Your search keyword '"STAT1 Transcription Factor"' showing total 7,960 results

1. Opposing tumor-cell-intrinsic and -extrinsic roles of the IRF1 transcription factor in antitumor immunity

Author

Purbey, Prabhat K, Seo, Joowon, Paul, Manash K, Iwamoto, Keisuke S, Daly, Allison E, Feng, An-Chieh, Champhekar, Ameya S, Langerman, Justin, Campbell, Katie M, Schaue, Dörthe, McBride, William H, Dubinett, Steven M, Ribas, Antoni, Smale, Stephen T, and Scumpia, Philip O

Subjects

Biological Sciences, Immunotherapy, Genetics, Cancer, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Inflammatory and immune system, Animals, Humans, Mice, B7-H1 Antigen, Cell Line, Tumor, Immunity, Interferon Regulatory Factor-1, