Ag-stimulated lymphocytes. In this capacity, MALT1 has two functions, acting as a scaffolding protein and as a substrate-specific protease. MALT1 is also required for NF-κB–dependent induction of proinflammatory cytokines after FcεR1 stimulation in mast cells, implicating a role in allergy. Because MALT1 remains understudied in this context, we sought to investigate how MALT1 proteolytic activity contributes to the overall allergic response. We compared bone marrow–derived mast cells from MALT1 knockout (MALT1−/−) and MALT1 protease-deficient (MALTPD/PD) mice to wild-type cells. We found that MALT1−/− and MALT1PD/PD mast cells are equally impaired in cytokine production following FcεRI stimulation, indicating that MALT1 scaffolding activity is insufficient to drive the cytokine response and that MALT1 protease activity is essential. In addition to cytokine production, acute mast cell degranulation is a critical component of allergic response. Intriguingly, whereas degranulation is MALT1-independent, MALT1PD/PD mice are protected from vascular edema induced by either passive cutaneous anaphylaxis or direct challenge with histamine, a major granule component. This suggests a role for MALT1 protease activity in endothelial cells targeted by mast cell–derived vasoactive substances. Indeed, we find that in human endothelial cells, MALT1 protease is activated following histamine treatment and is required for histamine-induced permeability. We thus propose a dual role for MALT1 protease in allergic response, mediating 1) IgE-dependent mast cell cytokine production, and 2) histamine-induced endothelial permeability. This dual role indicates that therapeutic inhibitors of MALT1 protease could work synergistically to control IgE-mediated allergic disease.

Published

2020

11. Discovery of a First-in-Class Receptor Interacting Protein 2 (RIP2) Kinase Specific Clinical Candidate, 2-((4-(Benzo[d]thiazol-5-ylamino)-6-(tert-butylsulfonyl)quinazolin-7-yl)oxy)ethyl Dihydrogen Phosphate, for the Treatment of Inflammatory Diseases

Author

Pamela A. Haile, Linda N. Casillas, Bartholomew J. Votta, Gren Z. Wang, Adam K. Charnley, Xiaoyang Dong, Michael J. Bury, Joseph J. Romano, John F. Mehlmann, Bryan W. King, Karl F. Erhard, Charles R. Hanning, David B. Lipshutz, Biva M. Desai, Carol A. Capriotti, Michelle C. Schaeffer, Scott B. Berger, Mukesh K. Mahajan, Michael A. Reilly, Rakesh Nagilla, Elizabeth J. Rivera, Helen H. Sun, John K. Kenna, Allison M. Beal, Michael T. Ouellette, Mike Kelly, Gillian Stemp, Máire A. Convery, Anna Vossenkämper, Thomas T. MacDonald, Peter J. Gough, John Bertin, and Robert W. Marquis

Subjects

Drug Discovery, Molecular Medicine

Published

2019

12. Discovery and Lead-Optimization of 4,5-Dihydropyrazoles as Mono-Kinase Selective, Orally Bioavailable and Efficacious Inhibitors of Receptor Interacting Protein 1 (RIP1) Kinase

Author

Stéphane Sautet, Emilie Jigorel, Nicolas Faucher, Jamel Meslamani, Lara Kathryn Leister, Pascal Grondin, Julie A. Cox, Bryan W. King, Pamela Nassau, Gemma Victoria White, Brad J. Geddes, Alain Claude-Marie Daugan, Helen H. Sun, Michael T. Ouellette, Pauline Lamoureux, Elizabeth J. Rivera, Scott B. Berger, James H. Thorpe, Philip A. Harris, J. Mosley, Susan E. Hutchinson, Frédéric Donche, John Bertin, Sandra J. Hoffman, Natalie Wellaway, Patrick M. Eidam, Paris Ward, Florent Potvain, Clark A. Sehon, Sebastien Andre Campos, Robert W. Marquis, Peter J. Gough, Mukesh K. Mahajan, Veronique Beneton, Jae U. Jeong, Michelle C. Schaeffer, John D. Lich, Allison M. Beal, Rakesh Nagilla, James Michael Woolven, Bonnie L. Hoffman, Anderson Niall Andrew, Marie-Hélène Fouchet, Deepak Bandyopadhyay, Carol A. Capriotti, Rachel D. Totoritis, Joshua N. Finger, Kishore K. Pasikanti, David D. Wisnoski, Sze-Ling Ng, Nino Campobasso, Nicolas George, and Michael Reilly

Subjects

Models, Molecular, Encephalomyelitis, Autoimmune, Experimental, Multiple Sclerosis, Necroptosis, Biological Availability, Inflammation, Pharmacology, 01 natural sciences, Cell Line, Mice, Structure-Activity Relationship, 03 medical and health sciences, In vivo, Psoriasis, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Enzyme Inhibitors, 030304 developmental biology, 0303 health sciences, Kinase, Chemistry, RNA-Binding Proteins, Haplorhini, medicine.disease, Ulcerative colitis, High-Throughput Screening Assays, Rats, 0104 chemical sciences, Mice, Inbred C57BL, Nuclear Pore Complex Proteins, 010404 medicinal & biomolecular chemistry, Drug Design, Rheumatoid arthritis, Chronic Disease, Pyrazoles, Molecular Medicine, medicine.symptom, Retinitis Pigmentosa

Abstract

RIP1 kinase regulates necroptosis and inflammation and may play an important role in contributing to a variety of human pathologies, including inflammatory and neurological diseases. Currently, RIP1 kinase inhibitors have advanced into early clinical trials for evaluation in inflammatory diseases such as psoriasis, rheumatoid arthritis, and ulcerative colitis and neurological diseases such as amyotrophic lateral sclerosis and Alzheimer's disease. In this paper, we report on the design of potent and highly selective dihydropyrazole (DHP) RIP1 kinase inhibitors starting from a high-throughput screen and the lead-optimization of this series from a lead with minimal rat oral exposure to the identification of dihydropyrazole 77 with good pharmacokinetic profiles in multiple species. Additionally, we identified a potent murine RIP1 kinase inhibitor 76 as a valuable in vivo tool molecule suitable for evaluating the role of RIP1 kinase in chronic models of disease. DHP 76 showed efficacy in mouse models of both multiple sclerosis and human retinitis pigmentosa.

Published

2019

13. Necroptosis inhibition as a therapy for Niemann-Pick disease, type C1: Inhibition of RIP kinases and combination therapy with 2-hydroxypropyl-β-cyclodextrin

Author

John Bertin, Alexander Salman, Antony Cougnoux, Forbes D. Porter, S. Clifford, and S.-L. Ng

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Combination therapy, Endocrinology, Diabetes and Metabolism, Necroptosis, Apoptosis, Pharmacology, Biochemistry, Article, Excipients, Mice, Necrosis, 03 medical and health sciences, RIPK1, Endocrinology, Niemann-Pick C1 Protein, hemic and lymphatic diseases, Genetics, Animals, Medicine, Cognitive decline, Kinase activity, Molecular Biology, Neuroinflammation, Mice, Knockout, Mice, Inbred BALB C, Kinase, business.industry, Intracellular Signaling Peptides and Proteins, Proteins, nutritional and metabolic diseases, Niemann-Pick Disease, Type C, Combined Modality Therapy, 2-Hydroxypropyl-beta-cyclodextrin, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Receptor-Interacting Protein Serine-Threonine Kinases, NPC1, business

Abstract

Niemann-Pick disease, type C1 (NPC1) is an inborn error of metabolism that results in endolysosomal accumulation of unesterified cholesterol. Clinically, NPC1 manifests as cholestatic liver disease in the newborn or as a progressive neurogenerative condition characterized by cerebellar ataxia and cognitive decline. Currently there are no FDA approved therapies for NPC1. Thus, understanding the pathological processes that contribute to neurodegeneration will be important in both developing and testing potential therapeutic interventions. Neuroinflammation and necroptosis contribute to the NPC1 pathological cascade. Receptor Interacting Protein Kinase 1 and 3 (RIPK1 and RIPK3), are protein kinases that play a central role in mediating neuronal necroptosis. Our prior work suggested that pharmacological inhibition of RIPK1 had a significant but modest beneficial effect; however, the inhibitors used in that study had suboptimal pharmacokinetic properties. In this work we evaluated both pharmacological and genetic inhibition of RIPK1 kinase activity. Lifespan in both Npc1(−/−)mice treated with GSK’547, a RIPK1 inhibitor with better pharmacokinetic properties, and Npc1(−/−) :Ripk1(kd/kd) double mutant mice was significantly increased. In both cases the increase in lifespan was modest, suggesting that the therapeutic potential of RIPK1 inhibition, as a monotherapy, is limited. We thus investigated the potential of combining RIPK1 inhibition with 2-hydroxypropyl-β-cyclodextrin (HPβCD) therapy HPβCD has been shown to slow neurological disease progression in NPC1 mice, cats and patients. HPpβCD appeared to have an additive positive effect on the pathology and survival of Npc1(−/−):Ripk1(kd/kd) mice. RIPK1 and RIPK3 are both critical components of the necrosome, thus we were surprised to observe no increase survival in Npc1(−/−);Ripk3(−/−) mice compared to Npc1(−/−) mice. These data suggest that although necroptosis is occurring in NPC1, the observed effects of RIPK1 inhibition may be related to its RIPK3-independent role in neuroinflammation and cytokine production.

Published

2018

14. Stage-Dependent Impact of RIPK1 Inhibition on Atherogenesis: Dual Effects on Inflammation and Foam Cell Dynamics

Author

Qing Wan, Hong Chen, John Bertin, Zekun Peng, Yonghu Huang, Brad J. Geddes, Yuze Zhang, Jean-Luc Tran, Michael Reilly, Guoli Yang, Miao Wang, Haojie Rao, and Huihui Li

Subjects

Programmed cell death, RIPK1, CD36, Inflammation, Pharmacology, Cardiovascular Medicine, Macrophage, Medicine, Diseases of the circulatory (Cardiovascular) system, Protein kinase A, Receptor, Foam cell, Original Research, biology, business.industry, Monocyte, foam cells, macrophages, reverse cholesterol transport, medicine.anatomical_structure, cell death, inflammation, RC666-701, biology.protein, lipids (amino acids, peptides, and proteins), medicine.symptom, atherosclerosis, Cardiology and Cardiovascular Medicine, business

Abstract

Objective: Atherosclerosis is an arterial occlusive disease with hypercholesterolemia and hypertension as common risk factors. Advanced-stage stenotic plaque, which features inflammation and necrotic core formation, is the major reason for clinical intervention. Receptor interacting serine/threonine-protein kinase 1 (RIPK1) mediates inflammation and cell death and is expressed in atherosclerotic lesions. The role of RIPK1 in advanced-stage atherosclerosis is unknown.Approach and Results: To investigate the effect of RIPK1 inhibition in advanced atherosclerotic plaque formation, we used ApoESA/SA mice, which exhibit hypercholesterolemia, and develop angiotensin-II mediated hypertension upon administration of doxycycline in drinking water. These mice readily develop severe atherosclerosis, including that in coronary arteries. Eight-week-old ApoESA/SA mice were randomized to orally receive a highly selective RIPK1 inhibitor (RIPK1i, GSK547) mixed with a western diet, or control diet. RIPK1i administration reduced atherosclerotic plaque lesion area at 2 weeks of treatment, consistent with suppressed inflammation (MCP-1, IL-1β, TNF-α) and reduced monocyte infiltration. However, administration of RIPK1i unexpectedly exacerbated atherosclerosis at 4 weeks of treatment, concomitant with increased macrophages and lipid deposition in the plaques. Incubation of isolated macrophages with oxidized LDL resulted in foam cell formation in vitro. RIPK1i treatment promoted such foam cell formation while suppressing the death of these cells. Accordingly, RIPK1i upregulated the expression of lipid metabolism-related genes (Cd36, Ppara, Lxrα, Lxrb, Srebp1c) in macrophage foam cells with ABCA1/ABCG1 unaltered. Furthermore, RIPK1i treatment inhibited ApoA1 synthesis in the liver and reduced plasma HDL levels.Conclusion: RIPK1 modulates the development of atherosclerosis in a stage-dependent manner, implicating both pro-atherosclerotic (monocyte infiltration and inflammation) and anti-atherosclerotic effects (suppressing foam cell accumulation and promoting ApoA1 synthesis). It is critical to identify an optimal therapeutic duration for potential clinical use of RIPK1 inhibitor in atherosclerosis or other related disease indications.

Published

2021

15. A diamidobenzimidazole STING agonist protects against SARS-CoV-2 infection

Author

Sze-Ling Ng, René Maehr, Angel I. Morales-Ramos, Krishna-Mohan Parsi, Philip S. Landis, Liraz Shmuel-Galia, Zhaozhao Jiang, G. Scott Pesiridis, John Cruz, Ruth Wilson, Ramanjulu Joshi M, John Bertin, Katherine A. Fitzgerald, and Fiachra Humphries

Subjects

0301 basic medicine, viruses, Immunology, medicine.disease_cause, Virus, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Medicine, Research Articles, Coronavirus, Lung, business.industry, R-Articles, Respiratory disease, General Medicine, medicine.disease, Virology, Sting, 030104 developmental biology, medicine.anatomical_structure, Viral replication, business, 030217 neurology & neurosurgery, Respiratory tract

Abstract

Coronaviruses are a family of RNA viruses that cause acute and chronic diseases of the upper and lower respiratory tract in humans and other animals. SARS-CoV-2 is a recently emerged coronavirus that has led to a global pandemic causing a severe respiratory disease known as COVID-19 with significant morbidity and mortality worldwide. The development of antiviral therapeutics are urgently needed while vaccine programs roll out worldwide. Here we describe a diamidobenzimidazole compound, diABZI-4, that activates STING and is highly effective in limiting SARS-CoV-2 replication in cells and animals. diABZI-4 inhibited SARS-CoV-2 replication in lung epithelial cells. Administration of diABZI-4 intranasally before or even after virus infection conferred complete protection from severe respiratory disease in K18-ACE2-transgenic mice infected with SARS-CoV-2. Intranasal delivery of diABZI-4 induced a rapid short-lived activation of STING, leading to transient proinflammatory cytokine production and lymphocyte activation in the lung associated with inhibition of viral replication. Our study supports the use of diABZI-4 as a host-directed therapy which mobilizes antiviral defenses for the treatment and prevention of COVID-19., Pharmacological activation of STING protects against SARS-CoV-2 infection.

Published

2021

16. Protective Effects of Necrostatin-1 in Acute Pancreatitis: Partial Involvement of Receptor Interacting Protein Kinase 1

Author

Mohammad Awais, Wei Huang, Wenhao Cai, John Bertin, Alexei V. Tepikin, Li Wen, Jane A Armstrong, Michael Chvanov, David N. Criddle, Rajarshi Mukherjee, Robert Sutton, Peter J. Gough, Diane Latawiec, and Yulin Ouyang

Subjects

0301 basic medicine, Male, Programmed cell death, Indoles, RIPK1, acute pancreatitis, indoleamine 2,3-dioxygenase, QH301-705.5, Necroptosis, necroptosis, Acinar Cells, Pharmacology, Protective Agents, Article, Bile Acids and Salts, 03 medical and health sciences, 0302 clinical medicine, medicine, Acinar cell, Animals, Indoleamine-Pyrrole 2,3,-Dioxygenase, Biology (General), Protein kinase A, Indoleamine 2,3-dioxygenase, Pancreas, Kinase, Chemistry, Imidazoles, General Medicine, medicine.disease, epacadostat, digestive system diseases, Mice, Inbred C57BL, receptor-interacting protein kinase 1, 030104 developmental biology, cell death, Pancreatitis, 030220 oncology & carcinogenesis, Alcohols, Receptor-Interacting Protein Serine-Threonine Kinases, Acute pancreatitis, Calcium, necrostatin-1, Reactive Oxygen Species, Ceruletide

Abstract

Acute pancreatitis (AP) is a severe and potentially fatal disease caused predominantly by alcohol excess and gallstones, which lacks a specific therapy. The role of Receptor-Interacting Protein Kinase 1 (RIPK1), a key component of programmed necrosis (Necroptosis), is unclear in AP. We assessed the effects of RIPK1 inhibitor Necrostatin-1 (Nec-1) and RIPK1 modification (RIPK1K45A: kinase dead) in bile acid (TLCS-AP), alcoholic (FAEE-AP) and caerulein hyperstimulation (CER-AP) mouse models. Involvement of collateral Nec-1 target indoleamine 2,3-dioxygenase (IDO) was probed with the inhibitor Epacadostat (EPA). Effects of Nec-1 and RIPK1K45A were also compared on pancreatic acinar cell (PAC) fate in vitro and underlying mechanisms explored. Nec-1 markedly ameliorated histological and biochemical changes in all models. However, these were only partially reduced or unchanged in RIPK1K45A mice. Inhibition of IDO with EPA was protective in TLCS-AP. Both Nec-1 and RIPK1K45A modification inhibited TLCS- and FAEE-induced PAC necrosis in vitro. Nec-1 did not affect TLCS-induced Ca2+ entry in PACs, however, it inhibited an associated ROS elevation. The results demonstrate protective actions of Nec-1 in multiple models. However, RIPK1-dependent necroptosis only partially contributed to beneficial effects, and actions on targets such as IDO are likely to be important.

Published

2021

17. Human rhinovirus promotes STING trafficking to replication organelles to promote viral replication

Author

Martha Triantafilou, Joshi Ramanjulu, Lee M. Booty, Gisela Jimenez-Duran, Hakan Keles, Ken Saunders, Neysa Nevins, Emma Koppe, Louise K. Modis, G. Scott Pesiridis, John Bertin, and Kathy Triantafilou

Subjects

Organelles, Multidisciplinary, Rhinovirus, virus diseases, General Physics and Astronomy, Humans, RNA Viruses, General Chemistry, Virus Replication, eye diseases, General Biochemistry, Genetics and Molecular Biology, Enterovirus

Abstract

Human rhinovirus (HRV), like coronavirus (HCoV), are positive-strand RNA viruses that cause both upper and lower respiratory tract illness, with their replication facilitated by concentrating RNA-synthesizing machinery in intracellular compartments made of modified host membranes, referred to as replication organelles (ROs). Here we report a non-canonical, essential function for stimulator of interferon genes (STING) during HRV infections. While the canonical function of STING is to detect cytosolic DNA and activate inflammatory responses, HRV infection triggers the release of STIM1-bound STING in the ER by lowering Ca2+, thereby allowing STING to interact with phosphatidylinositol 4-phosphate (PI4P) and traffic to ROs to facilitates viral replication and transmission via autophagy. Our results thus hint a critical function of STING in HRV viral replication and transmission, with possible implications for other RO-mediated RNA viruses.

Published

2020

18. Receptor-interacting protein 1 kinase inhibition therapeutically ameliorates experimental T cell-dependent colitis in mice

Author

Gail Pearse, Isobel Harada, Tom Slocombe, Scott B. Berger, John Bertin, Allison M. Beal, Kathryn Fountain, Andrea C. Haynes, Alison Rowles, and Thomas Gobbetti

Subjects

Cancer Research, T cell, T-Lymphocytes, Immunology, Mice, SCID, Cellular and Molecular Neuroscience, Mice, medicine, Animals, Humans, Colitis, lcsh:QH573-671, Chemistry, lcsh:Cytology, Comment, Cell Biology, Chronic inflammation, Kinase inhibition, medicine.disease, Disease Models, Animal, medicine.anatomical_structure, Pharmacodynamics, Cancer research, Female, RECEPTOR-INTERACTING PROTEIN

Published

2020

19. RIPK1 gene variants associate with obesity in humans and can be therapeutically silenced to reduce obesity in mice

Author

Anne-Claire Duchez, Markku Laakso, Kirsi H. Pietiläinen, Ludovic Boytard, Calvin Pan, David Smyth, Richard G. Lee, Marcus Alvarez, Joshua W. Kandiah, Peter J. Gough, Aldons J. Lusis, Peter Liu, Paulina Lau, Majid Nikpay, My-Anh Nguyen, Scott B. Berger, Denuja Karunakaran, Hailey Wyatt, Adil Rasheed, Barbara C. Vanderhyden, John Bertin, Michele Geoffrion, Sébastien Soubeyrand, Päivi Pajukanta, David P. Cook, Adam W. Turner, Katey J. Rayner, Bhama Ramkhelawon, Ruth McPherson, and Mary-Ellen Harper

Subjects

Male, Endocrinology, Diabetes and Metabolism, Necroptosis, Subcutaneous Fat, Adipose tissue, Mice, Obese, Inflammation, Genome-wide association study, Biology, FTO gene, Article, 03 medical and health sciences, RIPK1, Mice, 0302 clinical medicine, Physiology (medical), Internal Medicine, medicine, Adipocytes, Gene silencing, Animals, Humans, Gene Silencing, Obesity, 030304 developmental biology, 0303 health sciences, Innate immune system, Polymorphism, Genetic, Cell Biology, Glucose Tolerance Test, 3. Good health, Mice, Inbred C57BL, Basic-Leucine Zipper Transcription Factors, Adipose Tissue, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, medicine.symptom, Energy Metabolism, 030217 neurology & neurosurgery

Abstract

Obesity is a major public health burden worldwide and is characterized by chronic low-grade inflammation driven by the cooperation of the innate immune system and dysregulated metabolism in adipose tissue and other metabolic organs. Receptor-interacting serine/threonine-protein kinase 1 (RIPK1) is a central regulator of inflammatory cell function that coordinates inflammation, apoptosis and necroptosis in response to inflammatory stimuli. Here we show that genetic polymorphisms near the human RIPK1 locus associate with increased RIPK1 gene expression and obesity. We show that one of these single nucleotide polymorphisms is within a binding site for E4BP4 and increases RIPK1 promoter activity and RIPK1 gene expression in adipose tissue. Therapeutic silencing of RIPK1 in vivo in a mouse model of diet-induced obesity dramatically reduces fat mass, total body weight and improves insulin sensitivity, while simultaneously reducing macrophage and promoting invariant natural killer T cell accumulation in adipose tissue. These findings demonstrate that RIPK1 is genetically associated with obesity, and reducing RIPK1 expression is a potential therapeutic approach to target obesity and related diseases.

Published

2020

20. RIPK1 Mediates TNF-Induced Intestinal Crypt Apoptosis During Chronic NF-κB Activation

Author

P J Gough, Koji Taniguchi, Núria Planell, John Bertin, Soumita Das, Matija Zelic, Manolis Pasparakis, Philip A. Harris, Samuel B. Ho, Ricard Garcia-Carbonell, Shih Jing Yao, Joan Font-Burgada, Michelle A. Kelliher, Azucena Salas, Jerry Wong, Michael Karin, Monica Guma, Shalin A. Desai, and Brigid S. Boland

Subjects

0301 basic medicine, WT, wild type, Indoles, Ulcerative, Apoptosis, Crohn's Disease, Oral and gastrointestinal, IEC, intestinal epithelial cell, Mice, 0302 clinical medicine, Crohn Disease, 2.1 Biological and endogenous factors, Gene Knock-In Techniques, RNA-Seq, Intestinal Mucosa, Aetiology, Intestinal Epithelial Cell, TNF, tumor necrosis factor, Cultured, IBD, inflammatory bowel disease, Cell Death, Chemistry, Kinase, Caspase 3, Gastroenterology, Imidazoles, Colonoscopy, Colitis, 3. Good health, I-kappa B Kinase, Cc-8, cleaved caspase-8, Organoids, Receptor-Interacting Protein Serine-Threonine Kinases, I.p., intraperitoneally, LPS, lipopolysaccharide, 030211 gastroenterology & hepatology, Tumor necrosis factor alpha, Cc-3, cleaved caspase-3, NF, nuclear factor, IHC, immunohistochemistry, Adult, Programmed cell death, RIPK1, Colon, Cells, Knockout, Primary Cell Culture, IBD, Ripoptosome, PBS, phosphate-buffered saline, Qpcr, quantitative polymerase chain reaction, digestive system, Autoimmune Disease, 03 medical and health sciences, CHX, cycloheximide, Ileum, Animals, Humans, lcsh:RC799-869, Kinase activity, IB, immunoblotting, Protein kinase A, Hepatology, Animal, Tumor Necrosis Factor-alpha, Nec-1, necrostatin-1, Inflammatory Bowel Disease, Transcription Factor RelA, Epithelial Cells, digestive system diseases, UC, ulcerative colitis, 030104 developmental biology, BHA, butylated hydroxyanisole, DPI, phenyleneiodonium, Disease Models, Cancer research, lcsh:Diseases of the digestive system. Gastroenterology, CD, Crohn's disease, Digestive Diseases

Abstract

Background and Aims: Tumor necrosis factor (TNF) is a major pathogenic effector and a therapeutic target in inflammatory bowel disease (IBD), yet the basis for TNF-induced intestinal epithelial cell (IEC) death is unknown, because TNF does not kill normal IECs. Here, we investigated how chronic nuclear factor (NF)- κB activation, which occurs in human IBD, promotes TNF-dependent IEC death in mice. Methods: Human IBD specimens were stained for p65 and cleaved caspase-3. C57BL/6 mice with constitutively active IKKβ in IEC (Ikkβ(EE)IEC), Ripk1D138N/D138N knockin mice, and Ripk3-/- mice were injected with TNF or lipopolysaccharide. Enteroids were also isolated from these mice and challenged with TNF with or without RIPK1 and RIPK3 inhibitors or butylated hydroxyanisole. Ripoptosome-mediated caspase-8 activation was assessed by immunoprecipitation. Results: NF-κB activation in human IBD correlated with appearance of cleaved caspase-3. Congruently, unlike normal mouse IECs that are TNF-resistant, IECs in Ikkβ(EE)IEC mice and enteroids were susceptible to TNF-dependent apoptosis, which depended on the protein kinase function of RIPK1. Constitutively active IKKβ facilitated ripoptosome formation, a RIPK1 signaling complex that mediates caspase-8 activation by TNF. Butylated hydroxyanisole treatment and RIPK1 inhibitors attenuated TNF-induced and ripoptosome-mediated caspase-8 activation and IEC death in vitro and in vivo. Conclusions: Contrary to common expectations, chronic NF-κB activation induced intestinal crypt apoptosis after TNF stimulation, resulting in severe mucosal erosion. RIPK1 kinase inhibitors selectively inhibited TNF destructive properties while preserving its survival and proliferative properties, which do not require RIPK1 kinase activity. RIPK1 kinase inhibition could be a potential treatment for IBD. Keywords: IBD, RIPK1, Intestinal Epithelial Cell, Ripoptosome, Cell Death

Published

2020

21. t-BuOOH induces ferroptosis in human and murine cell lines

Author

Peter J. Gough, Berenike Linz, Teodora Nikolova, Dagmar Faust, Peter Wipf, John Bertin, Christian Turmann, Anna Sophia Schröder, Christine Wenz, Stefan Krautwald, and Cornelia Dietrich

Subjects

Keratinocytes, 0301 basic medicine, Programmed cell death, Cardiolipins, Cell Survival, Health, Toxicology and Mutagenesis, Apoptosis, Phenylenediamines, Biology, Toxicology, medicine.disease_cause, Cell Line, Lipid peroxidation, Mice, 03 medical and health sciences, RIPK1, chemistry.chemical_compound, tert-Butylhydroperoxide, Quinoxalines, medicine, Animals, Humans, Spiro Compounds, Protein kinase A, Membrane Potential, Mitochondrial, chemistry.chemical_classification, Cyclohexylamines, Reactive oxygen species, Kinase, Hydrogen Peroxide, General Medicine, Molecular biology, Cell biology, 030104 developmental biology, chemistry, NIH 3T3 Cells, Lipid Peroxidation, Reactive Oxygen Species, Oxidative stress

Abstract

Reactive oxygen species (ROS)-induced apoptosis has been extensively studied. Increasing evidence suggests that ROS, for instance, induced by hydrogen peroxide (H2O2), might also trigger regulated necrotic cell death pathways. Almost nothing is known about the cell death pathways triggered by tertiary-butyl hydroperoxide (t-BuOOH), a widely used inducer of oxidative stress. The lipid peroxidation products induced by t-BuOOH are involved in the pathophysiology of many diseases, such as cancer, cardiovascular diseases, or diabetes. In this study, we exposed murine fibroblasts (NIH3T3) or human keratinocytes (HaCaT) to t-BuOOH (50 or 200 μM, respectively) which induced a rapid necrotic cell death. Well-established regulators of cell death, i.e., p53, poly(ADP)ribose polymerase-1 (PARP-1), the stress kinases p38 and c-Jun N-terminal-kinases 1/2 (JNK1/2), or receptor-interacting serine/threonine protein kinase 1 (RIPK1) and 3 (RIPK3), were not required for t-BuOOH-mediated cell death. Using the selective inhibitors ferrostatin-1 (1 μM) and liproxstatin-1 (1 μM), we identified ferroptosis, a recently discovered cell death mechanism dependent on iron and lipid peroxidation, as the main cell death pathway. Accordingly, t-BuOOH exposure resulted in a ferrostatin-1- and liproxstatin-1-sensitive increase in lipid peroxidation and cytosolic ROS. Ferroptosis was executed independently from other t-BuOOH-mediated cellular damages, i.e., loss of mitochondrial membrane potential, DNA double-strand breaks, or replication block. H2O2 did not cause ferroptosis at equitoxic concentrations (300 μM) and induced a (1) lower and (2) ferrostatin-1- or liproxstatin-1-insensitive increase in lipid peroxidation. We identify that t-BuOOH and H2O2 produce a different pattern of lipid peroxidation, thereby leading to different cell death pathways and present t-BuOOH as a novel inducer of ferroptosis.

Published

2017

22. Genetic Inhibition of Receptor Interacting Protein Kinase-1 Reduces Cell Death and Improves Functional Outcome After Intracerebral Hemorrhage in Mice

Author

Lauren M. McAllister, Alexei Degterev, Yi Zheng, Joon Yong Chung, Limin Wu, Michael J. Whalen, Sevda Lule, John Bertin, Eng H. Lo, William J Edmiston, Emily Levy, and Peter J. Gough

Subjects

0301 basic medicine, Programmed cell death, Necrosis, Blotting, Western, Morris water navigation task, Apoptosis, Pharmacology, Article, Mice, 03 medical and health sciences, RIPK1, 0302 clinical medicine, medicine, Animals, Maze Learning, Protein Kinase Inhibitors, Cerebral Hemorrhage, Neurons, Advanced and Specialized Nursing, Intracerebral hemorrhage, Behavior, Animal, Cell Death, Kinase, business.industry, Point mutation, Brain, medicine.disease, Immunohistochemistry, 030104 developmental biology, Protein kinase domain, Receptor-Interacting Protein Serine-Threonine Kinases, Mutation, Immunology, Neurology (clinical), medicine.symptom, Cardiology and Cardiovascular Medicine, business, 030217 neurology & neurosurgery

Abstract

Background and Purpose— Recent studies using cultured cells and rodent intracerebral hemorrhage (ICH) models have implicated RIPK1 (receptor interacting protein kinase-1) as a driver of programmed necrosis and secondary injury based on use of chemical inhibitors. However, these inhibitors have off-target effects and cannot be used alone to prove a role for RIPK1. The aim of the current study was to examine the effect of genetic inhibition of the kinase domain of RIPK1 in a mouse ICH model. Methods— We subjected 2 lines of mice with RIPK1 point mutations of the kinase domain (K45A and D138N), rendering them kinase inactive, to autologous blood ICH and measured acute cell death and functional outcome. Results— Compared with wild-type controls, RIPK1 K45A/K45A and RIPK1 D138N/D138N had significantly less cells with plasmalemma permeability, less acute neuronal cell death, less weight loss and more rapid weight gain to baseline, and improved performance in a Morris water maze paradigm after autologous blood ICH. In addition, mice systemically administered GSK′963, a potent, specific, brain penetrant small molecule RIPK1 inhibitor, had reduced acute neuronal death at 24 hours after ICH. Conclusions— The data show that the kinase domain of RIPK1 is a disease driver of ICH, mediating both acute cell death and functional outcome, and support development of RIPK1 inhibitors as therapeutic agents for human ICH.

Published

2017

23. RIPK1-dependent apoptosis bypasses pathogen blockade of innate signaling to promote immune defense

Author

Baofeng Hu, Igor E. Brodsky, Ruth Choa, Kendra Asklof, Elisabet Bjanes, Elisabeth L. Buza, Alexandra DeLaney, Falon Gray, Lance W. Peterson, Meghan A. Wynosky-Dolfi, Christopher P. Dillon, Peter J. Gough, Douglas R. Green, Naomi H. Philip, Scott B. Berger, and John Bertin

Subjects

0301 basic medicine, Cell signaling, Programmed cell death, MAP Kinase Signaling System, Immunology, Yersinia pseudotuberculosis Infections, Apoptosis, Biology, 03 medical and health sciences, RIPK1, Immunity, Animals, Immunology and Allergy, Kinase activity, Research Articles, Disease Resistance, Mice, Knockout, Innate immune system, Effector, Macrophages, Brief Definitive Report, Models, Immunological, NF-kappa B, biochemical phenomena, metabolism, and nutrition, Survival Analysis, Immunity, Innate, 3. Good health, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Yersinia pseudotuberculosis, Receptor-Interacting Protein Serine-Threonine Kinases, Host-Pathogen Interactions, Cytokines, Signal transduction, Signal Transduction

Abstract

RIPK1 regulates cytokine signaling and cell death during infection and inflammation. Peterson et al. show that RIPK1 kinase activity triggers apoptosis in response to bacterial pathogen blockade of innate immune signaling and that this pathway of effector-triggered immunity is critical for a successful antibacterial response., Many pathogens deliver virulence factors or effectors into host cells in order to evade host defenses and establish infection. Although such effector proteins disrupt critical cellular signaling pathways, they also trigger specific antipathogen responses, a process termed “effector-triggered immunity.” The Gram-negative bacterial pathogen Yersinia inactivates critical proteins of the NF-κB and MAPK signaling cascade, thereby blocking inflammatory cytokine production but also inducing apoptosis. Yersinia-induced apoptosis requires the kinase activity of receptor-interacting protein kinase 1 (RIPK1), a key regulator of cell death, NF-κB, and MAPK signaling. Through the targeted disruption of RIPK1 kinase activity, which selectively disrupts RIPK1-dependent cell death, we now reveal that Yersinia-induced apoptosis is critical for host survival, containment of bacteria in granulomas, and control of bacterial burdens in vivo. We demonstrate that this apoptotic response provides a cell-extrinsic signal that promotes optimal innate immune cytokine production and antibacterial defense, demonstrating a novel role for RIPK1 kinase–induced apoptosis in mediating effector-triggered immunity to circumvent pathogen inhibition of immune signaling.

Published

2017

24. Kinase Activities of RIPK1 and RIPK3 Can Direct IFN-β Synthesis Induced by Lipopolysaccharide

Author

Alexei Degterev, Matija Zelic, Siddharth Balachandran, Michelle A. Kelliher, Nikolai Slavov, Danish Saleh, Saumil Shah, Katherine A. Fitzgerald, Apostolos Polykratis, Peter J. Gough, Malek Najjar, Manolis Pasparakis, Joan Mecsas, John Bertin, Michelle K. Paczosa, Shoko Nogusa, and Michael J. Whalen

Subjects

Lipopolysaccharides, 0301 basic medicine, Lipopolysaccharide, Necroptosis, Immunology, Apoptosis, Biology, Article, Mice, Necrosis, 03 medical and health sciences, RIPK1, chemistry.chemical_compound, 0302 clinical medicine, Klebsiella, Gram-Negative Bacteria, Animals, Immunology and Allergy, Phosphorylation, Central element, Innate immune system, Kinase, Effector, Macrophages, Interferon-beta, Yersinia, Cell biology, Toll-Like Receptor 4, 030104 developmental biology, chemistry, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, TLR4

Abstract

The innate immune response is a central element of the initial defense against bacterial and viral pathogens. Macrophages are key innate immune cells that upon encountering pathogen-associated molecular patterns respond by producing cytokines, including IFN-β. In this study, we identify a novel role for RIPK1 and RIPK3, a pair of homologous serine/threonine kinases previously implicated in the regulation of necroptosis and pathologic tissue injury, in directing IFN-β production in macrophages. Using genetic and pharmacologic tools, we show that catalytic activity of RIPK1 directs IFN-β synthesis induced by LPS in mice. Additionally, we report that RIPK1 kinase–dependent IFN-β production may be elicited in an analogous fashion using LPS in bone marrow–derived macrophages upon inhibition of caspases. Notably, this regulation requires kinase activities of both RIPK1 and RIPK3, but not the necroptosis effector protein, MLKL. Mechanistically, we provide evidence that necrosome-like RIPK1 and RIPK3 aggregates facilitate canonical TRIF–dependent IFN-β production downstream of the LPS receptor TLR4. Intriguingly, we also show that RIPK1 and RIPK3 kinase–dependent synthesis of IFN-β is markedly induced by avirulent strains of Gram-negative bacteria, Yersinia and Klebsiella, and less so by their wild-type counterparts. Overall, these observations identify unexpected roles for RIPK1 and RIPK3 kinases in the production of IFN-β during the host inflammatory responses to bacterial infection and suggest that the axis in which these kinases operate may represent a target for bacterial virulence factors.

Published

2017

25. Discovery of a First-in-Class Receptor Interacting Protein 1 (RIP1) Kinase Specific Clinical Candidate (GSK2982772) for the Treatment of Inflammatory Diseases

Author

Xiaoyang Dong, Anna Vossenkämper, Attiq Rahman, Viera Kasparcova, Robert Singhaus, Joshua N. Finger, Bryan W. King, Patrick M. Eidam, Michael Reilly, David D. Wisnoski, Scott B. Berger, John D. Lich, James Kang, Michael T. Ouellette, Lauren Dare, Philip A. Harris, Julie A. Cox, Nathan A. Miller, John Bertin, Michelle C. Schaeffer, Deepak Bandyopadhyay, Daohua Zhang, Alan R. Rendina, Clark A. Sehon, Sandra J. Hoffman, Peter J. Gough, Rachel D. Totoritis, Thomas T. MacDonald, Yunfeng Lan, Paris Ward, Barbara A. Swift, Robert W. Marquis, Lara Kathryn Leister, Rakesh Nagilla, Elizabeth J. Rivera, Helen H. Sun, Carol A. Capriotti, Nino Campobasso, Ruth Lehr, Christina S. Pao, and Jae U. Jeong

Subjects

0301 basic medicine, Swine, Necroptosis, Anti-Inflammatory Agents, Inflammation, Pharmacology, Mice, 03 medical and health sciences, Dogs, 0302 clinical medicine, Psoriasis, Drug Discovery, medicine, Animals, Humans, Potency, Protein Kinase Inhibitors, Tumor Necrosis Factor-alpha, Chemistry, Kinase, Haplorhini, Benzazepines, medicine.disease, Ulcerative colitis, Rats, Molecular Docking Simulation, 030104 developmental biology, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Rheumatoid arthritis, Cytokines, Swine, Miniature, Molecular Medicine, Colitis, Ulcerative, Rabbits, medicine.symptom, RECEPTOR-INTERACTING PROTEIN

Abstract

RIP1 regulates necroptosis and inflammation and may play an important role in contributing to a variety of human pathologies, including immune-mediated inflammatory diseases. Small-molecule inhibitors of RIP1 kinase that are suitable for advancement into the clinic have yet to be described. Herein, we report our lead optimization of a benzoxazepinone hit from a DNA-encoded library and the discovery and profile of clinical candidate GSK2982772 (compound 5), currently in phase 2a clinical studies for psoriasis, rheumatoid arthritis, and ulcerative colitis. Compound 5 potently binds to RIP1 with exquisite kinase specificity and has excellent activity in blocking many TNF-dependent cellular responses. Highlighting its potential as a novel anti-inflammatory agent, the inhibitor was also able to reduce spontaneous production of cytokines from human ulcerative colitis explants. The highly favorable physicochemical and ADMET properties of 5, combined with high potency, led to a predicted low oral dose in humans.

Published

2017

26. Discovery of a First-in-Class Receptor Interacting Protein 2 (RIP2) Kinase Specific Clinical Candidate, 2-((4-(Benzo[

Author

Pamela A, Haile, Linda N, Casillas, Bartholomew J, Votta, Gren Z, Wang, Adam K, Charnley, Xiaoyang, Dong, Michael J, Bury, Joseph J, Romano, John F, Mehlmann, Bryan W, King, Karl F, Erhard, Charles R, Hanning, David B, Lipshutz, Biva M, Desai, Carol A, Capriotti, Michelle C, Schaeffer, Scott B, Berger, Mukesh K, Mahajan, Michael A, Reilly, Rakesh, Nagilla, Elizabeth J, Rivera, Helen H, Sun, John K, Kenna, Allison M, Beal, Michael T, Ouellette, Mike, Kelly, Gillian, Stemp, Máire A, Convery, Anna, Vossenkämper, Thomas T, MacDonald, Peter J, Gough, John, Bertin, and Robert W, Marquis

Subjects

Male, Swine, Colitis, Phosphates, Molecular Docking Simulation, Rats, Sprague-Dawley, Mice, Dogs, Receptor-Interacting Protein Serine-Threonine Kinase 2, Drug Discovery, Quinazolines, Animals, Humans, Swine, Miniature, Benzothiazoles, Protein Kinase Inhibitors

Abstract

RIP2 kinase has been identified as a key signal transduction partner in the NOD2 pathway contributing to a variety of human pathologies, including immune-mediated inflammatory diseases. Small-molecule inhibitors of RIP2 kinase or its signaling partners on the NOD2 pathway that are suitable for advancement into the clinic have yet to be described. Herein, we report our discovery and profile of the prodrug clinical compound, inhibitor

Published

2019

27. Discovery of Pyrazolocarboxamides as Potent and Selective Receptor Interacting Protein 2 (RIP2) Kinase Inhibitors

Author

Arthur Shu, Yiqian Lian, Huijie Li, Curt Dale Haffner, Terry Vincent Hughes, Ami S. Lakdawala, Julie A. Cox, Pamela A. Haile, Constantine Kreatsoulas, Beth Anne Knapp-Reed, Lisa M. Shewchuk, David B. Lipshutz, John F. Mehlmann, Michael T. Ouellette, Christopher J Aquino, Mark Elban, Nicole Cathleen Goodwin, Huiqiang Zhou, Adam Kenneth Charnley, Bartholomew J. Votta, Robert W. Marquis, Joseph J. Romano, Linda N. Casillas, Peter J. Gough, Máire A. Convery, and John Bertin

Subjects

Bicyclic molecule, 010405 organic chemistry, Kinase, Chemistry, Organic Chemistry, Pyrazole, 01 natural sciences, Biochemistry, 0104 chemical sciences, RIPK2, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, NOD2, Drug Discovery, NOD1, Transferase, RECEPTOR-INTERACTING PROTEIN

Abstract

[Image: see text] Herein we report the discovery of pyrazolocarboxamides as novel, potent, and kinase selective inhibitors of receptor interacting protein 2 kinase (RIP2). Fragment based screening and design principles led to the identification of the inhibitor series, and X-ray crystallography was used to inform key structural changes. Through key substitutions about the N1 and C5 N positions on the pyrazole ring significant kinase selectivity and potency were achieved. Bridged bicyclic pyrazolocarboxamide 11 represents a selective and potent inhibitor of RIP2 and will allow for a more detailed investigation of RIP2 inhibition as a therapeutic target for autoinflammatory disorders.

Published

2019

28. Identification of a RIP1 Kinase Inhibitor Clinical Candidate (GSK3145095) for the Treatment of Pancreatic Cancer

Author

Joshua N. Finger, Michael T. Ouellette, Helen H. Sun, Robert W. Marquis, Viera Kasparcova, James H. Thorpe, Scott B. Berger, Philip A. Harris, Rakesh Nagilla, George Miller, Anirudh Chirala, James Kang, Elizabeth J. Rivera, John Bertin, Peter J. Gough, Mukesh K. Mahajan, Daohua Zhang, John D. Lich, Julie A. Cox, Wei Wang, Lara Kathryn Leister, Jill M. Marinis, Rachel D. Totoritis, Patrick M. Eidam, Michael Reilly, Jae U. Jeong, Dongling Wu, and Alan R. Rendina

Subjects

Programmed cell death, T cell, type III kinase inhibitors, pancreatic cancer, Inflammation, 01 natural sciences, Biochemistry, Pancreatic cancer, Drug Discovery, medicine, RIP1, 010405 organic chemistry, Kinase, business.industry, Organic Chemistry, Cancer, medicine.disease, Phenotype, Featured Letter, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, medicine.anatomical_structure, Cancer research, Adenocarcinoma, medicine.symptom, business

Abstract

RIP1 regulates cell death and inflammation and is believed to play an important role in contributing to a variety of human pathologies, including immune-mediated inflammatory diseases and cancer. While small-molecule inhibitors of RIP1 kinase have been advanced to the clinic for inflammatory diseases and CNS indications, RIP1 inhibitors for oncology indications have yet to be described. Herein we report on the discovery and profile of GSK3145095 (compound 6). Compound 6 potently binds to RIP1 with exquisite kinase specificity and has excellent activity in blocking RIP1 kinase-dependent cellular responses. Highlighting its potential as a novel cancer therapy, the inhibitor was also able to promote a tumor suppressive T cell phenotype in pancreatic adenocarcinoma organ cultures. Compound 6 is currently in phase 1 clinical studies for pancreatic adenocarcinoma and other selected solid tumors.

Published

2019

29. RIPK1 and Caspase-8 Ensure Chromosome Stability Independently of Their Role in Cell Death and Inflammation

Author

Peter J. Gough, David Robertson, Nieves Peltzer, Luca L. Fava, Holly Anderton, Manolis Pasparakis, Alexey I. Nesvizhskii, Katiuscia Bianchi, Marius Dannappel, Timo Glatter, Philip A. Harris, Tencho Tenev, Arnaud J. Legrand, Alexander Schmidt, Andreas Villunger, Gianmaria Liccardi, Pascal Meier, Manuel D. Haschka, John Silke, Alessandro Annibaldi, Maurice Darding, Hannah Schünke, Rebecca Feltham, John Bertin, and Laura Ramos Garcia

Subjects

Fas-Associated Death Domain Protein, CASP8 and FADD-Like Apoptosis Regulating Protein, Apoptosis, Cell Cycle Proteins, Inbred C57BL, caspase-8, Chromosome segregation, Mice, 0302 clinical medicine, Chromosome Segregation, Phosphorylation, Tissue homeostasis, Mice, Knockout, 0303 health sciences, Caspase 8, Protein-Serine-Threonine Kinases, 3. Good health, Cell biology, cell death, Receptor-Interacting Protein Serine-Threonine Kinases, Colonic Neoplasms, cell cycle, PLK1, HT29 Cells, Ripoptosome assembly, Signal Transduction, RIPK1, chromosomal instability, Necroptosis, Knockout, Ripoptosome, Mitosis, Protein Serine-Threonine Kinases, Biology, Article, 03 medical and health sciences, BUBR1, cancer, mitosis, ripoptosome, Aneuploidy, Animals, Fibroblasts, Humans, Inflammation, Mice, Inbred C57BL, Proto-Oncogene Proteins, Chromosomal Instability, Molecular Biology, Metaphase, 030304 developmental biology, Cell Biology, 030217 neurology & neurosurgery

Abstract

Summary Receptor-interacting protein kinase (RIPK) 1 functions as a key mediator of tissue homeostasis via formation of Caspase-8 activating ripoptosome complexes, positively and negatively regulating apoptosis, necroptosis, and inflammation. Here, we report an unanticipated cell-death- and inflammation-independent function of RIPK1 and Caspase-8, promoting faithful chromosome alignment in mitosis and thereby ensuring genome stability. We find that ripoptosome complexes progressively form as cells enter mitosis, peaking at metaphase and disassembling as cells exit mitosis. Genetic deletion and mitosis-specific inhibition of Ripk1 or Caspase-8 results in chromosome alignment defects independently of MLKL. We found that Polo-like kinase 1 (PLK1) is recruited into mitotic ripoptosomes, where PLK1’s activity is controlled via RIPK1-dependent recruitment and Caspase-8-mediated cleavage. A fine balance of ripoptosome assembly is required as deregulated ripoptosome activity modulates PLK1-dependent phosphorylation of downstream effectors, such as BUBR1. Our data suggest that ripoptosome-mediated regulation of PLK1 contributes to faithful chromosome segregation during mitosis., Graphical Abstract, Highlights • A RIPK1/FADD/Caspase-8/cFLIP complex (ripoptosome) forms during mitosis • The mitotic kinase PLK1 binds to RIPK1 and is recruited into mitotic ripoptosomes • PLK1 is cleaved by Caspase-8 in a RIPK1-dependent manner • Deletion and inhibition of RIPK1 or Caspase-8 lead to chromosomal instability, Liccardi et al. show that ripoptosome complexes assemble during physiological mitosis and regulate PLK1 activity via RIPK1-dependent recruitment and Caspase-8-mediated cleavage. These results reveal a direct role for RIPK1 and Caspase-8 in controlling chromosome segregation during mitosis.

Published

2019

30. MALT1 Protease Activation Triggers Acute Disruption of Endothelial Barrier Integrity via CYLD Cleavage

Author

Dong Hu, Peter C. Lucas, Emily M. Hess, Linda R. Klei, Katherine Oravecz-Wilson, Kevin Foley, Linda M. McAllister-Lucas, Vincent J. Concel, Robert L. Panek, Rachel E. Bridwell, Matthew Van Beek, Simon C. Watkins, Phillip C. Delekta, Peter J. Gough, Shufang Gu, Adrian T. Ting, Kelly M. Bailey, Danielle N. Alfano, and John Bertin

Subjects

0301 basic medicine, Microtubules, NF-κB, Mice, chemistry.chemical_compound, CARMA3, lcsh:QH301-705.5, NF-kappa B, thrombin, BCL10, Deubiquitinating Enzyme CYLD, I-kappa B Kinase, Neoplasm Proteins, 3. Good health, Cell biology, Endothelial stem cell, Cysteine Endopeptidases, Caspases, Paracellular transport, endothelial permeability, medicine.symptom, Protease activated receptor-1 (PAR1), Signal Transduction, medicine.drug, Primary Cell Culture, CYLD, G protein-coupled receptor (GPCR), Mice, Transgenic, Inflammation, Biology, Article, Permeability, General Biochemistry, Genetics and Molecular Biology, Cell Line, 03 medical and health sciences, Thrombin, Immune system, medicine, Animals, Receptor, PAR-1, CARD10, Bcl10, Endothelial Cells, Biological Transport, CARD Signaling Adaptor Proteins, MALT1, 030104 developmental biology, Gene Expression Regulation, lcsh:Biology (General), chemistry, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, MALT1 protease

Abstract

SummaryMicrovascular endothelial cells maintain a tight barrier to prevent passage of plasma and circulating immune cells into the extravascular tissue compartment, yet endothelial cells respond rapidly to vasoactive substances, including thrombin, allowing transient paracellular permeability. This response is a cornerstone of acute inflammation, but the mechanisms responsible are still incompletely understood. Here, we demonstrate that thrombin triggers MALT1 to proteolytically cleave cylindromatosis (CYLD). Fragmentation of CYLD results in microtubule disruption and a cascade of events leading to endothelial cell retraction and an acute permeability response. This finding reveals an unexpected role for the MALT1 protease, which previously has been viewed mostly as a driver of pro-inflammatory NF-κB signaling in lymphocytes. Thus, MALT1 not only promotes immune cell activation but also acutely regulates endothelial cell biology, actions that together facilitate tissue inflammation. Pharmacologic inhibition of MALT1 may therefore have synergistic impact by targeting multiple disparate steps in the overall inflammatory response.

Published

2016

31. RIPK3 Activates Parallel Pathways of MLKL-Driven Necroptosis and FADD-Mediated Apoptosis to Protect against Influenza A Virus

Author

Stuart C. Sealfon, Christopher P. Dillon, Swantje Liedmann, Douglas R. Green, Shalini Sharma, Roshan J. Thapa, Justin P. Ingram, Andrew Oberst, Carolina B. López, Peter J. Gough, Rachelle Kosoff, Edward S. Mocarski, Siddharth Balachandran, Boris M. Hartmann, Shoko Nogusa, Paul G. Thomas, William J. Kaiser, Katherine Verbist, Thomas H. Oguin, John Bertin, Oliver E. Sturm, and Diego A. Rodriguez

Subjects

0301 basic medicine, Fas-Associated Death Domain Protein, Necroptosis, Apoptosis, Biology, Microbiology, Article, Cell Line, Mice, Necrosis, 03 medical and health sciences, RIPK1, 0302 clinical medicine, Orthomyxoviridae Infections, Virology, Animals, Humans, FADD, Kinase activity, Mice, Knockout, Innate immune system, Kinase, Signal transducing adaptor protein, Epithelial Cells, Fibroblasts, Protein kinase R, Cell biology, Disease Models, Animal, 030104 developmental biology, Influenza A virus, Receptor-Interacting Protein Serine-Threonine Kinases, biology.protein, Parasitology, Protein Multimerization, Protein Kinases, 030215 immunology

Abstract

Influenza A virus (IAV) is a lytic virus in primary cultures of many cell types and in vivo. We report that the kinase RIPK3 is essential for IAV-induced lysis of mammalian fibroblasts and lung epithelial cells. Replicating IAV drives assembly of a RIPK3-containing complex that includes the kinase RIPK1, the pseudokinase MLKL, and the adaptor protein FADD, and forms independently of signaling by RNA-sensing innate immune receptors (RLRs, TLRs, PKR), or the cytokines type I interferons and TNF-α. Downstream of RIPK3, IAV activates parallel pathways of MLKL-driven necroptosis and FADD-mediated apoptosis, with the former reliant on RIPK3 kinase activity and neither on RIPK1 activity. Mice deficient in RIPK3 or doubly deficient in MLKL and FADD, but not MLKL alone, are more susceptible to IAV than their wild-type counterparts, revealing an important role for RIPK3-mediated apoptosis in antiviral immunity. Collectively, these results outline RIPK3-activated cytolytic mechanisms essential for controlling respiratory IAV infection.

Published

2016

32. RIPK1 and RIPK3 Kinases Promote Cell-Death-Independent Inflammation by Toll-like Receptor 4

Author

Michael J. Whalen, Michelle A. Kelliher, Peter J. Gough, Danish Saleh, John Bertin, Saumil Shah, Apostolos Polykratis, Siddharth Balachandran, Alexander Poltorak, Malek Najjar, Manolis Pasparakis, Albert K. Tai, Alexei Degterev, Matija Zelic, Shoko Nogusa, and Joshua N. Finger

Subjects

Lipopolysaccharides, 0301 basic medicine, MAPK/ERK pathway, Immunology, Mice, Necrosis, 03 medical and health sciences, RIPK1, Animals, Immunology and Allergy, Cells, Cultured, Caspase, Inflammation, Mice, Knockout, Caspase 8, Mice, Inbred BALB C, Toll-like receptor, Innate immune system, biology, Kinase, Macrophages, Immunity, Innate, Cell biology, Mice, Inbred C57BL, Adaptor Proteins, Vesicular Transport, 030104 developmental biology, Infectious Diseases, TRIF, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, biology.protein, Female, Signal transduction, Transcriptome, Signal Transduction

Abstract

Macrophages are a crucial component of the innate immune system in sensing pathogens and promoting local and systemic inflammation. RIPK1 and RIPK3 are homologous kinases, previously linked to activation of necroptotic death. In this study, we have described roles for these kinases as master regulators of pro-inflammatory gene expression induced by lipopolysaccharide, independent of their well-documented cell death functions. In primary macrophages, this regulation was elicited in the absence of caspase-8 activity, required the adaptor molecule TRIF, and proceeded in a cell autonomous manner. RIPK1 and RIPK3 kinases promoted sustained activation of Erk, cFos, and NF-κB, which were required for inflammatory changes. Utilizing genetic and pharmacologic tools, we showed that RIPK1 and RIPK3 account for acute inflammatory responses induced by lipopolysaccharide in vivo; notably, this regulation did not require exogenous manipulation of caspases. These findings identified a new pharmacologically accessible pathway that may be relevant to inflammatory pathologies.

Published

2016

33. RIPK1 and PGAM5 Control Leishmania Replication through Distinct Mechanisms

Author

Kendi Okuda, Valéria M. Borges, Sakthi Balaji, Aline Silva Barreto, Ricardo T. Gazzinelli, Francis Ka-Ming Chan, Roque P. Almeida, John Bertin, Marcelo T. Bozza, Nivea Farias Luz, and Peter J. Gough

Subjects

0301 basic medicine, Programmed cell death, Necroptosis, Interleukin-1beta, Immunology, Heme, Nitric Oxide, Article, Host-Parasite Interactions, Mice, 03 medical and health sciences, chemistry.chemical_compound, RIPK1, 0302 clinical medicine, Phosphoprotein Phosphatases, Animals, Humans, Immunology and Allergy, Kinase activity, Leishmaniasis, Leishmania, Cell Death, biology, Kinase, Effector, Macrophages, biology.organism_classification, Cell biology, 030104 developmental biology, chemistry, Receptor-Interacting Protein Serine-Threonine Kinases, Leishmaniasis, Visceral, 030215 immunology

Abstract

Leishmaniasis is an important parasitic disease found in the tropics and subtropics. Cutaneous and visceral leishmaniasis affect an estimated 1.5 million people worldwide. Despite its human health relevance, relatively little is known about the cell death pathways that control Leishmania replication in the host. Necroptosis is a recently identified form of cell death with potent antiviral effects. Receptor interacting protein kinase 1 (RIPK1) is a critical kinase that mediates necroptosis downstream of death receptors and TLRs. Heme, a product of hemoglobin catabolism during certain intracellular pathogen infections, is also a potent inducer of macrophage necroptosis. We found that human visceral leishmaniasis patients exhibit elevated serum levels of heme. Therefore, we examined the impact of heme and necroptosis on Leishmania replication. Indeed, heme potently inhibited Leishmania replication in bone marrow–derived macrophages. Moreover, we found that inhibition of RIPK1 kinase activity also enhanced parasite replication in the absence of heme. We further found that the mitochondrial phosphatase phosphoglycerate mutase family member 5 (PGAM5), a putative downstream effector of RIPK1, was also required for inhibition of Leishmania replication. In mouse infection, both PGAM5 and RIPK1 kinase activity are required for IL-1β expression in response to Leishmania. However, PGAM5, but not RIPK1 kinase activity, was directly responsible for Leishmania-induced IL-1β secretion and NO production in bone marrow–derived macrophages. Collectively, these results revealed that RIPK1 and PGAM5 function independently to exert optimal control of Leishmania replication in the host.

