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1. ADAR1 averts fatal type I interferon induction by ZBP1

Author

Huipeng Jiao, Laurens Wachsmuth, Simone Wolf, Juliane Lohmann, Masahiro Nagata, Göksu Gökberk Kaya, Nikos Oikonomou, Vangelis Kondylis, Manuel Rogg, Martin Diebold, Simon E. Tröder, Branko Zevnik, Marco Prinz, Christoph Schell, George R. Young, George Kassiotis, and Manolis Pasparakis

Subjects
Model organisms, Chemical Biology & High Throughput, Multidisciplinary, FOS: Clinical medicine, Genome Integrity & Repair, Immunology, Tumour Biology, Genetics & Genomics, Computational & Systems Biology
Abstract

Mutations of theADAR1gene encoding an RNA deaminase cause severe diseases associated with chronic activation of type I interferon (IFN) responses, including Aicardi–Goutières syndrome and bilateral striatal necrosis1–3. The IFN-inducible p150 isoform of ADAR1 contains a Zα domain that recognizes RNA with an alternative left-handed double-helix structure, termed Z-RNA4,5. HemizygousADAR1mutations in the Zα domain cause type I IFN-mediated pathologies in humans2,3and mice6–8; however, it remains unclear how the interaction of ADAR1 with Z-RNA prevents IFN activation. Here we show that Z-DNA-binding protein 1 (ZBP1), the only other protein in mammals known to harbour Zα domains9, promotes type I IFN activation and fatal pathology in mice with impaired ADAR1 function. ZBP1 deficiency or mutation of its Zα domains reduced the expression of IFN-stimulated genes and largely prevented early postnatal lethality in mice with hemizygous expression of ADAR1 with mutated Zα domain (Adar1mZα/–mice).Adar1mZα/–mice showed upregulation and impaired editing of endogenous retroelement-derived complementary RNA reads, which represent a likely source of Z-RNAs activating ZBP1. Notably, ZBP1 promoted IFN activation and severe pathology inAdar1mZα/–mice in a manner independent of RIPK1, RIPK3, MLKL-mediated necroptosis and caspase-8-dependent apoptosis, suggesting a novel mechanism of action. Thus, ADAR1 prevents endogenous Z-RNA-dependent activation of pathogenic type I IFN responses by ZBP1, suggesting that ZBP1 could contribute to type I interferonopathies caused byADAR1mutations.

Published
2022

2. Supplementary Data from IκB Kinase α Is Required for Development and Progression of KRAS-Mutant Lung Adenocarcinoma

Author

Georgios T. Stathopoulos, Antonia Marazioti, Manolis Pasparakis, Timothy S. Blackwell, Fiona E. Yull, Sebastian Marwitz, Torsten Goldmann, Vasileios Armenis, Theodora Agalioti, Magda Spella, Nikolaos I. Kanellakis, Ioanna Giopanou, Marina Lianou, Georgia A. Giotopoulou, Maria Papageorgopoulou, Ioannis Lilis, and Malamati Vreka

Abstract

Supplementary file containing Supplementary Methods (pertaining to reagents, imaging, immunoblotting, cellular studies, microarray data, NF-κB ELISA, PCR, cell culture, histology, cytology, flow cytometry, constructs, and cellular Assays), 4 Supplementary Tables (pertaining to number of experimental mice, PCR primers, antibodies, and lentiviral shRNA pools), and 7 Supplementary Figures (described in the main and Supplementary text).

Published
2023

3. Data from IκB Kinase α Is Required for Development and Progression of KRAS-Mutant Lung Adenocarcinoma

Author

Georgios T. Stathopoulos, Antonia Marazioti, Manolis Pasparakis, Timothy S. Blackwell, Fiona E. Yull, Sebastian Marwitz, Torsten Goldmann, Vasileios Armenis, Theodora Agalioti, Magda Spella, Nikolaos I. Kanellakis, Ioanna Giopanou, Marina Lianou, Georgia A. Giotopoulou, Maria Papageorgopoulou, Ioannis Lilis, and Malamati Vreka

Abstract

Although oncogenic activation of NFκB has been identified in various tumors, the NFκB–activating kinases (inhibitor of NFκB kinases, IKK) responsible for this are elusive. In this study, we determined the role of IKKα and IKKβ in KRAS-mutant lung adenocarcinomas induced by the carcinogen urethane and by respiratory epithelial expression of oncogenic KRASG12D. Using NFκB reporter mice and conditional deletions of IKKα and IKKβ, we identified two distinct early and late activation phases of NFκB during chemical and genetic lung adenocarcinoma development, which were characterized by nuclear translocation of RelB, IκBβ, and IKKα in tumor-initiated cells. IKKα was a cardinal tumor promoter in chemical and genetic KRAS-mutant lung adenocarcinoma, and respiratory epithelial IKKα-deficient mice were markedly protected from the disease. IKKα specifically cooperated with mutant KRAS for tumor induction in a cell-autonomous fashion, providing mutant cells with a survival advantage in vitro and in vivo. IKKα was highly expressed in human lung adenocarcinoma, and a heat shock protein 90 inhibitor that blocks IKK function delivered superior effects against KRAS-mutant lung adenocarcinoma compared with a specific IKKβ inhibitor. These results demonstrate an actionable requirement for IKKα in KRAS-mutant lung adenocarcinoma, marking the kinase as a therapeutic target against this disease.Significance: These findings report a novel requirement for IKKα in mutant KRAS lung tumor formation, with potential therapeutic applications. Cancer Res; 78(11); 2939–51. ©2018 AACR.

Published
2023

4. ZBP1 causes inflammation by inducing RIPK3-mediated necroptosis and RIPK1 kinase activity-independent apoptosis

Author

Lioba Körner, Laurens Wachsmuth, Snehlata Kumari, Robin Schwarzwer, Huipeng Jiao, and Manolis Pasparakis

Abstract

Z-DNA binding protein 1 (ZBP1) has important functions in anti-viral immunity and in the regulation of inflammatory responses. ZBP1 induces necroptosis by directly engaging and activating RIPK3, however, the mechanisms by which ZBP1 induces inflammation and in particular the role of RIPK1 and the contribution of cell death-independent signaling remain elusive. Here we show that ZBP1 causes inflammation by inducing RIPK3-mediated necroptosis and RIPK1-caspase-8-mediated apoptosis. ZBP1 induced TNFR1-independent skin inflammation in mice with epidermis-specific ablation of FADD by triggering keratinocyte necroptosis. Moreover, transgenic expression of C-terminally truncated constitutively active ZBP1 (ZBP1ca) in mouse epidermis caused skin inflammation that was only partially inhibited by abrogation of RIPK3-MLKL-dependent necroptosis and fully prevented by combined deficiency in MLKL and caspase-8. Importantly, ZBP1ca induced caspase-8-mediated skin inflammation by RHIM-dependent but kinase activity-independent RIPK1 signaling. Furthermore, ZBP1ca-induced inflammatory cytokine production in the skin was completely prevented by combined inhibition of apoptosis and necroptosis arguing against a cell death-independent pro-inflammatory function of ZBP1. Collectively, these results showed that ZBP1 induces inflammation by activating necroptosis and RIPK1 kinase activity-independent apoptosis.

Published
2023

5. RIPK1 blocks T cell senescence mediated by RIPK3 and caspase-8

Author

Takayuki Imanishi, Midori Unno, Natsumi Yoneda, Yasutaka Motomura, Miho Mochizuki, Takaharu Sasaki, Manolis Pasparakis, and Takashi Saito

Subjects
Multidisciplinary
Abstract

Receptor-interacting protein kinase 1 (RIPK1) regulates cell death and inflammation. Here, we show that T cell–specific RIPK1 deficiency in mice leads to the premature senescence of T cells and induces various age-related diseases, resulting in premature death. RIPK1 deficiency causes higher basal activation of mTORC1 (mechanistic target of rapamycin complex 1) that drives enhanced cytokine production, induction of senescence-related genes, and increased activation of caspase-3/7, which are restored by inhibition of mTORC1. Critically, normal aged T cells exhibit similar phenotypes and responses. Mechanistically, a combined deficiency of RIPK3 and caspase-8 inhibition restores the impaired proliferative responses; the elevated activation of Akt, mTORC1, extracellular signal–regulated kinase, and caspase-3/7; and the increased expression of senescence-related genes in RIPK1-deficient CD4 T cells. Last, we revealed that the senescent phenotype of RIPK1-deficient and aged CD4 T cells is restored in the normal tissue environment. Thus, we have clarified the function of RIPK3 and caspase-8 in inducing CD4 T cell senescence, which is modulated by environmental signals.

Published
2023

6. Airway epithelial cell necroptosis contributes to asthma exacerbation in a mouse model of house dust mite-induced allergic inflammation

Author

Nikos Oikonomou, Manolis Pasparakis, Ariadne Androulidaki, Hamida Hammad, Antonis Chatzigiagkos, Vassilis Aidinis, Bart N. Lambrecht, Martjin J Schuijs, and Pulmonary Medicine

Subjects
0301 basic medicine, HOMEOSTASIS, Fas-Associated Death Domain Protein, Mice, 0302 clinical medicine, Medicine and Health Sciences, Basic Helix-Loop-Helix Transcription Factors, Immunology and Allergy, Medicine, FADD, Mice, Knockout, biology, Pyroglyphidae, DEATH, TRIGGERS, respiratory system, Immunohistochemistry, APOPTOSIS, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Necroptosis, Disease Progression, Airway Remodeling, Respiratory virus, Disease Susceptibility, EXPRESSION, Immunology, INTERLEUKIN-1-ALPHA, Respiratory Mucosa, IMMUNITY, Article, Allergic inflammation, 03 medical and health sciences, RIPK1, CASPASE-8, Animals, Humans, Kinase activity, Death domain, RELEASE, House dust mite, business.industry, Biology and Life Sciences, Allergens, Immunoglobulin E, biology.organism_classification, Asthma, Enzyme Activation, Disease Models, Animal, 030104 developmental biology, Receptors, Aryl Hydrocarbon, CREOLA BODIES, biology.protein, business, Biomarkers
Abstract

Regulation of epithelial cell death has emerged as a key mechanism controlling immune homeostasis in barrier surfaces. Necroptosis is a type of regulated necrotic cell death induced by receptor interacting protein kinase 3 (RIPK3) that has been shown to cause inflammatory pathologies in different tissues. The role of regulated cell death and particularly necroptosis in lung homeostasis and disease remains poorly understood. Here we show that mice with Airway Epithelial Cell (AEC)-specific deficiency of Fas-associated with death domain (FADD), an adapter essential for caspase-8 activation, developed exacerbated allergic airway inflammation in a mouse model of asthma induced by sensitization and challenge with house dust mite (HDM) extracts. Genetic inhibition of RIPK1 kinase activity by crossing to mice expressing kinase inactive RIPK1 as well as RIPK3 or MLKL deficiency prevented the development of exaggerated HDM-induced asthma pathology in FADDAEC-KO mice, suggesting that necroptosis of FADD-deficient AECs augmented the allergic immune response. These results reveal a role of AEC necroptosis in amplifying airway allergic inflammation and suggest that necroptosis could contribute to asthma exacerbations caused by respiratory virus infections inducing AEC death.

Published
2021

7. Inhibition of MLKL impairs abdominal aortic aneurysm development by attenuating smooth muscle cell necroptosis

Author

Harshal N Nemade, Dennis Mehrkens, Hannah Sophia Lottermoser, Zeynep Ece Yilmaz, Patrick Schelemei, Felix Ruben Picard, Simon Geißen, Gülsah Fülgen Schwab, Friedrich Felix Hoyer, Henning Guthoff, Alexander Hof, Felix Sebastian Nettersheim, Agapios Sachinidis, Holger Winkels, Stefan Baldus, Manolis Pasparakis, Matti Adam, and Martin Mollenhauer

Abstract

BackgroundReceptor-interacting serine/threonine-protein kinase 1 and 3 (RIPK1 and RIPK3) dependent cell death has been identified as a crucial mediator of abdominal aortic aneurysm (AAA) development. RIPK3 mediates phosphorylation of Mixed lineage kinase domain like pseudokinase (MLKL) thereby inducing its oligomerization and translocation to the cell membrane. Given the dual role of RIPKs being involved in necroptosis as well as in apoptosis induction, the specific role of MLKL-induced necroptotic cell death in AAA remains unclear.MethodsWe monitored elastase-perfusion (PPE) induced progression of AAA in C57BL/6N (WT), RIPK1 kinase-inactive (Ripk1D138N/D138N), MLKL knockout (Mlkl−/−) and MLKL phospho-deficient (MlklAA) mice by ultrasound measurements, histological analyses and bulk mRNA sequencing to assess structural and molecular aortic changes. Bone marrow transplantations in WT andMlklAAmice were utilized to dissect the role of MLKL in smooth muscle cells (SMCs) and myeloid cells in AAA development. MLKL expressing human SMCs were generated to investigate necroptosis-induced proinflammatory cytokine secretion and subsequent polymorphonuclear neutrophil (PMN) migration and activation in vitro.ResultsUltrasound analysis showed that ~70% of the WT animals developed PPE induced-AAA with significant aortic structural alterations and enhanced myeloid cell infiltration. In contrast,Ripk1D138N/D138N,MlklAA, andMlkl−/−mice were protected from AAA. This protection was associated with reduced adverse extracellular matrix (ECM) remodeling and leukocyte infiltration. MLKL deficiency was associated with a significant downregulation of genes involved in fibrinolysis, anti-inflammatory response, immune response and complement activation in aortic tissue in AAA. Bone marrow transplantation studies showed the lack of MLKL in SMCs to be the main driver of AAA protection. Proinflammatory cytokine secretion was elevated in necroptosis induced SMCs and resulted in a significant accumulation and activation of PMN.ConclusionsOverall, these findings indicate that MLKL-induced necroptotic SMC death and subsequent proinflammatory leukocyte activation play a causative role in AAA development and suggest that pharmacological inhibition of MLKL may represent a promising treatment strategy for AAA disease.

Published
2022

8. NIK/MAP3K14 in hepatocytes orchestrates NASH to hepatocellular carcinoma progression via JAK2/STAT5 inhibition

Author

Anna Juliane Vesting, Alexander Jais, Paul Klemm, Lukas Steuernagel, Peter Wienand, Morten Fog-Tonnesen, Henning Hvid, Anna–Lena Schumacher, Christian Kukat, Hendrik Nolte, Theodoros Georgomanolis, Janine Altmüller, Manolis Pasparakis, Andreas Schmidt, Marcus Krüger, Marc Schmidt Supprian, Ari Waisman, Beate Katharina Straub, Nathanael Raschzok, Michel Bernier, Andreas L. Birkenfeld, Nadine Hövelmeyer, Jens C. Brüning, and F. Thomas Wunderlich

Subjects
Cell Biology, Technology Platforms, Nik In Nash To Hcc Progression, Nik-mediated Jak2 Inhibition Impairs Stat5 Signaling, Molecular Biology
Abstract

OBJECTIVE: Nonalcoholic fatty liver disease (NAFLD) ranges from steatosis to nonalcoholic steatohepatitis (NASH), which often progresses to hepatocellular carcinoma (HCC) through a largely undefined mechanism. NASH and HCC depend on inflammatory signaling, whose master regulator is the NFkappaB transcription factor family, activated by canonical and non-canonical pathways. METHODS: Here, we investigated non-canonical NFkappaB-inducing kinase (NIK/MAP3K14) in metabolic NASH, NASH to HCC transition, and DEN-induced HCC. To this end, we performed dietary and chemical interventions in mice that were analyzed via single nucleus sequencing, gene expression and histochemical methods. Ultimately, we verified our mouse results in human patient samples. RESULTS: We revealed that hepatocyte-specific NIK deficiency (NIKLKO) ameliorated metabolic NASH complications and reduced hepatocarcinogenesis, independent of its role in the NFkappaB pathway. Instead, hepatic NIK attenuated hepatoprotective JAK2/STAT5 signaling that is a prerequisite for NASH and NASH to HCC progression in mice and humans. CONCLUSIONS: Our data suggest NIK-mediated inhibitory JAK2 phosphorylation at serine 633 that might be amenable for future therapeutic interventions in patients.

Published
2022

9. NEMO- and RelA-dependent NF-κB Signaling Promotes Small Cell Lung Cancer

Author

Lioba Koerner, Marcel Schmiel, Tsun-Po Yang, Martin Peifer, Reinhard Buettner, and Manolis Pasparakis

Subjects
Cell Biology, Molecular Biology
Abstract

Small cell lung cancer (SCLC) is an aggressive type of lung cancer driven by combined loss of the tumor suppressors RB1 and TP53. SCLC is highly metastatic and despite good initial response to chemotherapy patients usually relapse, resulting in poor survival. Therefore, better understanding of the mechanisms driving SCLC pathogenesis is required to identify new therapeutic targets. Here we identified a critical role of the IKK/NF-κB signaling pathway in SCLC development. Using a relevant mouse model of SCLC, we found that ablation of NEMO/IKKγ, the regulatory subunit of the IKK complex that is essential for activation of canonical NF-κB signaling, strongly delayed the onset and growth of SCLC resulting in considerably prolonged survival. In addition, ablation of the main NF-κB family member p65/RelA also delayed the onset and growth of SCLC and prolonged survival, albeit to a lesser extent than NEMO. Interestingly, constitutive activation of IKK/NF-κB signaling within the tumor cells did not exacerbate the pathogenesis of SCLC, suggesting that endogenous NF-κB levels are sufficient to fully support tumor development. Moreover, TNFR1 deficiency did not affect the development of SCLC, showing that TNF signaling does not play an important role in this tumor type. Taken together, our results revealed that IKK/NF-κB signaling plays an important role in promoting SCLC, identifying the IKK/NF-κB pathway as a promising therapeutic target.

Published
2022

10. Smooth muscle cell specific NEMO deficiency inhibits atherosclerosis in ApoE

Author

Takashi Imai, Trieu-My Van, Manolis Pasparakis, and Apostolos Polykratis

Subjects
Inflammation, Mice, Inbred C57BL, Mice, Knockout, Mice, Multidisciplinary, Apolipoproteins E, Myocytes, Smooth Muscle, Intracellular Signaling Peptides and Proteins, NF-kappa B, Animals, Endothelial Cells, Atherosclerosis, Plaque, Atherosclerotic
Abstract

The development of atherosclerotic plaques is the result of a chronic inflammatory response coordinated by stromal and immune cellular components of the vascular wall. While endothelial cells and leukocytes are well-recognised mediators of inflammation in atherosclerosis, the role of smooth muscle cells (SMCs) remains incompletely understood. Here we aimed to address the role of canonical NF-κB signalling in SMCs in the development of atherosclerosis. We investigated the role of NF-κB signalling in SMCs in atherosclerosis by employing SMC-specific ablation of NEMO, an IKK complex subunit that is essential for canonical NF-κB activation, in ApoE−/− mice. We show that SMC-specific ablation of NEMO (NEMOSMCiKO) inhibited high fat diet induced atherosclerosis in ApoE−/− mice. NEMOSMCiKO/ApoE−/− mice developed less and smaller atherosclerotic plaques, which contained fewer macrophages, decreased numbers of apoptotic cells and smaller necrotic areas and showed reduced inflammation compared to the plaques of ApoE−/− mice. In addition, the plaques of NEMOSMCiKO/ApoE−/− mice showed higher expression of α-SMA and lower expression of the transcriptional factor KLF4 compared to those of ApoE−/− mice. Consistently, in vitro, NEMO-deficient SMCs exhibited reduced proliferation and migration, as well as decreased KLF4 expression and lower production of IL-6 and MCP-1 upon inflammatory stimulus (TNF or LPS) compared to NEMO-expressing SMCs. In conclusion, NEMO-dependent activation of NF-κB signalling in SMCs critically contributes to the pathogenesis of atherosclerosis by regulating SMC proliferation, migration and phenotype switching in response to inflammatory stimuli.

Published
2022

11. p62 Promotes Survival and Hepatocarcinogenesis in Mice with Liver-Specific NEMO Ablation

Author

Vangelis Kondylis, Farina Schneider, Fabian Schorn, Nikos Oikonomou, Beate Katharina Straub, Sabine Werner, Philip Rosenstiel, and Manolis Pasparakis

Subjects
Cancer Research, autophagy, genetic mouse models, Oncology, IκB kinase (IKK) complex, hepatocarcinogenesis, Keap1-Nrf2 activation, chronic liver disease, respiratory system, liver injury
Abstract

SQSTM1/p62 is a multitasking protein that functions as an autophagy receptor, but also as a signaling hub regulating diverse cellular pathways. p62 accumulation in mice with autophagydeficient hepatocytes mediates liver damage and hepatocarcinogenesis through Nrf2 overactivation, yet the role of the p62-Keapl-Nrf2 axis in cell death and hepatocarcinogenesis in the absence of underlying autophagy defects is less clear. Here, we addressed the role of p62 and Nrf2 activation in a chronic liver disease model, namely mice with liver parenchymal cell-specific knockout of NEMO (NEMOLPC-KO), in which we demonstrate that they show no inherent autophagy impairment. Unexpectedly, systemic p62 ablation aggravated the phenotype and caused early postnatal lethality in NEMO(LPC-KO )mice. Expression of a p62 mutant (p624Ex2-5), which retains the ability to form aggregates and activate Nrf2 signaling, did not cause early lethality, but exacerbated hepatocarcinogenesis in these mice. Our immunohistological and molecular analyses showed that the increased tumor burden was only consistent with increased expression/stability of p624Ex2-5 driving Nrf2 hyperactivation, but not with other protumorigenic functions of p62, such as mTOR activation, cMYC upregulation or increased fibrosis. Surprisingly, forced activation of Nrf2 per se did not increase liver injury or tumor burden in NEMOLPC-KO mice, suggesting that autophagy impairment is a necessary prerequisite to unleash the Nrf2 oncogenic potential in mice with autophagy-competent hepatocytes., Cancers, 14 (10), ISSN:2072-6694

Published
2022

12. Z-nucleic-acid sensing triggers ZBP1-dependent necroptosis and inflammation

Author

Robin Schwarzer, Amanda Fisher, Snehlata Kumari, George Kassiotis, Rebecca Lane, Remzi Onur Eren, Huipeng Jiao, Manolis Pasparakis, William J. Kaiser, George R. Young, Juan Lin, and Laurens Wachsmuth

Subjects
Male, 0301 basic medicine, ZBP1, Necroptosis, Active Transport, Cell Nucleus, Endogeny, Skin Diseases, Mice, 03 medical and health sciences, RIPK1, 0302 clinical medicine, Nucleic Acids, medicine, Animals, Nuclear export signal, RNA, Double-Stranded, Inflammation, Caspase 8, Multidisciplinary, Chemistry, RNA-Binding Proteins, RNA, Cell biology, Mice, Inbred C57BL, Cell nucleus, 030104 developmental biology, medicine.anatomical_structure, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Nucleic acid, Female
Abstract

The biological function of Z-DNA and Z-RNA, nucleic acid structures with a left-handed double helix, is poorly understood1–3. Z-DNA-binding protein 1 (ZBP1; also known as DAI or DLM-1) is a nucleic acid sensor that contains two Zα domains that bind Z-DNA4,5 and Z-RNA6–8. ZBP1 mediates host defence against some viruses6,7,9–14 by sensing viral nucleic acids6,7,10. RIPK1 deficiency, or mutation of its RIP homotypic interaction motif (RHIM), triggers ZBP1-dependent necroptosis and inflammation in mice15,16. However, the mechanisms that induce ZBP1 activation in the absence of viral infection remain unknown. Here we show that Zα-dependent sensing of endogenous ligands induces ZBP1-mediated perinatal lethality in mice expressing RIPK1 with mutated RHIM (Ripk1mR/mR), skin inflammation in mice with epidermis-specific RIPK1 deficiency (RIPK1E-KO) and colitis in mice with intestinal epithelial-specific FADD deficiency (FADDIEC-KO). Consistently, functional Zα domains were required for ZBP1-induced necroptosis in fibroblasts that were treated with caspase inhibitors or express RIPK1 with mutated RHIM. Inhibition of nuclear export triggered the Zα-dependent activation of RIPK3 in the nucleus resulting in cell death, which suggests that ZBP1 may recognize nuclear Z-form nucleic acids. We found that ZBP1 constitutively bound cellular double-stranded RNA in a Zα-dependent manner. Complementary reads derived from endogenous retroelements were detected in epidermal RNA, which suggests that double-stranded RNA derived from these retroelements may act as a Zα-domain ligand that triggers the activation of ZBP1. Collectively, our results provide evidence that the sensing of endogenous Z-form nucleic acids by ZBP1 triggers RIPK3-dependent necroptosis and inflammation, which could underlie the development of chronic inflammatory conditions—particularly in individuals with mutations in RIPK1 and CASP817–20. Analyses of mouse models of inflammation suggest some chronic inflammatory conditions may result from Z-DNA-binding protein 1 sensing endogenous Z-form nucleic acids—such as those of endogenous retroelements—through its Zα domains.

Published
2020

13. Mutations that prevent caspase cleavage of RIPK1 cause autoinflammatory disease

Author

Natasha Silke, Manfred Boehm, Amanda K. Ombrello, Ivona Aksentijevich, Deborah L. Stone, Tina Romeo, Marco J Herold, Laurens Wachsmuth, Christine Biben, Beverly K. Barham, Lin Liu, Andrew J. Gross, Sergio D. Rosenzweig, Patrycja Hoffmann, Natalia Sampaio Moura, Gustavo Gutierrez-Cruz, Daniel L. Kastner, Steven E. Boyden, Kristien J. M. Zaal, Anne K. Voss, Holly Anderton, Anne Jones, Hongying Wang, Tobias Kratina, John Silke, Michael J. Lenardo, James C. Mullikin, Kate E. Lawlor, David B. Beck, Mark D. McKenzie, Amanda Light, Anthony K. Shum, Jae Jin Chae, Massimo Gadina, Qing Zhou, Diep Chau, Gineth Pinto-Patarroyo, Hirotsugu Oda, Geryl Wood, Mary Blake, Nima Etemadi, Kristy Shield-Artin, Edwin D. Hawkins, Monique Stoffels, Cathrine Hall, Dan Yang, Wanxia Li Tsai, Hye Sun Kuehn, Natalia I. Dmitrieva, Seth L. Masters, Lixin Zheng, Andrew J. Kueh, Manolis Pasparakis, and Najoua Lalaoui

Subjects
Male, 0301 basic medicine, Programmed cell death, General Science & Technology, Knockout, Necroptosis, Caspase 3, Inflammation, Biology, Inbred C57BL, Caspase 8, Article, Mice, 03 medical and health sciences, RIPK1, 0302 clinical medicine, medicine, Animals, Humans, Kinase activity, Mice, Knockout, Multidisciplinary, Hereditary Autoinflammatory Diseases, MAP Kinase Kinase Kinases, medicine.disease, Pedigree, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Mutation, Female, medicine.symptom, Periodic fever syndrome
Abstract

Receptor Interacting Protein Kinase 1 (RIPK1) is a key regulator of innate immune signalling pathways. To ensure an optimal inflammatory response, RIPK1 is post-translationally regulated by well characterised ubiquitylation and phosphorylation events, as well as caspase-8 mediated cleavage1–7. The physiological relevance of this cleavage remains unclear, though it is believed to inhibit activation of RIPK3 and necroptosis8. Here we show that heterozygous missense mutations p.D324N, p.D324H and p.D324Y prevent caspase cleavage of RIPK1 in humans and result in early-onset periodic fever episodes and severe intermittent lymphadenopathy, a condition we designate ‘Cleavage-resistant RIPK1-Induced Autoinflammatory’ (CRIA) syndrome. To define the mechanism for this disease we generated a cleavage-resistant Ripk1D325A mutant mouse strain. While Ripk1-/- mice die postnatally from systemic inflammation, Ripk1D325A/D325A mice died during embryogenesis. Embryonic lethality was completely prevented by combined loss of Casp8 and Ripk3 but not by loss of Ripk3 or Mlkl alone. Loss of RIPK1 kinase activity also prevented Ripk1D325A/D325A embryonic lethality, however the mice died before weaning from multi organ inflammation in a RIPK3 dependent manner. Consistently, Ripk1D325A/D325A and Ripk1D325A/+ cells were hypersensitive to RIPK3 dependent TNF-induced apoptosis and necroptosis. Heterozygous Ripk1D325A/+ mice were viable and grossly normal, but were hyper-responsive to inflammatory stimuli in vivo. Our results demonstrate the importance of caspase-mediated RIPK1 cleavage during embryonic development and show that caspase cleavage of RIPK1 not only inhibits necroptosis but maintains inflammatory homeostasis throughout life.

Published
2019

15. A20 prevents inflammasome-dependent arthritis by inhibiting macrophage necroptosis through its ZnF7 ubiquitin-binding domain

Author

Yoshitaka Shirasaki, Bernhard Holzmann, Sotaro Uemura, Marietta Armaka, Manolis Pasparakis, Geert van Loo, Apostolos Polykratis, Masayuki Miura, Arne Martens, Mai Yamagishi, George Kollias, Yoshifumi Yamaguchi, and Remzi Onur Eren

Subjects
Lipopolysaccharides, Programmed cell death, Ubiquitin binding, Inflammasomes, Necroptosis, Inflammatory arthritis, Interleukin-1beta, Kruppel-Like Transcription Factors, Arthritis, Deubiquitinating enzyme, Mice, Necrosis, 03 medical and health sciences, RIPK1, 0302 clinical medicine, immune system diseases, ddc:570, hemic and lymphatic diseases, medicine, Animals, Humans, Tumor Necrosis Factor alpha-Induced Protein 3, 030304 developmental biology, Inflammation, 0303 health sciences, biology, Ubiquitin, Chemistry, Macrophages, NF-kappa B, Inflammasome, Cell Biology, medicine.disease, Cell biology, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Mutation, biology.protein, Protein Kinases, Protein Binding, medicine.drug
Abstract

Deficiency in the deubiquitinating enzyme A20 causes severe inflammation in mice, and impaired A20 function is associated with human inflammatory diseases. A20 has been implicated in negatively regulating NF-κB signalling, cell death and inflammasome activation; however, the mechanisms by which A20 inhibits inflammation in vivo remain poorly understood. Genetic studies in mice revealed that its deubiquitinase activity is not essential for A20 anti-inflammatory function. Here we show that A20 prevents inflammasome-dependent arthritis by inhibiting macrophage necroptosis and that this function depends on its zinc finger 7 (ZnF7). We provide genetic evidence that RIPK1 kinase-dependent, RIPK3-MLKL-mediated necroptosis drives inflammasome activation in A20-deficient macrophages and causes inflammatory arthritis in mice. Single-cell imaging revealed that RIPK3-dependent death caused inflammasome-dependent IL-1β release from lipopolysaccharide-stimulated A20-deficient macrophages. Importantly, mutation of the A20 ZnF7 ubiquitin binding domain caused arthritis in mice, arguing that ZnF7-dependent inhibition of necroptosis is critical for A20 anti-inflammatory function in vivo.

Published
2019

16. The SARS-CoV-2 main protease M

Author

Jan, Wenzel, Josephine, Lampe, Helge, Müller-Fielitz, Raphael, Schuster, Marietta, Zille, Kristin, Müller, Markus, Krohn, Jakob, Körbelin, Linlin, Zhang, Ümit, Özorhan, Vanessa, Neve, Julian U G, Wagner, Denisa, Bojkova, Mariana, Shumliakivska, Yun, Jiang, Anke, Fähnrich, Fabian, Ott, Valentin, Sencio, Cyril, Robil, Susanne, Pfefferle, Florent, Sauve, Caio Fernando Ferreira, Coêlho, Jonas, Franz, Frauke, Spiecker, Beate, Lembrich, Sonja, Binder, Nina, Feller, Peter, König, Hauke, Busch, Ludovic, Collin, Roberto, Villaseñor, Olaf, Jöhren, Hermann C, Altmeppen, Manolis, Pasparakis, Stefanie, Dimmeler, Jindrich, Cinatl, Klaus, Püschel, Matija, Zelic, Dimitry, Ofengeim, Christine, Stadelmann, François, Trottein, Ruben, Nogueiras, Rolf, Hilgenfeld, Markus, Glatzel, Vincent, Prevot, and Markus, Schwaninger

Subjects
Male, Mice, Knockout, Mesocricetus, SARS-CoV-2, Intracellular Signaling Peptides and Proteins, Brain, Mice, Transgenic, Article, Mice, Inbred C57BL, Mice, Blood-Brain Barrier, Cricetinae, Chlorocebus aethiops, Microvessels, Animals, Humans, Female, Vero Cells, Coronavirus 3C Proteases, Central nervous system infections
Abstract

Coronavirus disease 2019 (COVID-19) can damage cerebral small vessels and cause neurological symptoms. Here we describe structural changes in cerebral small vessels of patients with COVID-19 and elucidate potential mechanisms underlying the vascular pathology. In brains of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)-infected individuals and animal models, we found an increased number of empty basement membrane tubes, so-called string vessels representing remnants of lost capillaries. We obtained evidence that brain endothelial cells are infected and that the main protease of SARS-CoV-2 (Mpro) cleaves NEMO, the essential modulator of nuclear factor-κB. By ablating NEMO, Mpro induces the death of human brain endothelial cells and the occurrence of string vessels in mice. Deletion of receptor-interacting protein kinase (RIPK) 3, a mediator of regulated cell death, blocks the vessel rarefaction and disruption of the blood–brain barrier due to NEMO ablation. Importantly, a pharmacological inhibitor of RIPK signaling prevented the Mpro-induced microvascular pathology. Our data suggest RIPK as a potential therapeutic target to treat the neuropathology of COVID-19., A novel study led by scientists in Lübeck, Germany, shows that SARS-CoV-2-infected brain endothelial cells undergo cell death due to the cleavage of NEMO by the viral protease Mpro, potentially causing cerebral COVID-19 and ‘long COVID’ symptoms.

Published
2020

17. Sequential activation of necroptosis and apoptosis cooperates to mediate vascular and neural pathology in stroke

Author

Jinwoo Lee, Daichao Xu, Junying Yuan, Palak Amin, Wanjin Li, H. Wang, Manolis Pasparakis, Michelle A. Kelliher, and Masanori Gomi Naito

Subjects
Male, Programmed cell death, Necroptosis, Ischemia, Apoptosis, RIPK1, Mice, Conditional gene knockout, medicine, Animals, Neuroinflammation, Inflammation, Mice, Knockout, Multidisciplinary, Cell Death, business.industry, Neurodegeneration, Biological Sciences, medicine.disease, MAP Kinase Kinase Kinases, Stroke, Brain Injuries, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, business
Abstract

Apoptosis and necroptosis are two regulated cell death mechanisms; however, the interaction between these cell death pathways in vivo is unclear. Here we used cerebral ischemia/reperfusion as a model to investigate the interaction between apoptosis and necroptosis. We show that the activation of RIPK1 sequentially promotes necroptosis followed by apoptosis in a temporally specific manner. Cerebral ischemia/reperfusion insult rapidly activates necroptosis to promote cerebral hemorrhage and neuroinflammation. Ripk3 deficiency reduces cerebral hemorrhage and delays the onset of neural damage mediated by inflammation. Reduced cerebral perfusion resulting from arterial occlusion promotes the degradation of TAK1, a suppressor of RIPK1, and the transition from necroptosis to apoptosis. Conditional knockout of TAK1 in microglial/infiltrated macrophages and neuronal lineages sensitizes to ischemic infarction by promoting apoptosis. Taken together, our results demonstrate the critical role of necroptosis in mediating neurovascular damage and hypoperfusion-induced TAK1 loss, which subsequently promotes apoptosis and cerebral pathology in stroke and neurodegeneration.

Published
2020

18. Correction: A20 protects cells from TNF-induced apoptosis through linear ubiquitin-dependent and -independent mechanisms

Author

Manolis Pasparakis, Peter Vandenabeele, Dario Priem, Wim Declercq, Adrian T. Ting, Geert van Loo, Michael Devos, Sarah Druw, Mathieu J.M. Bertrand, Karolina Slowicka, and Arne Martens

Subjects
Cancer Research, Cellular and Molecular Neuroscience, Programmed cell death, Ubiquitin, biology, Chemistry, Apoptosis, Immunology, Cancer research, biology.protein, Tumor necrosis factor alpha, Cell Biology, Disease
Abstract

The original version of this article contained an error in the name of one of the co-authors (Wim Declercq). This has been corrected in the PDF and HTML versions.