Published

2016

34. K45A mutation of RIPK1 results in poor necroptosis and cytokine signaling in macrophages, which impacts inflammatory responses in vivo

Author

John Bertin, Michael G. Schlossmacher, Subash Sad, Bojan Shutinoski, Dikchha Rijal, Norah A. Alturki, and P J Gough

Subjects

Salmonella typhimurium, 0301 basic medicine, Programmed cell death, Necroptosis, Apoptosis, Caspase 8, Inhibitor of Apoptosis Proteins, Mice, Necrosis, 03 medical and health sciences, RIPK1, Animals, Phosphorylation, Molecular Biology, Caspase, Inflammation, Original Paper, biology, Lysine, Macrophages, JNK Mitogen-Activated Protein Kinases, Cell Biology, Shock, Septic, Cell biology, Endotoxins, STAT1 Transcription Factor, 030104 developmental biology, Receptors, Tumor Necrosis Factor, Type I, Receptor-Interacting Protein Serine-Threonine Kinases, Mutation, Cancer research, biology.protein, Cytokines, Tumor necrosis factor alpha, Protein Multimerization, Signal transduction, Cell activation, Protein Kinases, Signal Transduction

Abstract

Receptor interacting protein kinase 1 (RIPK1) participates in several cell signaling complexes that promote cell activation and cell death. Stimulation of RIPK1 in the absence of caspase signaling induces regulated necrosis (necroptosis), which promotes an inflammatory response. Understanding of the mechanisms through which RIPK1 promotes inflammation has been unclear. Herein we have evaluated the impact of a K45A mutation of RIPK1 on necroptosis of macrophages and the activation of inflammatory response. We show that K45A mutation of RIPK1 results in attenuated necroptosis of macrophages in response to stimulation with LPS, TNFα and IFNβ in the absence of caspase signaling. Impairment in necroptosis correlated with poor phosphorylation of RIPK1, RIPK3 and reduced trimerization of MLKL. Furthermore, K45A mutation of RIPK1 resulted in poor STAT1 phosphorylation (at S727) and expression of RANTES and MIP-1α following TNF-R engagement in the absence of caspase activation. Our results further indicate that in the absence of stimulation by pathogen-associated molecular patterns (PAMPs), cellular inhibitors of apoptotic proteins (cIAPs) prevent the K45-dependent auto-phosphorylation of RIPK1, leading to resistance against necroptosis. Finally, RIPK1(K45A) mice displayed attenuated inflammatory response in vivo as they were significantly resistant against endotoxin shock, but highly susceptible against a challenge with Salmonella typhimurium. This correlated with reduced expression of IL-1β and ROS, and poor processing of caspase 8 by RIPK1(K45A) macrophages. Overall, these results indicate that K45 mediated kinase activity of RIPK1 is not only important for necroptosis but it also has a key role in promoting cytokine signaling and host response to inflammatory stimuli.

Published

2016

35. The Mitochondrial Phosphatase PGAM5 Is Dispensable for Necroptosis but Promotes Inflammasome Activation in Macrophages

Author

Carey L. O'Donnell, Raymond M. Welsh, Maria Jose de Rosa, Francis Ka-Ming Chan, Nivea Farias Luz, Peter J. Gough, Sakthi Balaji, Kenta Moriwaki, and John Bertin

Subjects

Male, 0301 basic medicine, Inflammasomes, Fas-Associated Death Domain Protein, Interleukin-1beta, Apoptosis, Mice, Phosphoprotein Phosphatases, Immunology and Allergy, FADD, MACROPHAGES, Cells, Cultured, Mice, Knockout, Caspase 8, biology, Caspase 1, Inflammasome, Mitochondria, Cell biology, DNA-Binding Proteins, Receptor-Interacting Protein Serine-Threonine Kinases, CIENCIAS NATURALES Y EXACTAS, PGAM5, Signal Transduction, medicine.drug, Programmed cell death, Otras Ciencias Biológicas, Necroptosis, Immunology, Article, Vesicular stomatitis Indiana virus, Ciencias Biológicas, 03 medical and health sciences, RIPK1, AIM2, NLR Family, Pyrin Domain-Containing 3 Protein, medicine, Animals, NECROPTOSIS, Inflammation, Macrophages, Dendritic Cells, Phosphoric Monoester Hydrolases, Mice, Inbred C57BL, 030104 developmental biology, biology.protein, Carrier Proteins, Reactive Oxygen Species

Abstract

The cytokine IL-1β is intimately linked to many pathological inflammatory conditions. Mature IL-1β secretion requires cleavage by the inflammasome. Recent evidence indicates that many cell death signal adaptors have regulatory roles in inflammasome activity. These include the apoptosis inducers FADD and caspase 8, and the necroptosis kinases receptor interacting protein kinase 1 (RIPK1) and RIPK3. PGAM5 is a mitochondrial phosphatase that has been reported to function downstream of RIPK3 to promote necroptosis and IL-1β secretion. To interrogate the biological function of PGAM5, we generated Pgam5−/− mice. We found that Pgam5−/− mice were smaller compared with wild type littermates, and male Pgam5−/− mice were born at sub-Mendelian ratio. Despite these growth and survival defects, Pgam5−/− cells responded normally to multiple inducers of apoptosis and necroptosis. Rather, we found that PGAM5 is critical for IL-1β secretion in response to NLRP3 and AIM2 inflammasome agonists. Moreover, vesicular stomatosis virus–induced IL-1β secretion was impaired in Pgam5−/− bone marrow–derived macrophages, but not in Ripk3−/− bone marrow–derived dendritic cells, indicating that PGAM5 functions independent of RIPK3 to promote inflammasome activation. Mechanistically, PGAM5 promotes ASC polymerization, maintenance of mitochondrial integrity, and optimal reactive oxygen species production in response to inflammasome signals. Hence PGAM5 is a novel regulator of inflammasome and caspase 1 activity that functions independently of RIPK3. Fil: Moriwaki, Kenta. University of Massachussets; Estados Unidos Fil: Farias Luz, Nivea. Universidade Federal da Bahia; Brasil. University of Massachussets; Estados Unidos Fil: Balaji, Sakthi. University of Massachussets; Estados Unidos Fil: de Rosa, Maria Jose. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Bahía Blanca. Instituto de Investigaciones Bioquímicas de Bahía Blanca. Universidad Nacional del Sur. Instituto de Investigaciones Bioquímicas de Bahía Blanca; Argentina. Universidad Nacional del Sur. Departamento de Biología, Bioquímica y Farmacia; Argentina Fil: O'Donnell, Carey L.. University of Massachussets; Estados Unidos Fil: Gough, Peter J.. Glaxo Smith Kline; Estados Unidos Fil: Bertin, John. Glaxo Smith Kline; Estados Unidos Fil: Welsh, Raymond M.. University of Massachussets; Estados Unidos Fil: Chan, Francis Ka Ming. University of Massachussets; Estados Unidos

Published

2016

36. Publisher Correction: RIPK1 gene variants associate with obesity in humans and can be therapeutically silenced to reduce obesity in mice

Author

Ludovic Boytard, Marcus Alvarez, Joshua W. Kandiah, Kirsi H. Pietiläinen, Päivi Pajukanta, Mary-Ellen Harper, Denuja Karunakaran, Calvin Pan, Peter Liu, Sébastien Soubeyrand, My-Anh Nguyen, Aldons J. Lusis, Hailey Wyatt, Richard G. Lee, Adil Rasheed, Barbara C. Vanderhyden, Paulina Lau, Scott B. Berger, Peter J. Gough, John Bertin, Anne-Claire Duchez, Markku Laakso, David Smyth, Michele Geoffrion, Katey J. Rayner, Bhama Ramkhelawon, Ruth McPherson, David P. Cook, Adam W. Turner, and Majid Nikpay

Subjects

business.industry, RIPK1 gene, Physiology (medical), Endocrinology, Diabetes and Metabolism, Internal Medicine, MEDLINE, Medicine, Cell Biology, business, Bioinformatics, medicine.disease, Obesity

Published

2020

37. Correction to Identification of Quinoline-Based RIP2 Kinase Inhibitors with an Improved Therapeutic Index to the hERG Ion Channel

Author

Elizabeth J. Rivera, Brian Donovan, Ami S. Lakdawala, Nikolay V. Plotnikov, Xiaoyang Dong, Barry S. Brown, Robert Singhaus, Khuram W. Chaudhary, Rachel D. Totoritis, Adam Kenneth Charnley, Michael Reilly, Terry Vincent Hughes, Joseph J. Romano, Pamela A. Haile, Robert W. Marquis, Michael Jonathan Bury, John F. Mehlmann, Gren Z. Wang, Rakesh Nagilla, Bartholomew J. Votta, Barbara A. Swift, Linda N. Casillas, Demartino Michael P, Peter J. Gough, Mukesh K. Mahajan, Carol A. Capriotti, Biva M. Desai, Scott B. Berger, Carol LePage, Helen H. Sun, David B. Lipshutz, John Bertin, Máire A. Convery, Chaya Duraiswami, and Michael T. Ouellette

Subjects

biology, Kinase, Organic Chemistry, Quinoline, hERG, Pharmacology, Biochemistry, chemistry.chemical_compound, Therapeutic index, chemistry, Drug Discovery, biology.protein, Identification (biology), Ion channel

Published

2020

38. Elevated A20 promotes TNF-induced and RIPK1-dependent intestinal epithelial cell death

Author

Soumita Das, John Bertin, John T. Chang, Ricard Garcia-Carbonell, Michelle A. Kelliher, Michael Karin, David L. Boone, Roman Sasik, Lisa Abernathy Close, Ju Youn Kim, P J Gough, Philip A. Harris, Samuel B. Ho, William J. Sandborn, Peter B. Ernst, Thomas L. Wong, Brigid S. Boland, Jerry Wong, and Monica Guma

Subjects

0301 basic medicine, RIPK1, 1.1 Normal biological development and functioning, Ripoptosome, Mice, Transgenic, Apoptosis, Crohn's Disease, Autoimmune Disease, Transgenic, Oral and gastrointestinal, Epithelial Damage, Mice, 03 medical and health sciences, Intestinal mucosa, inflammatory bowel disease, Underpinning research, immune system diseases, hemic and lymphatic diseases, Animals, Humans, 2.1 Biological and endogenous factors, Intestinal Mucosa, Aetiology, Tumor Necrosis Factor alpha-Induced Protein 3, Caspase 8, Multidisciplinary, Tumor Necrosis Factor-alpha, Caspase 3, Chemistry, NF-kappa B, Inflammatory Bowel Diseases, Intestinal epithelium, Cell biology, A20, 030104 developmental biology, PNAS Plus, Receptor-Interacting Protein Serine-Threonine Kinases, intestinal epithelial cells, Tumor necrosis factor alpha, Protein Multimerization, Digestive Diseases

Abstract

Intestinal epithelial cell (IEC) death is a common feature of inflammatory bowel disease (IBD) that triggers inflammation by compromising barrier integrity. In many patients with IBD, epithelial damage and inflammation are TNF-dependent. Elevated TNF production in IBD is accompanied by increased expression of the TNFAIP3 gene, which encodes A20, a negative feedback regulator of NF-κB. A20 in intestinal epithelium from patients with IBD coincided with the presence of cleaved caspase-3, and A20 transgenic (Tg) mice, in which A20 is expressed from an IEC-specific promoter, were highly susceptible to TNF-induced IEC death, intestinal damage, and shock. A20-expressing intestinal organoids were also susceptible to TNF-induced death, demonstrating that enhanced TNF-induced apoptosis was a cell-autonomous property of A20. This effect was dependent on Receptor Interacting Protein Kinase 1 (RIPK1) activity, and A20 was found to associate with the Ripoptosome complex, potentiating its ability to activate caspase-8. A20-potentiated RIPK1-dependent apoptosis did not require the A20 deubiquitinase (DUB) domain and zinc finger 4 (ZnF4), which mediate NF-κB inhibition in fibroblasts, but was strictly dependent on ZnF7 and A20 dimerization. We suggest that A20 dimers bind linear ubiquitin to stabilize the Ripoptosome and potentiate its apoptosis-inducing activity.

Published

2018

39. Use of RIP1 Kinase Small-Molecule Inhibitors in Studying Necroptosis

Author

Allison M, Beal, John, Bertin, and Michael A, Reilly

Subjects

Mice, Inbred C57BL, Small Molecule Libraries, Mice, Necrosis, Fibrosarcoma, Macrophages, GTPase-Activating Proteins, Tumor Cells, Cultured, Animals, Apoptosis, Tissue Distribution, Signal Transduction

Abstract

RIP1 kinase plays a key role in regulating signaling pathways downstream of a number of innate immune receptors such as TNFRI and TLRs. The discovery of Necrostatin-1 (Nec-1) as a small-molecule inhibitor of RIP1 kinase has been very instrumental in defining the necroptotic and other signalling pathways regulated by RIP1, but certain characteristics of Nec-1 limits its utility in experimental systems. Next generation RIP1 kinase inhibitors have been identified and the use of these tool inhibitors along with Nec-1 has revealed that RIP1 is emerging as a key driver of inflammation and tissue injury in the pathogenesis of various diseases. Further studying the role of RIP1 to carefully unravel the complex biology requires the selection of the correct tool small-molecule inhibitors. In addition, it is important to consider the proper application of current tool inhibitors and understand the current limitiations. Here we will discuss key parameters that need to be considered when selecting and applying tool inhibitors to novel biological assays and systems. General protocols to explore the in vitro and in vivo potency, cellular selectivity, and pharmacokinetic properties of current small-molecule inhibitors of RIP1 kinase are provided.