Published
2020

19. New insights into the regulation of apoptosis, necroptosis, and pyroptosis by receptor interacting protein kinase 1 and caspase-8

Author

Robin Schwarzer, Lucie Laurien, and Manolis Pasparakis

Subjects
Programmed cell death, Necroptosis, Inflammation, Apoptosis, Biology, Caspase 8, 03 medical and health sciences, RIPK1, Necrosis, 0302 clinical medicine, ddc:570, medicine, Pyroptosis, Animals, Humans, Cell Death Signaling, 030304 developmental biology, 0303 health sciences, Cell Biology, 3. Good health, Cell biology, Receptor-Interacting Protein Serine-Threonine Kinases, medicine.symptom, 030217 neurology & neurosurgery, Signal Transduction
Abstract

Necroptosis and pyroptosis are inflammatory forms of regulated necrotic cell death as opposed to apoptosis that is generally considered immunologically silent. Recent studies revealed unexpected links in the pathways regulating and executing cell death in response to activation of signaling cascades inducing apoptosis, necroptosis, and pyroptosis. Emerging evidence suggests that receptor interacting protein kinase 1 and caspase-8 control the cross-talk between apoptosis, necroptosis, and pyroptosis and determine the type of cell death induced in response to activation of cell death signaling.

Published
2020

20. CD11b + CD103 - Sentinel DCs Relay a Tunable Antibacterial NFκB Response in Intestinal Epithelial Cells Via TNF

Author

Katerina Vlantis, Mikael E. Sellin, Luigi Tortola, Giverny Ganz, Markus Furter, Toshihiro Nakamura, Danjiela Heide, Manolis Pasparakis, Anna A. Müller-Hauser, Manfred Kopf, Annika Hausmann, Boas Felmy, Wolf-Dietrich Hardt, Laurens Wachsmuth, Leo Kunz, Timm Schroeder, Dorothée L. Berthold, Stefan A. Fattinger, Mathias Heikenwalder, Tamas Dolowschiak, and Manja Barthel-Scherrer

Subjects
biology, Chemistry, Crypt, Inflammation, Epithelium, Cell biology, medicine.anatomical_structure, Integrin alpha M, In vivo, biology.protein, TLR4, medicine, Tumor necrosis factor alpha, Secretion, medicine.symptom
Abstract

Intestinal epithelial cell (IEC) NFκB signaling regulates the fine balance between mucosal homeostasis and inflammation. It is not fully understood which signals tune this balance, and how bacterial exposure elicits the process. Pure LPS induces epithelial NFκB activation in vivo. We found that in mice, IECs do not respond directly to LPS. Instead, CD11b+ CD103- intercrypt DCs sense LPS via TLR4 and secrete TNF to elicit epithelial NFκB signaling in their immediate neighborhood. This response is relevant also during oral enteropathogen infection. The DC-TNF-IEC axis avoids responses to luminal microbiota LPS, but enables localized or tissue-wide epithelial NFκB responses in proportion to the microbial threat. Thereby, the CD11b+ CD103- intercrypt DCs serve as important sentinels for Gram-negative microbes breaching the epithelial barrier. The tunability of this crypt response allows induction of defense mechanisms at an appropriate scale according to localization and intensity of microbial triggers.

Published
2020

21. 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

22. Dendritic Cell RIPK1 Maintains Immune Homeostasis by Preventing Inflammation and Autoimmunity

Author

Joanne A. O’Donnell, Michelle A. Kelliher, Jesse Lehman, Justine E. Roderick, Katherine A. Fitzgerald, Nicole Hermance, Ann Marshak-Rothstein, Matija Zelic, Stephen Lyle, Manolis Pasparakis, Dalia Martinez-Marin, and Ciara G. Doran

Subjects
0301 basic medicine, Programmed cell death, Necroptosis, Immunology, Lymphadenopathy, Autoimmunity, Inflammation, Biology, Systemic inflammation, medicine.disease_cause, Mice, Necrosis, 03 medical and health sciences, RIPK1, medicine, Animals, Immunology and Allergy, Autoantibodies, Mice, Knockout, B-Lymphocytes, Gene Expression Profiling, Toll-Like Receptors, Immunity, Dendritic Cells, Dendritic cell, Fibrosis, Cell biology, Disease Models, Animal, 030104 developmental biology, Receptor-Interacting Protein Serine-Threonine Kinases, Myeloid Differentiation Factor 88, Cytokines, Signal transduction, medicine.symptom, Signal Transduction
Abstract

Necroptosis is a form of cell death associated with inflammation; however, the biological consequences of chronic necroptosis are unknown. Necroptosis is mediated by RIPK1, RIPK3, and MLKL kinases but in hematopoietic cells RIPK1 has anti-inflammatory roles and functions to prevent necroptosis. Here we interrogate the consequences of chronic necroptosis on immune homeostasis by deleting Ripk1 in mouse dendritic cells. We demonstrate that deregulated necroptosis results in systemic inflammation, tissue fibrosis, and autoimmunity. We show that inflammation and autoimmunity are prevented upon expression of kinase inactive RIPK1 or deletion of RIPK3 or MLKL. We provide evidence that the inflammation is not driven by microbial ligands, but depends on the release of danger-associated molecular patterns and MyD88-dependent signaling. Importantly, although the inflammation is independent of type I IFN and the nucleic acid sensing TLRs, blocking these pathways rescues the autoimmunity. These mouse genetic studies reveal that chronic necroptosis may underlie human fibrotic and autoimmune disorders.

Published
2018

23. Concern over use of the term Z-DNA

Author

Manolis Pasparakis, Edward S. Mocarski, Andrew H.-J. Wang, Alan Herbert, Karen M. Vasquez, and Thomas M. Jovin

Subjects
Z-DNA, Multidisciplinary, DNA, Z-Form, Nucleic Acid Conformation, DNA, Computational biology, Biology, Term (time)
Published
2021

24. CCR2+monocytic myeloid-derived suppressor cells (M-MDSCs) inhibit collagen degradation and promote lung fibrosis by producing transforming growth factor-β1

Author

Doriana Ricci, Xavier Izquierdo Carerra, Raynal Devosse, Mihaly Palmai-Pallag, François Huaux, Astrid Lebrun, Saloua Ibouraadaten, Yousof Yakoub, Mathilde Chantry, Dominique Lison, Manolis Pasparakis, Sandra Lo Re, Francine Uwambayinema, and Lisa Brombin

Subjects
0301 basic medicine, Metalloproteinase, Chemistry, Inflammation, Tissue inhibitor of metalloproteinase, medicine.disease, Pathology and Forensic Medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Fibrosis, 030220 oncology & carcinogenesis, Immunology, Fibrocyte, medicine, Cancer research, Myeloid-derived Suppressor Cell, medicine.symptom, Progenitor cell, Transforming growth factor
Abstract

Monocytes infiltrating scar tissue are predominantly viewed as progenitor cells. Here, we show that tissue CCR2+ monocytes have specific immunosuppressive and profibrotic functions. CCR2+ monocytic cells are acutely recruited to the lung before the onset of silica-induced fibrosis in mice. These tissue monocytes are defined as monocytic myeloid-derived suppressor cells (M-MDSCs) because they significantly suppress T-lymphocyte proliferation in vitro. M-MDSCs collected from silica-treated mice also express transforming growth factor (TGF)-β1, which stimulates lung fibroblasts to release tissue inhibitor of metalloproteinase (TIMP)-1, an inhibitor of metalloproteinase collagenolytic activity. By using LysMCreCCR2loxP/loxP mice, we show that limiting CCR2+ M-MDSC accumulation reduces the pulmonary contents of TGF-β1, TIMP-1 and collagen after silica treatment. M-MDSCs do not differentiate into lung macrophages, granulocytes or fibrocytes during pulmonary fibrogenesis. Collectively, our data indicate that M-MDSCs contribute to lung fibrosis by specifically promoting a non-degrading collagen microenvironment. Copyright © 2017 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published
2017

25. 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

26. The interplay of IKK, NF-κB and RIPK1 signaling in the regulation of cell death, tissue homeostasis and inflammation

Author

Vangelis Kondylis, Manolis Pasparakis, Katerina Vlantis, and Snehlata Kumari

Subjects
0301 basic medicine, Programmed cell death, Necroptosis, Immunology, Inflammation, IκB kinase, Biology, 03 medical and health sciences, RIPK1, chemistry.chemical_compound, medicine, Animals, Homeostasis, Humans, Immunology and Allergy, FADD, Tissue homeostasis, Wound Healing, Cell Death, NF-kappa B, NF-κB, I-kappa B Kinase, Cell biology, 030104 developmental biology, chemistry, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, biology.protein, medicine.symptom, Signal Transduction
Abstract

Regulated cell death pathways have important functions in host defense and tissue homeostasis. Studies in genetic mouse models provided evidence that cell death could cause inflammation in different tissues. Inhibition of RIPK3-MLKL-dependent necroptosis by FADD and caspase-8 was identified as a key mechanism preventing inflammation in epithelial barriers. Moreover, the interplay between IKK/NF-κB and RIPK1 signaling was recognized as a critical determinant of tissue homeostasis and inflammation. NEMO was shown to regulate RIPK1 kinase activity-mediated apoptosis by NF-κB-dependent and -independent functions, which are critical for averting chronic tissue injury and inflammation in the intestine and the liver. In addition, RIPK1 was shown to exhibit kinase activity-independent functions that are essential for preventing cell death, maintaining tissue architecture and inhibiting inflammation. In the intestine, RIPK1 acts as a scaffold to prevent epithelial cell apoptosis and preserve tissue integrity. In the skin, RIPK1 functions via its RHIM to counteract ZBP1/DAI-dependent activation of RIPK3-MLKL-dependent necroptosis and inflammation. Collectively, these studies provided evidence that the regulation of cell death signaling plays an important role in the maintenance of tissue homeostasis, and suggested that cell death could be causally involved in the pathogenesis of inflammatory diseases.

Published
2017

27. Lipid signalling drives proteolytic rewiring of mitochondria by YME1L

Author

Hans-Georg Sprenger, Sinika Henschke, Yue Zhao, Jiahui Li, Nicola Zamboni, Robin Schwarzer, Takashi Tatsuta, Jan Riemer, Manolis Pasparakis, Hendrik Nolte, Thomas MacVicar, Barbara Lindner, Jens C. Brüning, Thomas Langer, Fiona Carola Mayer, Yohsuke Ohba, Marcus Krüger, Markus Habich, and Christiane J. Bruns

Subjects
0301 basic medicine, Cell, mTORC1, Mechanistic Target of Rapamycin Complex 1, Mitochondrion, Cell Line, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Cell Proliferation, Multidisciplinary, Chemistry, Cell growth, Metalloendopeptidases, Lipid metabolism, Lipid Metabolism, Lipids, Cell Hypoxia, Mitochondria, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Proteostasis, Mitochondrial biogenesis, 030220 oncology & carcinogenesis, Proteolysis, ATPases Associated with Diverse Cellular Activities, Reprogramming
Abstract

Reprogramming of mitochondria provides cells with the metabolic flexibility required to adapt to various developmental transitions such as stem cell activation or immune cell reprogramming, and to respond to environmental challenges such as those encountered under hypoxic conditions or during tumorigenesis(1-3). Here we show that the i-AAA protease YME1L rewires the proteome of pre-existing mitochondria in response to hypoxia or nutrient starvation. Inhibition of mTORC1 induces a lipid signalling cascade via the phosphatidic acid phosphatase LIPIN1, which decreases phosphatidylethanolamine levels in mitochondrial membranes and promotes proteolysis. YME1L degrades mitochondrial protein translocases, lipid transfer proteins and metabolic enzymes to acutely limit mitochondrial biogenesis and support cell growth. YME1L-mediated mitochondrial reshaping supports the growth of pancreatic ductal adenocarcinoma (PDAC) cells as spheroids or xenografts. Similar changes to the mitochondrial proteome occur in the tumour tissues of patients with PDAC, suggesting that YME1L is relevant to the pathophysiology of these tumours. Our results identify the mTORC1-LIPIN1-YME1L axis as a post-translational regulator of mitochondrial proteostasis at the interface between metabolism and mitochondrial dynamics.

Published
2019

28. FADD and Caspase-8 Regulate Gut Homeostasis and Inflammation by Controlling MLKL- and GSDMD-Mediated Death of Intestinal Epithelial Cells

Author

Manolis Pasparakis, Achim Tresch, Huipeng Jiao, Robin Schwarzer, and Laurens Wachsmuth

Subjects
0301 basic medicine, Programmed cell death, Necroptosis, Fas-Associated Death Domain Protein, Immunology, Inflammation, Apoptosis, Biology, Caspase 8, 03 medical and health sciences, RIPK1, Mice, 0302 clinical medicine, ddc:570, medicine, Immunology and Allergy, Animals, Homeostasis, Ileitis, FADD, Intestinal Mucosa, Mice, Knockout, Cell Death, Gene Expression Profiling, Pyroptosis, Intracellular Signaling Peptides and Proteins, Epithelial Cells, Phosphate-Binding Proteins, medicine.disease, Inflammatory Bowel Diseases, Immunohistochemistry, 3. Good health, Cell biology, Disease Models, Animal, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, biology.protein, Disease Susceptibility, medicine.symptom, Protein Kinases
Abstract

Pathways controlling intestinal epithelial cell (IEC) death regulate gut immune homeostasis and contribute to the pathogenesis of inflammatory bowel diseases. Here we show that caspase-8 and its adapter FADD act in IECs to regulate intestinal inflammation downstream of Z-DNA binding protein 1 (ZBP1)- and tumor necrosis factor receptor-1 (TNFR1)-mediated receptor interacting protein kinase 1 (RIPK1) and RIPK3 signaling. Mice with IEC-specific FADD or caspase-8 deficiency developed colitis dependent on mixed lineage kinase-like (MLKL)-mediated epithelial cell necroptosis. However, MLKL deficiency fully prevented ileitis caused by epithelial caspase-8 ablation, but only partially ameliorated ileitis in mice lacking FADD in IECs. Our genetic studies revealed that caspase-8 and gasdermin-D (GSDMD) were both required for the development of MLKL-independent ileitis in mice with epithelial FADD deficiency. Therefore, FADD prevents intestinal inflammation downstream of ZBP1 and TNFR1 by inhibiting both MLKL-induced necroptosis and caspase-8-GSDMD-dependent pyroptosis-like death of epithelial cells.

Published
2019

29. Autophosphorylation at serine 166 regulates RIP kinase 1-mediated cell death and inflammation

Author

Mathieu J.M. Bertrand, Lucie Laurien, Snehlata Kumari, Teresa Corona, Masahiro Nagata, Robin Schwarzer, Vangelis Kondylis, Manolis Pasparakis, Janica L Wiederstein, Tom Delanghe, Hannah Schünke, and Marcus Krüger

Subjects
0301 basic medicine, HOMEOSTASIS, General Physics and Astronomy, Apoptosis, Hepatitis, ACTIVATION, STEATOHEPATITIS, Phosphoserine, 0302 clinical medicine, HEPATOCELLULAR-CARCINOMA, Neoplasms, Medicine and Health Sciences, Phosphorylation, lcsh:Science, PHOSPHORYLATION, Skin, Multidisciplinary, Kinase, Chemistry, Autophosphorylation, Intracellular Signaling Peptides and Proteins, Alanine Transaminase, Colitis, 3. Good health, Cell biology, APOPTOSIS, Receptor-Interacting Protein Serine-Threonine Kinases, Necroptosis, EXPRESSION, Programmed cell death, NEMO/IKK-GAMMA, Genotype, Science, Genetics and Molecular Biology, Bone Marrow Cells, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, RIPK1, Sepsis, Animals, Kinase activity, NECROPTOSIS, Inflammation, Tumor Necrosis Factor-alpha, Macrophages, Biology and Life Sciences, General Chemistry, Mice, Inbred C57BL, MICE, 030104 developmental biology, General Biochemistry, Mutation, lcsh:Q, 030217 neurology & neurosurgery
Abstract

Receptor interacting protein kinase 1 (RIPK1) regulates cell death and inflammatory responses downstream of TNFR1 and other receptors, and has been implicated in the pathogenesis of inflammatory and degenerative diseases. RIPK1 kinase activity induces apoptosis and necroptosis, however the mechanisms and phosphorylation events regulating RIPK1-dependent cell death signaling remain poorly understood. Here we show that RIPK1 autophosphorylation at serine 166 plays a critical role for the activation of RIPK1 kinase-dependent apoptosis and necroptosis. Moreover, we show that S166 phosphorylation is required for RIPK1 kinase-dependent pathogenesis of inflammatory pathologies in vivo in four relevant mouse models. Mechanistically, we provide evidence that trans autophosphorylation at S166 modulates RIPK1 kinase activation but is not by itself sufficient to induce cell death. These results show that S166 autophosphorylation licenses RIPK1 kinase activity to induce downstream cell death signaling and inflammation, suggesting that S166 phosphorylation can serve as a reliable biomarker for RIPK1 kinase-dependent pathologies., Receptor interacting protein kinase 1 (RIPK1) regulates cell death and inflammatory responses. Here the authors show that autophosphorylation at Ser166 is required for RIPK1-mediated cell death and inflammation in mouse models of inflammatory pathologies, making Ser166 phosphorylation a possible biomarker for RIPK1-mediated inflammatory diseases.

Published
2019

30. A20 protects cells from TNF-induced apoptosis through linear ubiquitin-dependent and -independent mechanisms

Author

Peter Vandenabeele, Manolis Pasparakis, Wim Declercq, Geert van Loo, Mathieu J.M. Bertrand, Adrian T. Ting, Dario Priem, Sarah Druwé, Michael Devos, Arne Martens, and Karolina Slowicka

Subjects
Cancer Research, Programmed cell death, medicine.medical_treatment, Immunology, NF-KAPPA-B, CYLD, Apoptosis, Article, ACTIVATION, Cellular and Molecular Neuroscience, RIPK1, Mice, Stress signalling, Ubiquitin, INFLAMMATION, immune system diseases, hemic and lymphatic diseases, BINDING, medicine, Medicine and Health Sciences, Animals, Humans, CHAINS, lcsh:QH573-671, PHOSPHORYLATION, Ubiquitins, Tumor Necrosis Factor alpha-Induced Protein 3, COMPLEX, biology, lcsh:Cytology, Chemistry, DEATH, Biology and Life Sciences, Correction, Cell Biology, Ubiquitin ligase, Cell biology, Cytokine, Receptors, Tumor Necrosis Factor, Type I, biology.protein, Tumor necrosis factor alpha, Signal transduction, POLYUBIQUITIN, Signal Transduction
Abstract

The cytokine TNF promotes inflammation either directly by activating the MAPK and NF-κB signaling pathways, or indirectly by triggering cell death. A20 is a potent anti-inflammatory molecule, and mutations in the gene encoding A20 are associated with a wide panel of inflammatory pathologies, both in human and in the mouse. Binding of TNF to TNFR1 triggers the NF-κB-dependent expression of A20 as part of a negative feedback mechanism preventing sustained NF-κB activation. Apart from acting as an NF-κB inhibitor, A20 is also well-known for its ability to counteract the cytotoxic potential of TNF. However, the mechanism by which A20 mediates this function and the exact cell death modality that it represses have remained incompletely understood. In the present study, we provide in vitro and in vivo evidences that deletion of A20 induces RIPK1 kinase-dependent and -independent apoptosis upon single TNF stimulation. We show that constitutively expressed A20 is recruited to TNFR1 signaling complex (Complex I) via its seventh zinc finger (ZF7) domain, in a cIAP1/2-dependent manner, within minutes after TNF sensing. We demonstrate that Complex I-recruited A20 protects cells from apoptosis by stabilizing the linear (M1) ubiquitin network associated to Complex I, a process independent of its E3 ubiquitin ligase and deubiquitylase (DUB) activities and which is counteracted by the DUB CYLD, both in vitro and in vivo. In absence of linear ubiquitylation, A20 is still recruited to Complex I via its ZF4 and ZF7 domains, but this time protects the cells from death by deploying its DUB activity. Together, our results therefore demonstrate two distinct molecular mechanisms by which constitutively expressed A20 protect cells from TNF-induced apoptosis.

Published
2019

31. RIPK1 counteracts ZBP1-mediated necroptosis to inhibit inflammation

Author

Apostolos Polykratis, Snehlata Kumari, Manolis Pasparakis, Trieu-My Van, Juan Lin, Laurens Wachsmuth, and Chun Kim

Subjects
Keratinocytes, 0301 basic medicine, Programmed cell death, Necroptosis, Apoptosis, Inflammation, Biology, Article, Mice, Necrosis, 03 medical and health sciences, RIPK1, 0302 clinical medicine, Protein Domains, medicine, Animals, Phosphorylation, Kinase activity, Protein kinase A, Glycoproteins, Skin, Multidisciplinary, RNA-Binding Proteins, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Mutation, Cancer research, medicine.symptom, Keratinocyte, Protein Kinases
Abstract

Receptor-interacting protein kinase 1 (RIPK1) regulates cell death and inflammation through kinase-dependent and -independent functions. RIPK1 kinase activity induces caspase-8-dependent apoptosis and RIPK3 and mixed lineage kinase like (MLKL)-dependent necroptosis. In addition, RIPK1 inhibits apoptosis and necroptosis through kinase-independent functions, which are important for late embryonic development and the prevention of inflammation in epithelial barriers. The mechanism by which RIPK1 counteracts RIPK3-MLKL-mediated necroptosis has remained unknown. Here we show that RIPK1 prevents skin inflammation by inhibiting activation of RIPK3-MLKL-dependent necroptosis mediated by Z-DNA binding protein 1 (ZBP1, also known as DAI or DLM1). ZBP1 deficiency inhibited keratinocyte necroptosis and skin inflammation in mice with epidermis-specific RIPK1 knockout. Moreover, mutation of the conserved RIP homotypic interaction motif (RHIM) of endogenous mouse RIPK1 (RIPK1mRHIM) caused perinatal lethality that was prevented by RIPK3, MLKL or ZBP1 deficiency. Furthermore, mice expressing only RIPK1mRHIM in keratinocytes developed skin inflammation that was abrogated by MLKL or ZBP1 deficiency. Mechanistically, ZBP1 interacted strongly with phosphorylated RIPK3 in cells expressing RIPK1mRHIM, suggesting that the RIPK1 RHIM prevents ZBP1 from binding and activating RIPK3. Collectively, these results show that RIPK1 prevents perinatal death as well as skin inflammation in adult mice by inhibiting ZBP1-induced necroptosis. Furthermore, these findings identify ZBP1 as a critical mediator of inflammation beyond its previously known role in antiviral defence and suggest that ZBP1 might be implicated in the pathogenesis of necroptosis-associated inflammatory diseases.

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. A brain microvasculature endothelial cell‐specific viral vector with the potential to treat neurovascular and neurological diseases

Author

Jakob Körbelin, Henning Seismann, Dirk A. Ridder, Stefan Michelfelder, Martin Trepel, Jacqueline Bannach, Melanie Lampe, Godwin Dogbevia, Agnes Hunger, Manolis Pasparakis, Jan Wenzel, Markus Schwaninger, and Jürgen A. Kleinschmidt

Subjects
0301 basic medicine, Genetic enhancement, Incontinentia pigmenti, Biology, Bioinformatics, medicine.disease_cause, medicine.disease, Viral vector, Endothelial stem cell, 03 medical and health sciences, Transduction (genetics), 030104 developmental biology, Capsid, Immunology, medicine, Molecular Medicine, ddc:610, Receptor, Adeno-associated virus
Abstract

Gene therapy critically relies on vectors that combine high transduction efficiency with a high degree of target specificity and that can be administered through a safe intravenous route. The lack of suitable vectors, especially for gene therapy of brain disorders, represents a major obstacle. Therefore, we applied an in vivo screening system of random ligand libraries displayed on adeno-associated viral capsids to select brain-targeted vectors for the treatment of neurovascular diseases. We identified a capsid variant showing an unprecedented degree of specificity and long-lasting transduction efficiency for brain microvasculature endothelial cells as the primary target of selection. A therapeutic vector based on this selected viral capsid was used to markedly attenuate the severe cerebrovascular pathology of mice with incontinentia pigmenti after a single intravenous injection. Furthermore, the versatility of this selection system will make it possible to select ligands for additional in vivo targets without requiring previous identification of potential target-specific receptors.