Published

2018

40. Identification of Quinoline-Based RIP2 Kinase Inhibitors with an Improved Therapeutic Index to the hERG Ion Channel

Author

Rachel D. Totoritis, Robert Singhaus, Brian Donovan, Nikolay V. Plotnikov, John F. Mehlmann, Terry Vincent Hughes, Michael Jonathan Bury, Pamela A. Haile, Khuram W. Chaudhary, Gren Z. Wang, Peter J. Gough, Biva M. Desai, Michael T. Ouellette, Michael Reilly, Mukesh K. Mahajan, Barry S. Brown, Scott B. Berger, Xiaoyang Dong, Carol A. Capriotti, Carol LePage, Bartholomew J. Votta, Helen H. Sun, David B. Lipshutz, John Bertin, Joseph J. Romano, Adam Kenneth Charnley, Ami S. Lakdawala, Robert W. Marquis, Barbara A. Swift, Rakesh Nagilla, Máire A. Convery, Demartino Michael P, Elizabeth J. Rivera, and Linda N. Casillas

Subjects

0301 basic medicine, biology, 010405 organic chemistry, Chemistry, Kinase, Organic Chemistry, hERG, Pharmacology, 01 natural sciences, Biochemistry, 0104 chemical sciences, Biological pathway, 03 medical and health sciences, 030104 developmental biology, Therapeutic index, In vivo, Drug Discovery, biology.protein, IC50, Ex vivo, Ion channel

Abstract

[Image: see text] RIP2 kinase was recently identified as a therapeutic target for a variety of autoimmune diseases. We have reported previously a selective 4-aminoquinoline-based RIP2 inhibitor GSK583 and demonstrated its effectiveness in blocking downstream NOD2 signaling in cellular models, rodent in vivo models, and human ex vivo disease models. While this tool compound was valuable in validating the biological pathway, it suffered from activity at the hERG ion channel and a poor PK/PD profile thereby limiting progression of this analog. Herein, we detail our efforts to improve both this off-target liability as well as the PK/PD profile of this series of inhibitors through modulation of lipophilicity and strengthening hinge binding ability. These efforts have led to inhibitor 7, which possesses high binding affinity for the ATP pocket of RIP2 (IC(50) = 1 nM) and inhibition of downstream cytokine production in human whole blood (IC(50) = 10 nM) with reduced hERG activity (14 μM).

Published

2018

41. Caspase-8 Collaborates with Caspase-11 to Drive Tissue Damage and Execution of Endotoxic Shock

Author

Shunsuke Otani, Eileen M. Burd, Scott B. Berger, Craig M. Coopersmith, Kristal M. Maner-Smith, John Bertin, Sandra J. Hoffman, Alexandra DeLaney, Gregory K. Tharp, Michelle C. Schaeffer, Linda Roback, Carol A. Capriotti, Peter J. Gough, Cedrick Young, Steven E. Bosinger, Zhe Liang, Nelson C. DiPaolo, Edward S. Mocarski, Dmitry M. Shayakhmetov, Igor E. Brodsky, Yanjun Feng, Pratyusha Mandal, John D. Lyons, and Eric A. Ortlund

Subjects

0301 basic medicine, Lipopolysaccharides, Male, Immunology, Apoptosis, Caspase-11, Caspase 8, Article, Proinflammatory cytokine, 03 medical and health sciences, RIPK1, 0302 clinical medicine, Intestine, Small, Immunology and Allergy, Animals, Kinase activity, Caspase, Cells, Cultured, Escherichia coli Infections, Inflammation, Mice, Knockout, biology, Tumor Necrosis Factor-alpha, Intracellular Signaling Peptides and Proteins, Interferon-beta, Phosphate-Binding Proteins, Shock, Septic, Caspases, Initiator, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, Caspases, Receptor-Interacting Protein Serine-Threonine Kinases, biology.protein, Tumor necrosis factor alpha, Female, Interferon Regulatory Factor-3, Apoptosis Regulatory Proteins, Spleen, Signal Transduction

Abstract

Summary The execution of shock following high dose E. coli lipopolysaccharide (LPS) or bacterial sepsis in mice required pro-apoptotic caspase-8 in addition to pro-pyroptotic caspase-11 and gasdermin D. Hematopoietic cells produced MyD88- and TRIF-dependent inflammatory cytokines sufficient to initiate shock without any contribution from caspase-8 or caspase-11. Both proteases had to be present to support tumor necrosis factor- and interferon-β-dependent tissue injury first observed in the small intestine and later in spleen and thymus. Caspase-11 enhanced the activation of caspase-8 and extrinsic cell death machinery within the lower small intestine. Neither caspase-8 nor caspase-11 was individually sufficient for shock. Both caspases collaborated to amplify inflammatory signals associated with tissue damage. Therefore, combined pyroptotic and apoptotic signaling mediated endotoxemia independently of RIPK1 kinase activity and RIPK3 function. These observations bring to light the relevance of tissue compartmentalization to disease processes in vivo where cytokines act in parallel to execute diverse cell death pathways.

Published

2018

42. Design of amidobenzimidazole STING receptor agonists with systemic activity

Author

Joshi M. Ramanjulu, G. Scott Pesiridis, Jingsong Yang, Nestor Concha, Robert Singhaus, Shu-Yun Zhang, Jean-Luc Tran, Patrick Moore, Stephanie Lehmann, H. Christian Eberl, Marcel Muelbaier, Jessica L. Schneck, Jim Clemens, Michael Adam, John Mehlmann, Joseph Romano, Angel Morales, James Kang, Lara Leister, Todd L. Graybill, Adam K. Charnley, Guosen Ye, Neysa Nevins, Kamelia Behnia, Amaya I. Wolf, Viera Kasparcova, Kelvin Nurse, Liping Wang, Ana C. Puhl, Yue Li, Michael Klein, Christopher B. Hopson, Jeffrey Guss, Marcus Bantscheff, Giovanna Bergamini, Michael A. Reilly, Yiqian Lian, Kevin J. Duffy, Jerry Adams, Kevin P. Foley, Peter J. Gough, Robert W. Marquis, James Smothers, Axel Hoos, and John Bertin

Subjects

0301 basic medicine, Agonist, Models, Molecular, medicine.drug_class, Endogeny, Ligands, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Animals, Humans, Receptor, Multidisciplinary, Innate immune system, business.industry, Endoplasmic reticulum, Cancer, Membrane Proteins, medicine.disease, eye diseases, Sting, 030104 developmental biology, 030220 oncology & carcinogenesis, Stimulator of interferon genes, Drug Design, Colonic Neoplasms, Cancer research, Benzimidazoles, Nucleotides, Cyclic, business

Abstract

Stimulator of interferon genes (STING) is a receptor in the endoplasmic reticulum that propagates innate immune sensing of cytosolic pathogen-derived and self DNA1. The development of compounds that modulate STING has recently been the focus of intense research for the treatment of cancer and infectious diseases and as vaccine adjuvants2. To our knowledge, current efforts are focused on the development of modified cyclic dinucleotides that mimic the endogenous STING ligand cGAMP; these have progressed into clinical trials in patients with solid accessible tumours amenable to intratumoral delivery3. Here we report the discovery of a small molecule STING agonist that is not a cyclic dinucleotide and is systemically efficacious for treating tumours in mice. We developed a linking strategy to synergize the effect of two symmetry-related amidobenzimidazole (ABZI)-based compounds to create linked ABZIs (diABZIs) with enhanced binding to STING and cellular function. Intravenous administration of a diABZI STING agonist to immunocompetent mice with established syngeneic colon tumours elicited strong anti-tumour activity, with complete and lasting regression of tumours. Our findings represent a milestone in the rapidly growing field of immune-modifying cancer therapies.

Published

2018

43. Pathogen blockade of TAK1 triggers caspase-8-dependent cleavage of gasdermin D and cell death

Author

Bettina L. Lee, Michelle A. Kelliher, Shiyu Xia, Katherine A. Fitzgerald, Peter J. Gough, Pontus Orning, Jon D. Goguen, Egil Lien, Nobuhiko Kayagaki, Alexandria Brooks, Megan K. Proulx, Dan Weng, Hao Wu, Zachary Best, Kristian K. Starheim, Scott B. Berger, Dmitry Ratner, and John Bertin

Subjects

0301 basic medicine, Programmed cell death, Inflammasomes, Regulator, IκB kinase, Cleavage (embryo), Caspase 8, Article, 03 medical and health sciences, RIPK1, Mice, 0302 clinical medicine, Bacterial Proteins, NLR Family, Pyrin Domain-Containing 3 Protein, Animals, Humans, Plague, Multidisciplinary, Cell Death, Chemistry, Effector, Pyroptosis, Intracellular Signaling Peptides and Proteins, Phosphate-Binding Proteins, MAP Kinase Kinase Kinases, Cell biology, I-kappa B Kinase, Mice, Inbred C57BL, 030104 developmental biology, 030220 oncology & carcinogenesis, Host-Pathogen Interactions, Proteolysis, Apoptosis Regulatory Proteins

Abstract

Limited proteolysis of gasdermin D (GSDMD) generates an N-terminal pore-forming fragment that controls pyroptosis in macrophages. GSDMD is processed via inflammasome-activated caspase-1 or -11. It is currently unknown whether macrophage GSDMD can be processed by other mechanisms. Here, we describe an additional pathway controlling GSDMD processing. The inhibition of TAK1 or IκB kinase (IKK) by the Yersinia effector protein YopJ elicits RIPK1- and caspase-8–dependent cleavage of GSDMD, which subsequently results in cell death. GSDMD processing also contributes to the NLRP3 inflammasome–dependent release of interleukin-1β (IL-1β). Thus, caspase-8 acts as a regulator of GSDMD-driven cell death. Furthermore, this study establishes the importance of TAK1 and IKK activity in the control of GSDMD cleavage and cytotoxicity.

Published

2018

44. LUBAC prevents lethal dermatitis by inhibiting cell death induced by TNF, TRAIL and CD95L

Author

Ayse U. Akarca, Sebastian Kupka, Andreas Strasser, Nieves Peltzer, Eva Rieser, Tobias L. Haas, Torsten Hartwig, Lucia Taraborrelli, Manolis Pasparakis, Martin Leverkus, Philippe Bouillet, Peter Draber, John Silke, Maurice Darding, Henning Walczak, Peter J. Gough, Teresa Marafioti, Aida Sarr, Antonella Montinaro, and John Bertin

Subjects

Genetics and Molecular Biology (all), 0301 basic medicine, Keratinocytes, Programmed cell death, Fas Ligand Protein, Science, Necroptosis, Ubiquitin-Protein Ligases, General Physics and Astronomy, Dermatitis, Mice, Transgenic, Caspase 8, Biochemistry, General Biochemistry, Genetics and Molecular Biology, TNF-Related Apoptosis-Inducing Ligand, Physics and Astronomy (all), 03 medical and health sciences, RIPK1, Medicine, Animals, Kinase activity, lcsh:Science, Receptor, Cells, Cultured, Skin, Mice, Knockout, Settore MED/06 - ONCOLOGIA MEDICA, Multidisciplinary, Cell Death, business.industry, Tumor Necrosis Factor-alpha, Chemistry (all), Intracellular Signaling Peptides and Proteins, General Chemistry, 3. Good health, Mice, Inbred C57BL, 030104 developmental biology, Animals, Newborn, Apoptosis, Cancer research, lcsh:Q, Tumor necrosis factor alpha, Biochemistry, Genetics and Molecular Biology (all), business, Carrier Proteins

Abstract

The linear ubiquitin chain assembly complex (LUBAC), composed of HOIP, HOIL-1 and SHARPIN, is required for optimal TNF-mediated gene activation and to prevent cell death induced by TNF. Here, we demonstrate that keratinocyte-specific deletion of HOIP or HOIL-1 (E-KO) results in severe dermatitis causing postnatal lethality. We provide genetic and pharmacological evidence that the postnatal lethal dermatitis in HoipE-KO and Hoil-1E-KO mice is caused by TNFR1-induced, caspase-8-mediated apoptosis that occurs independently of the kinase activity of RIPK1. In the absence of TNFR1, however, dermatitis develops in adulthood, triggered by RIPK1-kinase-activity-dependent apoptosis and necroptosis. Strikingly, TRAIL or CD95L can redundantly induce this disease-causing cell death, as combined loss of their respective receptors is required to prevent TNFR1-independent dermatitis. These findings may have implications for the treatment of patients with mutations that perturb linear ubiquitination and potentially also for patients with inflammation-associated disorders that are refractory to inhibition of TNF alone.