Published
2016

34. Opposing role of tumor necrosis factor receptor 1 signaling in T cell–mediated hepatitis and bacterial infection in mice

Author

Henning Walczak, Hanno Ehlken, Manolis Pasparakis, Vangelis Kondylis, George Kollias, Christoph Schramm, Hans-Willi Mittrücker, Marietta Armaka, Raluca Wroblewski, and Ansgar W. Lohse

Subjects
Lipopolysaccharides, Male, 0301 basic medicine, medicine.medical_specialty, T-Lymphocytes, T cell, Hepatitis, Animal, Biology, Listeria infection, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Concanavalin A, medicine, Animals, Receptor, Hepatitis, Hepatology, Myeloid-Derived Suppressor Cells, Endothelial Cells, medicine.disease, Listeria monocytogenes, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Liver, Receptors, Tumor Necrosis Factor, Type I, 030220 oncology & carcinogenesis, Immunology, Myeloid-derived Suppressor Cell, Tumor necrosis factor alpha, Tumor necrosis factor receptor 1
Abstract

UNLABELLED Death receptor (DR) ligands such as tumor necrosis factor (TNF) have been identified as fundamental mediators of liver damage both in mouse models and in humans. While the essential site of function of DR signaling is conceivably the hepatocyte, a systematic analysis is missing. Using mice with conditional gene ablation, we analyzed the tissue-specific function of DR signaling in T cell-dependent (concanavalin A) and independent (lipopolysaccharide/galactosamine) hepatitis and in models of bacterial infection (Listeria monocytogenes, lipopolysaccharide). We report that lipopolysaccharide/galactosamine-induced liver injury depends on hepatocyte-intrinsic TNF receptor 1 (p55, TNFR1). In contrast, we show that T cell-induced hepatitis was independent of TNFR1 signaling in hepatocytes, T cells, or endothelial cells. Moreover, T cell-induced hepatitis was independent of hepatocyte-intrinsic Fas-associated protein with death domain, TNF-related apoptosis-inducing ligand receptor, or Fas signaling. Instead, concanavalin A-induced hepatitis was completely prevented in mice with myeloid-derived cell (MDC)-specific deletion of TNFR1. Significantly, however, mice lacking TNFR1 in MDCs succumbed to listeria infection, although they displayed similar sensitivity toward endotoxin-induced septic shock when compared to control mice. These results suggest that TNFR1 signaling in MDCs is a critical mediator of both the detrimental and the protective functions of TNF in T cell-induced hepatitis and bacterial infection, respectively. CONCLUSION The critical site of action of DRs is completely dependent on the nature of hepatitis; the data specify MDCs as the essential cell type of TNFR1 function in T cell-mediated hepatitis and in the response to listeria, thereby identifying the opposing role of MDC TNFR1 in autoimmunity and bacterial infection. (Hepatology 2016;64:508-521).

Published
2016

35. A novel liposomal Clodronate depletes tumor-associated macrophages in primary and metastatic melanoma: Anti-angiogenic and anti-tumor effects

Author

Laura Emionite, Monica Loi, Emanuela Ognio, Patrizia Perri, Vangelis Kondylis, Antonio Daga, Fabian Schorn, Irene Cossu, Chiara Brignole, Domenico Ribatti, Manolis Pasparakis, Daniele Murgia, Fabio Pastorino, Francesca Piaggio, Federica Raggi, Christian Marinaccio, Mirco Ponzoni, and Daniela Di Paolo

Subjects
0301 basic medicine, Cell Survival, Angiogenesis, Melanoma, Experimental, Pharmaceutical Science, Antineoplastic Agents, Apoptosis, Mice, Transgenic, Spleen, Inflammation, Cell Line, Fatty Acids, Monounsaturated, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Cell Proliferation, Cell growth, business.industry, Macrophages, Melanoma, Fibroblasts, medicine.disease, Tumor Burden, Quaternary Ammonium Compounds, 030104 developmental biology, medicine.anatomical_structure, Liver, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Liposomes, Immunology, Cancer research, Cytokines, Clodronic acid, Female, Clodronic Acid, medicine.symptom, business, medicine.drug
Abstract

The depletion of tumor-associated macrophages (TAMs), involved in different stages of cancer development and progression, is an appealing strategy in cancer therapy. We developed novel Clodronate-containing liposomes (Clo-Lipo-DOTAP) presenting physicochemical properties (size distribution, polydispersity index and Z-potential) suited for safe storage and injections. In vitro, Clo-Lipo-DOTAP inhibited proliferation, reduced viability and induced apoptosis of a macrophage-like cell line in a dose- and time-dependent manner. In proof of functionality experiments, Clo-Lipo-DOTAP depleted macrophages in a genetic mouse model of chronic hepatitis and hepatocellular carcinoma leading to a significant reduction of F4/80-positive cells in the liver and spleen of treated mice compared to PBS-treated controls. The number of granulocytes, B and T lymphocytes was not affected. In B16/F10 subcutaneous melanoma-bearing mice, Clo-Lipo-DOTAP significantly reduced the volume of primary tumors (P In conclusion, the depletion of TAMs in primary and metastatic melanoma presents anti-tumor efficacy via inhibition of angiogenesis and modulation of inflammation related cytokines.

Published
2016

36. The pseudokinase MLKL activates PAD4-dependent NET formation in necroptotic neutrophils

Author

Mathilde Gavillet, Shu Wang, Ben A. Croker, David A. Williams, Michelle A. Kelliher, Meghan Bliss-Moreau, Sylvia Dietrich, Manolis Pasparakis, Alyce A. Chen, Akshay A. D’Cruz, Mary Speir, James E Vince, Arshed Al-Obeidi, Kate E. Lawlor, Maria Ericsson, and Razq Hakem

Subjects
0301 basic medicine, Methicillin-Resistant Staphylococcus aureus, Programmed cell death, Neutrophils, Apoptosis, Biochemistry, Cytoplast, Extracellular Traps, Article, Histones, 03 medical and health sciences, RIPK1, Microscopy, Electron, Transmission, Protein-Arginine Deiminase Type 4, Animals, Humans, Viability assay, Molecular Biology, Cells, Cultured, Mice, Knockout, Caspase 8, biology, Chemistry, Cell Biology, Neutrophil extracellular traps, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Histone, Cytoplasm, Receptor-Interacting Protein Serine-Threonine Kinases, biology.protein, Protein-Arginine Deiminases, Protein Kinases
Abstract

Neutrophil extracellular trap (NET) formation can generate short-term, functional anucleate cytoplasts and trigger loss of cell viability. We demonstrated that the necroptotic cell death effector mixed lineage kinase domain–like (MLKL) translocated from the cytoplasm to the plasma membrane and stimulated downstream NADPH oxidase– independent ROS production, loss of cytoplasmic granules, breakdown of the nuclear membrane, chromatin decondensation, histone hypercitrullination, and extrusion of bacteriostatic NETs. This process was coordinated by receptor-interacting protein kinase-1 (RIPK1), which activated the caspase-8–dependent apoptotic or RIPK3/ MLKL-dependent necroptotic death of mouse and human neutrophils. Genetic deficiency of RIPK3 and MLKL prevented NET formation but did not prevent cell death, which was because of residual caspase-8–dependent activity. Peptidylarginine deiminase 4 (PAD4) was activated downstream of RIPK1/RIPK3/MLKL and was required for maximal histone hypercitrullination and NET extrusion. This work defines a distinct signaling network that activates PAD4-dependent NET release for the control of methicillin-resistant Staphylococcus aureus (MRSA) infection.

Published
2018

37. RIP Kinases in Liver Cell Death, Inflammation and Cancer

Author

Manolis Pasparakis and Vangelis Kondylis

Subjects
0301 basic medicine, Programmed cell death, Necroptosis, Biology, 03 medical and health sciences, Liver disease, RIPK1, Necrosis, 0302 clinical medicine, Neoplasms, medicine, Animals, Humans, Protein kinase A, Molecular Biology, Cell Death, Kinase, Liver cell, Liver Diseases, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Liver, Hepatocyte, Cancer research, Molecular Medicine, 030217 neurology & neurosurgery
Abstract

Cell death is intrinsically linked to inflammatory liver disease and cancer development. Recent genetic studies have suggested that receptor-interacting protein kinase (RIPK)1 is implicated in liver disease pathogenesis by regulating caspase-dependent hepatocyte apoptosis induced by tumor necrosis factor (TNF) or other stimuli. In contrast, the contribution of caspase-independent RIPK3/mixed lineage kinase like (MLKL)-mediated hepatocyte necroptosis remains debatable. Hepatocyte apoptosis depends on the balance between RIPK1 prosurvival scaffolding functions and its kinase-activity-mediated proapoptotic function. Several regulatory steps promote the prosurvival role of RIPK1, including phosphorylation and ubiquitination of RIPK1 itself and other molecules involved in RIPK1 signaling. Pharmacological inhibition of liver damage by targeting RIPK1 signaling emerges as a potential therapeutic strategy to prevent chronic liver inflammation and hepatocarcinogenesis.

Published
2018

38. Connecting immune deficiency and inflammation

Author

Michelle A. Kelliher and Manolis Pasparakis

Subjects
0301 basic medicine, Inflammation, Multidisciplinary, business.industry, MEDLINE, Immunologic Deficiency Syndromes, Article, 03 medical and health sciences, 030104 developmental biology, Immune system, Immunology, medicine, Humans, medicine.symptom, business
Abstract

Receptor Interacting Serine/Threonine Kinase 1 (RIPK1) is a master regulator of signaling pathways leading to inflammation and cell death and is of medical interest as a drug target. Here, we report four patients from three unrelated families with complete RIPK1 deficiency caused by rare homozygous mutations. The patients suffered from recurrent infections, early-onset inflammatory bowel disease and progressive polyarthritis. They had immunodeficiency with lymphopenia and altered production of various cytokines revealed by whole-blood assays. In vitro, RIPK1-deficient cells showed impaired MAPK activation and cytokine secretion and were prone to necroptosis. Hematopoietic stem cell transplantation reversed cytokine production defects and resolved clinical symptoms in one patient. Thus, RIPK1 plays a critical role in the human immune system.

Published
2018

39. 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

40. Corticosteroids inhibit Mycobacterium tuberculosis-induced necrotic host cell death by abrogating mitochondrial membrane permeability transition

Author

Sandra Winter, Anna Esser, Marc Herb, Christian P. Pallasch, Edeltraud van Gumpel, Laurens Wachsmuth, Christoph Hölscher, Michael Schramm, Jessica Gräb, Melanie Fritsch, Manolis Pasparakis, Hamid Kashkar, Jan Rybniker, Fynn Schreiber, and Isabelle Suárez

Subjects
0301 basic medicine, Tuberculosis, p38 mitogen-activated protein kinases, Necroptosis, Science, General Physics and Astronomy, 02 engineering and technology, p38 Mitogen-Activated Protein Kinases, General Biochemistry, Genetics and Molecular Biology, Dexamethasone, Article, Mycobacterium tuberculosis, 03 medical and health sciences, Adrenal Cortex Hormones, Medicine, Humans, Phosphorylation, lcsh:Science, Protein kinase A, Receptor, Multidisciplinary, biology, business.industry, General Chemistry, 021001 nanoscience & nanotechnology, medicine.disease, biology.organism_classification, 030104 developmental biology, Receptors, Tumor Necrosis Factor, Type I, Mitochondrial Membranes, Cancer research, lcsh:Q, Tumor necrosis factor alpha, Tumor necrosis factor receptor 1, 0210 nano-technology, business, Signal Transduction
Abstract

Corticosteroids are host-directed drugs with proven beneficial effect on survival of tuberculosis (TB) patients, but their precise mechanisms of action in this disease remain largely unknown. Here we show that corticosteroids such as dexamethasone inhibit necrotic cell death of cells infected with Mycobacterium tuberculosis (Mtb) by facilitating mitogen-activated protein kinase phosphatase 1 (MKP-1)-dependent dephosphorylation of p38 MAPK. Characterization of infected mixed lineage kinase domain-like (MLKL) and tumor necrosis factor receptor 1 (TNFR1) knockout cells show that the underlying mechanism is independent from TNFα-signaling and necroptosis. Our results link corticosteroid function and p38 MAPK inhibition to abrogation of necrotic cell death mediated by mitochondrial membrane permeability transition, and open new avenues for research on novel host-directed therapies (HDT)., Corticosteroids are host-directed drugs that enhance survival of tuberculosis patients through unclear mechanisms. Here, Gräb et al. show that corticosteroids inhibit necrotic death of cells infected with Mycobacterium tuberculosis by facilitating MKP-1-dependent dephosphorylation of p38 MAPK.

Published
2018

41. Correction: Dendritic Cell RIPK1 Maintains Immune Homeostasis by Preventing Inflammation and Autoimmunity

Author

Justine E. Roderick, Michelle A. Kelliher, Ciara G. Doran, Matija Zelic, Joanne A. O’Donnell, Dalia Martinez-Marin, Manolis Pasparakis, Katherine A. Fitzgerald, Stephen Lyle, Jesse Lehman, Nicole Hermance, and Ann Marshak-Rothstein

Subjects
0106 biological sciences, 0301 basic medicine, business.industry, Immunology, chemical and pharmacologic phenomena, Inflammation, Dendritic cell, 030108 mycology & parasitology, medicine.disease_cause, 01 natural sciences, Article, Autoimmunity, 010602 entomology, 03 medical and health sciences, RIPK1, Immunology and Allergy, Medicine, Immune homeostasis, medicine.symptom, business
Abstract

Necroptosis is a form of cell death associated with inflammation, however the biological consequences of chronic necroptosis are unknown. Necroptosis is mediated by RIPK1, RIPK3 and MLKL kinases but in hematopoietic cells RIPK1 has anti-inflammatory roles and functions to prevent necroptosis. Here we interrogate the consequences of chronic necroptosis on immune homeostasis by deleting Ripk1 in mouse dendritic cells (DC). We demonstrate that deregulated necroptosis results in systemic inflammation, tissue fibrosis and autoimmunity. We show that inflammation and autoimmunity are prevented upon expression of kinase inactive RIPK1 or deletion of RIPK3 or MLKL. We provide evidence that the inflammation is not driven by microbial ligands, but depends on the release of danger-associated molecular patterns (DAMPs) and MyD88-dependent signaling. Importantly, whilst the inflammation is independent of type I interferon and the nucleic acid sensing TLRs, blocking these pathways rescues the autoimmunity. These mouse genetic studies reveal that chronic necroptosis may underlie human fibrotic and autoimmune disorders.

Published
2018

42. Innate Sensing by Mesenchymal TLR4/MyD88 Signals Promotes Spontaneous Intestinal Tumorigenesis

Author

Vasiliki Koliaraki, Apostolos Polykratis, Niki Chalkidi, David J. Hackam, Ari Waisman, Manolis Pasparakis, Werner Muller, Ana Henriques, Christos Tzaferis, and George Kollias

Subjects
Stroma, Mesenchymal stem cell, Knockout mouse, Gene expression, medicine, TLR4, Biology, Carcinogenesis, medicine.disease_cause, Phenotype, Ex vivo, Cell biology
Abstract

MyD88, an adaptor molecule downstream of innate pathways, plays a significant tumor-promoting role in sporadic intestinal carcinogenesis, which is dependent on its function in the stroma. Here, we show that deletion of MyD88 in intestinal mesenchymal cells (IMCs) significantly reduces Apc-mediated intestinal tumorigenesis. This phenotype is associated with decreased epithelial cell proliferation, altered inflammatory and tumorigenic immune cell infiltration, and modified gene expression similar to complete MyD88 knockout mice. Genetic deletion of TLR4, but not IL1R, in IMCs led to altered molecular profiles and reduction of intestinal tumors similar to the MyD88 deficiency. Ex vivo analysis in IMCs indicated that these effects are mediated through downstream signals involving growth factors, inflammatory and ECM-regulating genes, also found in human cancer-associated fibroblasts (CAFs). Our results provide the first direct evidence that during tumorigenesis, IMCs and CAFs are activated by innate TLR4/MyD88-mediated signals and respond to promote carcinogenesis in the intestine.

Published
2018

43. ATG16L1 orchestrates interleukin-22 signaling in the intestinal epithelium via cGAS–STING

Author

Anne Luzius, Svetlana Saveljeva, Robin Schwarzer, Go Ito, Konrad Aden, Markus Tschurtschenthaler, Stefan Schreiber, Stefan Krautwald, Arthur Kaser, Johannes Kuiper, Joya Bhattacharyya, Kareen Bartsch, Florian Tran, Philip Rosenstiel, Robert Häsler, Gunther Hartmann, Richard S. Blumberg, Maren Falk-Paulsen, Manolis Pasparakis, Stephanie T. Stengel, Lina Welz, Björn Rabe, Marlene Jentzsch, Raheleh Sheibani-Tezerji, Winfried Barchet, and Simone Lipinski

Subjects
0301 basic medicine, XBP1, medicine.medical_treatment, Immunology, Autophagy-Related Proteins, Biology, Article, Interleukin 22, Mice, 03 medical and health sciences, Intestinal mucosa, medicine, Animals, Humans, Immunology and Allergy, Intestinal Mucosa, Research Articles, Mice, Knockout, Interleukins, Autophagy, Genetic Variation, Membrane Proteins, Inflammatory Bowel Diseases, Nucleotidyltransferases, Intestinal epithelium, ddc, 3. Good health, Cell biology, 030104 developmental biology, Cytokine, Unfolded protein response, Caco-2 Cells, Signal transduction, Carrier Proteins, Signal Transduction
Abstract

Dysregulated autophagy and ER stress are involved in the etiology of human IBD. Aden et al. show that loss of ATG16L1 function renders intestinal epithelial cells vulnerable to IL-22–induced ER stress and necroptosis via STING signaling, which induces ileal inflammation in vivo., A coding variant of the inflammatory bowel disease (IBD) risk gene ATG16L1 has been associated with defective autophagy and deregulation of endoplasmic reticulum (ER) function. IL-22 is a barrier protective cytokine by inducing regeneration and antimicrobial responses in the intestinal mucosa. We show that ATG16L1 critically orchestrates IL-22 signaling in the intestinal epithelium. IL-22 stimulation physiologically leads to transient ER stress and subsequent activation of STING-dependent type I interferon (IFN-I) signaling, which is augmented in Atg16l1ΔIEC intestinal organoids. IFN-I signals amplify epithelial TNF production downstream of IL-22 and contribute to necroptotic cell death. In vivo, IL-22 treatment in Atg16l1ΔIEC and Atg16l1ΔIEC/Xbp1ΔIEC mice potentiates endogenous ileal inflammation and causes widespread necroptotic epithelial cell death. Therapeutic blockade of IFN-I signaling ameliorates IL-22–induced ileal inflammation in Atg16l1ΔIEC mice. Our data demonstrate an unexpected role of ATG16L1 in coordinating the outcome of IL-22 signaling in the intestinal epithelium., Graphical Abstract

Published
2018
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44. NEMO Prevents Steatohepatitis and Hepatocellular Carcinoma by Inhibiting RIPK1 Kinase Activity-Mediated Hepatocyte Apoptosis

Author

Hanno Ehlken, Trieu-My Van, Santosh Krishna-Subramanian, Manolis Pasparakis, Peter Schirmacher, Laura Ochoa-Callejero, Michelle A. Kelliher, Beate K. Straub, Vangelis Kondylis, Ulf Klein, HM Curth, Apostolos Polykratis, Nicole Heise, and Falk Weih

Subjects
Cancer Research, Carcinoma, Hepatocellular, Immunoblotting, Gene Expression, Apoptosis, IκB kinase, Biology, Article, 03 medical and health sciences, RIPK1, 0302 clinical medicine, medicine, Animals, Kinase activity, Protein kinase A, Cells, Cultured, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Reverse Transcriptase Polymerase Chain Reaction, business.industry, RELB, Liver Neoplasms, I-Kappa-B Kinase, Intracellular Signaling Peptides and Proteins, NF-kappa B, Cell Biology, medicine.disease, TRADD, Immunohistochemistry, I-kappa B Kinase, 3. Good health, Fatty Liver, Mice, Inbred C57BL, Liver, Oncology, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Cancer cell, Hepatocytes, Cancer research, Signal transduction, Steatohepatitis, Hepatocyte apoptosis, business, Signal Transduction
Abstract

Summary IκB kinase/nuclear factor κB (IKK/NF-κB) signaling exhibits important yet opposing functions in hepatocarcinogenesis. Mice lacking NEMO in liver parenchymal cells (LPC) spontaneously develop steatohepatitis and hepatocellular carcinoma (HCC) suggesting that NF-κB prevents liver disease and cancer. Here, we show that complete NF-κB inhibition by combined LPC-specific ablation of RelA, c-Rel, and RelB did not phenocopy NEMO deficiency, but constitutively active IKK2-mediated NF-κB activation prevented hepatocellular damage and HCC in NEMOLPC-KO mice. Knock-in expression of kinase inactive receptor-interacting protein kinase 1 (RIPK1) prevented hepatocyte apoptosis and HCC, while RIPK1 ablation induced TNFR1-associated death domain protein (TRADD)-dependent hepatocyte apoptosis and liver tumors in NEMOLPC-KO mice, revealing distinct kinase-dependent and scaffolding functions of RIPK1. Collectively, these results show that NEMO prevents hepatocarcinogenesis by inhibiting RIPK1 kinase activity-driven hepatocyte apoptosis through NF-κB-dependent and -independent functions., Graphical Abstract, Highlights • NF-κB inhibition in LPCs does not cause spontaneous HCC in contrast to NEMO ablation • Constitutive IKK2/NF-κB activation prevents liver damage and HCC in NEMOLPC-KO mice • RIPK1 kinase activity-mediated hepatocyte apoptosis drives HCC in NEMOLPC-KO mice • NEMO prevents formation of a RIPK1/FADD/Casp8 complex inducing hepatocyte apoptosis, Kondylis et al. identify an NF-κB-independent function of NEMO in controlling RIPK1 kinase activity-dependent apoptosis of hepatocytes and thus hepatocarcinogenesis. NEMO-mediated NF-κB activity and kinase activity-independent scaffold function of RIPK1 also regulate hepatocyte apoptosis.

Published
2015
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45. Brain endothelial TAK1 and NEMO safeguard the neurovascular unit

Author

Marc Schmidt-Supprian, Kristin Müller, Beate Lembrich, Manolis Pasparakis, Stijn Stroobants, Barry J. Bedell, Hartwig Wolburg, Lydia Sorokin, Markus Schwaninger, François Truchetet, Kathrin Töllner, Dirk Rades, Xin-Kang Tong, Jan Wenzel, Tobias Weber, Rudi D'Hooge, Lisanne Fischer, Panayiota Papadopoulos, Wolfgang Löscher, Cristina Elena Niturad, Dirk A. Ridder, Marilyn Grand'Maison, Julian C. Assmann, Eva Korpos, Edith Hamel, Detlef Balschun, Faculty of Economic and Social Sciences and Solvay Business School, and Neurology

Subjects
Male, Transcription Factor RelA/metabolism, Occludin, Epilepsy/genetics, 0302 clinical medicine, Immunology and Allergy, TNF Receptor-Associated Factor 6/metabolism, skin and connective tissue diseases, Medicine(all), Mice, Knockout, MAP Kinase Kinase Kinases/genetics, 0303 health sciences, Tight junction, I-kappa B Kinase/metabolism, Intracellular Signaling Peptides and Proteins, Brain, Incontinentia pigmenti, MAP Kinase Kinase Kinases, I-kappa B Kinase, 3. Good health, Cell biology, Endothelial stem cell, medicine.anatomical_structure, Blood-Brain Barrier, Cerebrovascular Circulation, Female, Signal transduction, Blood-Brain Barrier/metabolism, congenital, hereditary, and neonatal diseases and abnormalities, Immunology, Mice, Transgenic, Endothelial Cells/metabolism, Biology, Blood–brain barrier, Brain/blood supply, Article, 03 medical and health sciences, Incontinentia Pigmenti/metabolism, medicine, Occludin/metabolism, Animals, Incontinentia Pigmenti, Transcription factor, 030304 developmental biology, TNF Receptor-Associated Factor 6, Epilepsy, MAP kinase kinase kinase, Transcription Factor RelA, Endothelial Cells, Cell Biology, medicine.disease, Mice, Inbred C57BL, sense organs, Intracellular Signaling Peptides and Proteins/genetics, 030217 neurology & neurosurgery, Cerebrovascular Circulation/genetics, 030215 immunology
Abstract

Ridder et al. show that deletion of NEMO, a component of NF-kB signaling, in brain endothelial cells results in increased cerebral vascular permeability and endothelial cell death, and recapitulates the neurological symptoms observed in the genetic disease incontinentia pigmenti., Inactivating mutations of the NF-κB essential modulator (NEMO), a key component of NF-κB signaling, cause the genetic disease incontinentia pigmenti (IP). This leads to severe neurological symptoms, but the mechanisms underlying brain involvement were unclear. Here, we show that selectively deleting Nemo or the upstream kinase Tak1 in brain endothelial cells resulted in death of endothelial cells, a rarefaction of brain microvessels, cerebral hypoperfusion, a disrupted blood–brain barrier (BBB), and epileptic seizures. TAK1 and NEMO protected the BBB by activating the transcription factor NF-κB and stabilizing the tight junction protein occludin. They also prevented brain endothelial cell death in a NF-κB–independent manner by reducing oxidative damage. Our data identify crucial functions of inflammatory TAK1–NEMO signaling in protecting the brain endothelium and maintaining normal brain function, thus explaining the neurological symptoms associated with IP.