Published

2018

45. S100A12 and S100A8/9 proteins are biomarkers of articular disease activity in Blau syndrome

Author

Sebastiaan J. Vastert, Brigitte Bader-Meunier, Catherine Guly, Consuelo Modesto, Christine Pajot, Miroslav Harjacek, Carlos D. Rose, Akaluck Thatayatikom, Lin Wang, Caroline Thomee, Bart Votta, Jordi Anton, Kevin Foley, Gaëlle Chédeville, Philippe Brissaud, Rolando Cimaz, John Bertin, Antonio Naranjo Hernández, Carine Wouters, Friederike Mackensen, Jorge Julián Fernández-Martín, Eric Hachulla, Athimalaipet V Ramanan, and Rosa Merino

Subjects

0301 basic medicine, medicine.medical_specialty, business.industry, Arthritis, Blau syndrome, medicine.disease, Gastroenterology, Blood proteins, Rheumatology, S100A8, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Internal medicine, Cohort, medicine, Pharmacology (medical), business, S100 proteins, Uveitis, 030215 immunology, Cohort study

Abstract

OBJECTIVE: To identify biomarkers of articular and ocular disease activity in patients with Blau syndrome (BS). METHODS: Multiplex plasma protein arrays were performed in five BS patients and eight normal healthy volunteers (NHVs). Plasma S100A12 and S100A8/9 were subsequently measured by ELISA at baseline and 1-year follow-up in all patients from a prospective multicentre cohort study. CRP was measured using Meso Scale Discovery immunoassay. Active joint counts, standardization uveitis nomenclature for anterior uveitis cells and vitreous haze by Nussenblatt scale were the clinical parameters. RESULTS: Multiplex Luminex arrays identified S100A12 as the most significantly elevated protein in five selected BS vs eight NHVs and this was confirmed by ELISA on additional samples from the same five BS patients. In the patient cohort, S100A12 (n = 39) and S100A8/9 (n = 33) were significantly higher compared with NHVs (n = 44 for S100A12, n = 40 for S100A8/9) (P = 0.0000004 and P = 0.0003, respectively). Positive correlations between active joint counts and S100 levels were significant for S100A12 (P = 0.0008) and S100A8/9 (P = 0.015). CRP levels did not correlate with active joint count. Subgroup analysis showed significant association of S100 proteins with active arthritis (S100A12 P = 0.01, S100A8/9 P = 0.008). Active uveitis was not associated with increased S100 levels. CONCLUSION: S100 proteins are biomarkers of articular disease activity in BS and potential outcome measures in future clinical trials. As secreted neutrophil and macrophage products, S100 proteins may reflect the burden of granulomatous tissue in BS.

Published

2018

46. Use of RIP1 Kinase Small-Molecule Inhibitors in Studying Necroptosis

Author

Allison M. Beal, Michael Reilly, and John Bertin

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Innate immune system, Kinase, In vivo, Necroptosis, Computational biology, Biology, Signal transduction, Receptor, Small molecule, In vitro

Abstract

RIP1 kinase plays a key role in regulating signaling pathways downstream of a number of innate immune receptors such as TNFRI and TLRs. The discovery of Necrostatin-1 (Nec-1) as a small-molecule inhibitor of RIP1 kinase has been very instrumental in defining the necroptotic and other signalling pathways regulated by RIP1, but certain characteristics of Nec-1 limits its utility in experimental systems. Next generation RIP1 kinase inhibitors have been identified and the use of these tool inhibitors along with Nec-1 has revealed that RIP1 is emerging as a key driver of inflammation and tissue injury in the pathogenesis of various diseases. Further studying the role of RIP1 to carefully unravel the complex biology requires the selection of the correct tool small-molecule inhibitors. In addition, it is important to consider the proper application of current tool inhibitors and understand the current limitiations. Here we will discuss key parameters that need to be considered when selecting and applying tool inhibitors to novel biological assays and systems. General protocols to explore the in vitro and in vivo potency, cellular selectivity, and pharmacokinetic properties of current small-molecule inhibitors of RIP1 kinase are provided.

Published

2018

47. Application of DMPK toolbox in predicting human pharmacokinetics for back-up RIP1 inhibitors: Learnings from GSK2982772 in clinic

Author

Mukesh K. Mahajan, David Zhang, Jill M. Marinis, Robert W. Marquis, Steven Thomas, Michael Reilly, Lauren E. Richards-Peterson, Phil Harris, Debbie Tompson, Scott B. Berger, and John Bertin

Subjects

Pharmacology, Pharmacokinetics, business.industry, Pharmaceutical Science, Medicine, Pharmacology (medical), Computational biology, business, Toolbox

Published

2019

48. Structure Guided Design of Potent and Selective Ponatinib-Based Hybrid Inhibitors for RIPK1

Author

Saumil Shah, Shoko Nogusa, John Bertin, Gregory D. Cuny, Jenny L. Maki, Chalada Suebsuwong, Junying Yuan, Peter J. Gough, Malek Najjar, Soumya S. Ray, Roshan J. Thapa, Danish Saleh, Siddharth Balachandran, and Alexei Degterev

Subjects

Programmed cell death, Molecular Sequence Data, Allosteric regulation, Antineoplastic Agents, Pharmacology, Biology, Jurkat cells, Article, General Biochemistry, Genetics and Molecular Biology, Substrate Specificity, Jurkat Cells, Mice, chemistry.chemical_compound, RIPK1, In vivo, Animals, Humans, Amino Acid Sequence, lcsh:QH301-705.5, Protein Kinase Inhibitors, Ponatinib, HEK 293 cells, Imidazoles, Mice, Inbred C57BL, Molecular Docking Simulation, Pyridazines, HEK293 Cells, lcsh:Biology (General), chemistry, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, Female, Tumor necrosis factor alpha, Protein Binding

Abstract

SummaryRIPK1 and RIPK3, two closely related RIPK family members, have emerged as important regulators of pathologic cell death and inflammation. In the current work, we report that the Bcr-Abl inhibitor and anti-leukemia agent ponatinib is also a first-in-class dual inhibitor of RIPK1 and RIPK3. Ponatinib potently inhibited multiple paradigms of RIPK1- and RIPK3-dependent cell death and inflammatory tumor necrosis factor alpha (TNF-α) gene transcription. We further describe design strategies that utilize the ponatinib scaffold to develop two classes of inhibitors (CS and PN series), each with greatly improved selectivity for RIPK1. In particular, we detail the development of PN10, a highly potent and selective “hybrid” RIPK1 inhibitor, capturing the best properties of two different allosteric RIPK1 inhibitors, ponatinib and necrostatin-1. Finally, we show that RIPK1 inhibitors from both classes are powerful blockers of TNF-induced injury in vivo. Altogether, these findings outline promising candidate molecules and design approaches for targeting RIPK1- and RIPK3-driven inflammatory pathologies.

Published

2015

49. A RIPK3–Caspase 8 Complex Mediates Atypical Pro–IL-1β Processing

Author

Kenta Moriwaki, John Bertin, Francis Ka-Ming Chan, and Peter J. Gough

Subjects

Necroptosis, Blotting, Western, Interleukin-1beta, Immunology, Bone Marrow Cells, Enzyme-Linked Immunosorbent Assay, Transfection, Caspase 8, Article, Mice, RIPK1, Animals, Immunoprecipitation, Immunology and Allergy, Gene Knock-In Techniques, FADD, Caspase, Inflammation, Mice, Knockout, biology, NLRP1, Chemistry, Dendritic Cells, Cell biology, Enzyme Activation, Receptor-Interacting Protein Serine-Threonine Kinases, Death-inducing signaling complex, biology.protein, Caspase 10

Abstract

Caspase 8, the initiator caspase for death receptor–induced apoptosis, functions as a negative regulator of receptor interacting protein kinase 3 (RIPK3), an essential factor for TNF-, TLR3-, and TLR4-induced necroptosis. In certain situations, caspase 8 can also participate in pro–IL-1β processing. However, the biochemical complex that mediates caspase 8–mediated processing is not defined. In this study, we show that RIPK3 is crucial for caspase 1– and caspase 8–mediated pro–IL-1β and pro–IL-18 processing in bone marrow–derived dendritic cells (BMDCs) in response to LPS stimulation. Caspase 8–mediated pro–IL-1β processing requires intact RIPK1, RIPK3, TRIF, and FADD. In response to LPS, a complex that contains RIPK1, RIPK3, FADD, and caspase 8 is formed. Surprisingly, RIPK3-specific kinase inhibitors strongly enhanced caspase 8 activation and pro–IL-1β processing in LPS-stimulated BMDCs. However, studies in BMDCs expressing the kinase-inactive RIPK3-K51A mutant or RIPK1-K45A mutant showed that the kinase activity of neither RIPK1 nor RIPK3 is required for LPS-induced caspase 8 activation and IL-1β secretion. Hence, RIPK3 is an unexpected positive regulator of caspase 8 activity that promotes IL-1β maturation in BMDCs.

Published

2015

50. MLKL Requires the Inositol Phosphate Code to Execute Necroptosis

Author

Bradley P. Clarke, Nathaniel W. Brown, Hongyan Guo, Edward S. Mocarski, William J. Kaiser, Jan E. Carette, Dan E. McNamara, Tudor Moldoveanu, John D. York, Jonathan Diep, Christy R. Grace, Dorothea Fiedler, Jennifer Yinuo Cao, Scott J. Dixon, Andrew T. Hale, Peter J. Gough, John Bertin, and Cole M. Dovey

Subjects

0301 basic medicine, Programmed cell death, Necroptosis, Inositol Phosphates, Herpesvirus 1, Human, Biology, Jurkat cells, Gene Expression Regulation, Enzymologic, Article, 03 medical and health sciences, Jurkat Cells, Humans, Kinase activity, Phosphorylation, Inositol phosphate, Molecular Biology, chemistry.chemical_classification, Binding Sites, Cell Death, Kinase, Tumor Necrosis Factor-alpha, Cell Biology, Cell biology, Gene Expression Regulation, Neoplastic, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, chemistry, Receptor-Interacting Protein Serine-Threonine Kinases, Colonic Neoplasms, Mutation, Signal transduction, HT29 Cells, Protein Kinases, Signal Transduction

Abstract

Necroptosis is an important form of lytic cell death triggered by injury and infection, but whether mixed lineage kinase domain-like (MLKL) is sufficient to execute this pathway is unknown. In a genetic selection for human cell mutants defective for MLKL-dependent necroptosis, we identified mutations in IPMK and ITPK1, which encode inositol phosphate (IP) kinases that regulate the IP code of soluble molecules. We show that IP kinases are essential for necroptosis triggered by death receptor activation, herpesvirus infection, or a pro-necrotic MLKL mutant. In IP kinase mutant cells, MLKL failed to oligomerize and localize to membranes despite proper receptor-interacting protein kinase-3 (RIPK3)-dependent phosphorylation. We demonstrate that necroptosis requires IP-specific kinase activity and that a highly phosphorylated product, but not a lowly phosphorylated precursor, potently displaces the MLKL auto-inhibitory brace region. These observations reveal control of MLKL-mediated necroptosis by a metabolite and identify a key molecular mechanism underlying regulated cell death.

Published

2017