Published
2015

46. Hematopoietic stem cell quiescence and function are controlled by the CYLD–TRAF2–p38MAPK pathway

Author

Yilang Tang, Massimo Saini, Ari Waisman, Melania Tesio, Elizabeth Macintyre, Andreas Trumpp, Lisa von Paleske, Katja Müdder, and Manolis Pasparakis

Subjects
TRAF2, Tumor suppressor gene, MAP Kinase Signaling System, Immunology, Regulator, Biology, p38 Mitogen-Activated Protein Kinases, Article, Mice, medicine, Animals, Immunology and Allergy, Mice, Knockout, Regulation of gene expression, NF-kappa B, Hematopoietic stem cell, Cell Biology, Hematopoietic Stem Cells, TNF Receptor-Associated Factor 2, Phenotype, Deubiquitinating Enzyme CYLD, Cell biology, Cysteine Endopeptidases, Haematopoiesis, medicine.anatomical_structure, Gene Expression Regulation, Mutation, Stem cell
Abstract

Tesio at al. identify a novel pathway controlled by the tumor suppressor and deubiquitinase cylindromatosis (CYLD), which is involved in the regulation of hematopoietic stem cell quiescence and repopulation potential., The status of long-term quiescence and dormancy guarantees the integrity of hematopoietic stem cells (HSCs) during adult homeostasis. However the molecular mechanisms regulating HSC dormancy remain poorly understood. Here we show that cylindromatosis (CYLD), a tumor suppressor gene and negative regulator of NF-κB signaling with deubiquitinase activity, is highly expressed in label-retaining dormant HSCs (dHSCs). Moreover, Cre-mediated conditional elimination of the catalytic domain of CYLD induced dHSCs to exit quiescence and abrogated their repopulation and self-renewal potential. This phenotype is dependent on the interactions between CYLD and its substrate TRAF2 (tumor necrosis factor–associated factor 2). HSCs expressing a mutant CYLD with an intact catalytic domain, but unable to bind TRAF2, showed the same HSC phenotype. Unexpectedly, the robust cycling of HSCs lacking functional CYLD–TRAF2 interactions was not elicited by increased NF-κB signaling, but instead by increased activation of the p38MAPK pathway. Pharmacological inhibition of p38MAPK rescued the phenotype of CYLD loss, identifying the CYLD–TRAF2–p38MAPK pathway as a novel important regulator of HSC function restricting HSC cycling and promoting dormancy.

Published
2015

47. The Cdkn1a

Author

Alessandro, Torgovnick, Jan Michel, Heger, Vasiliki, Liaki, Jörg, Isensee, Anna, Schmitt, Gero, Knittel, Arina, Riabinska, Filippo, Beleggia, Lucie, Laurien, Uschi, Leeser, Christian, Jüngst, Florian, Siedek, Wenzel, Vogel, Niklas, Klümper, Hendrik, Nolte, Maike, Wittersheim, Lars, Tharun, Roberta, Castiglione, Marcus, Krüger, Astrid, Schauss, Sven, Perner, Manolis, Pasparakis, Reinhard, Büttner, Thorsten, Persigehl, Tim, Hucho, Grit Sophie, Herter-Sprie, Björn, Schumacher, and Hans Christian, Reinhardt

Subjects
Cyclin-Dependent Kinase Inhibitor p21, Carcinogenesis, Gene Dosage, Apoptosis, Mice, Transgenic, Cell Cycle Checkpoints, Fibroblasts, Embryo, Mammalian, Epithelium, Mice, Inbred C57BL, Mice, Cytoprotection, Drug Resistance, Neoplasm, Animals, Regeneration, Tumor Suppressor Protein p53, DNA Damage
Abstract

Cdkn1a, which encodes p21, functions as a major route for p53-mediated cell-cycle arrest. However, the consequence of Cdkn1a gene dosage on tumor suppression has not been systematically investigated. Here, we employed BAC transgenesis to generate a Cdkn1a

Published
2017

48. MK2 Phosphorylates RIPK1 to Prevent TNF-Induced Cell Death

Author

Isabel, Jaco, Alessandro, Annibaldi, Najoua, Lalaoui, Rebecca, Wilson, Tencho, Tenev, Lucie, Laurien, Chun, Kim, Kunzah, Jamal, Sidonie, Wicky John, Gianmaria, Liccardi, Diep, Chau, James M, Murphy, Gabriela, Brumatti, Rebecca, Feltham, Manolis, Pasparakis, John, Silke, and Pascal, Meier

Subjects
RIPK1, Fas-Associated Death Domain Protein, TNF, necroptosis, Apoptosis, p38, Protein Serine-Threonine Kinases, Transfection, Article, caspase-8, MK2, Mitogen-Activated Protein Kinase 14, Necrosis, cytokine, Animals, Humans, Phosphorylation, complex-II, Mice, Knockout, Caspase 8, Dose-Response Relationship, Drug, Tumor Necrosis Factor-alpha, Intracellular Signaling Peptides and Proteins, NF-kappa B, MAP Kinase Kinase Kinases, Mice, Inbred C57BL, IAPs, cell death, Multiprotein Complexes, Receptor-Interacting Protein Serine-Threonine Kinases, RNA Interference, HT29 Cells, Signal Transduction
Abstract

Summary TNF is an inflammatory cytokine that upon binding to its receptor, TNFR1, can drive cytokine production, cell survival, or cell death. TNFR1 stimulation causes activation of NF-κB, p38α, and its downstream effector kinase MK2, thereby promoting transcription, mRNA stabilization, and translation of target genes. Here we show that TNF-induced activation of MK2 results in global RIPK1 phosphorylation. MK2 directly phosphorylates RIPK1 at residue S321, which inhibits its ability to bind FADD/caspase-8 and induce RIPK1-kinase-dependent apoptosis and necroptosis. Consistently, a phospho-mimetic S321D RIPK1 mutation limits TNF-induced death. Mechanistically, we find that phosphorylation of S321 inhibits RIPK1 kinase activation. We further show that cytosolic RIPK1 contributes to complex-II-mediated cell death, independent of its recruitment to complex-I, suggesting that complex-II originates from both RIPK1 in complex-I and cytosolic RIPK1. Thus, MK2-mediated phosphorylation of RIPK1 serves as a checkpoint within the TNF signaling pathway that integrates cell survival and cytokine production., Graphical Abstract, Highlights • Phosphorylation of RIPK1 by MK2 acts as survival checkpoint in TNF signaling • TNF-induced activation of MK2 results in global RIPK1 phosphorylation • MK2-mediated phosphorylation suppresses RIPK1 kinase activation and cell death • Complex-II originates from RIPK1 in complex-I as well as cytosolic RIPK1, Jaco et al. show that MK2 directly phosphorylates RIPK1 at residue S321, suppressing the cytotoxic potential of RIPK1 and acting as a checkpoint within the TNF signaling pathway.

Published
2017

49. Epidermal p65/ <scp>NF</scp> ‐κB signalling is essential for skin carcinogenesis

Author

Manolis Pasparakis and Chun Kim

Subjects
Keratinocytes, Skin Neoplasms, Carcinogenesis, 9,10-Dimethyl-1,2-benzanthracene, NF-κB signalling, DMBA, Inflammation, Biology, medicine.disease_cause, Proinflammatory cytokine, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Research Articles, Skin, 030304 developmental biology, 0303 health sciences, integumentary system, skin carcinogenesis, NF-kappa B, Transcription Factor RelA, apoptosis, NFKB1, Molecular biology, Hedgehog signaling pathway, mouse models of cancer, 3. Good health, inflammation, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, medicine.symptom, Signal transduction, Gene Deletion, Signal Transduction
Abstract

The nuclear factor kappa B (NF-κB) signalling pathway exhibits both tumour-promoting and tumour-suppressing functions in different tissues and models of carcinogenesis. In particular in epidermal keratinocytes, NF-κB signalling was reported to exert primarily growth inhibitory and tumour-suppressing functions. Here, we show that mice with keratinocyte-restricted p65/RelA deficiency were resistant to 7, 12-dimethylbenz(a)anthracene (DMBA)-/12-O-tetra decanoylphorbol-13 acetate (TPA)-induced skin carcinogenesis. p65 deficiency sensitized epidermal keratinocytes to DNA damage-induced death in vivo and in vitro, suggesting that inhibition of p65-dependent prosurvival functions prevented tumour initiation by facilitating the elimination of cells carrying damaged DNA. In addition, lack of p65 strongly inhibited TPA-induced epidermal hyperplasia and skin inflammation by suppressing the expression of proinflammatory cytokines and chemokines by epidermal keratinocytes. Therefore, p65-dependent NF-κB signalling in keratinocytes promotes DMBA-/TPA-induced skin carcinogenesis by protecting keratinocytes from DNA damage-induced death and facilitating the establishment of a tumour-nurturing proinflammatory microenvironment.

Published
2014

50. Kinase-independent functions of RIPK1 regulate hepatocyte survival and liver carcinogenesis

Author

Vangelis Kondylis, Apostolos Polykratis, Manolis Pasparakis, Beate K. Straub, Nikoletta Papadopoulou, and Trieu-My Van

Subjects
0301 basic medicine, Programmed cell death, Liver tumor, Cell Survival, Necroptosis, Mice, Transgenic, Biology, Chronic liver disease, Proinflammatory cytokine, 03 medical and health sciences, Liver disease, Mice, Liver Neoplasms, Experimental, medicine, Animals, Diethylnitrosamine, Kinase activity, Transcription Factor RelA, General Medicine, medicine.disease, 3. Good health, Neoplasm Proteins, 030104 developmental biology, medicine.anatomical_structure, Cell Transformation, Neoplastic, Receptors, Tumor Necrosis Factor, Type I, Hepatocyte, Receptor-Interacting Protein Serine-Threonine Kinases, Cancer research, Hepatocytes, Signal Transduction, Research Article
Abstract

The mechanisms that regulate cell death and inflammation play an important role in liver disease and cancer. Receptor-interacting protein kinase 1 (RIPK1) induces apoptosis and necroptosis via kinase-dependent mechanisms and exhibits kinase-independent prosurvival and proinflammatory functions. Here, we have used genetic mouse models to study the role of RIPK1 in liver homeostasis, injury, and cancer. While ablating either RIPK1 or RelA in liver parenchymal cells (LPCs) did not cause spontaneous liver pathology, mice with combined deficiency of RIPK1 and RelA in LPCs showed increased hepatocyte apoptosis and developed spontaneous chronic liver disease and cancer that were independent of TNF receptor 1 (TNFR1) signaling. In contrast, mice with LPC-specific knockout of Ripk1 showed reduced diethylnitrosamine-induced (DEN-induced) liver tumorigenesis that correlated with increased DEN-induced hepatocyte apoptosis. Lack of RIPK1 kinase activity did not inhibit DEN-induced liver tumor formation, showing that kinase-independent functions of RIPK1 promote DEN-induced hepatocarcinogenesis. Moreover, mice lacking both RIPK1 and TNFR1 in LPCs displayed normal tumor formation in response to DEN, demonstrating that RIPK1 deficiency decreases DEN-induced liver tumor formation in a TNFR1-dependent manner. Therefore, these findings indicate that RIPK1 cooperates with NF-κB signaling to prevent TNFR1-independent hepatocyte apoptosis and the development of chronic liver disease and cancer, but acts downstream of TNFR1 signaling to promote DEN-induced liver tumorigenesis.

Published
2016

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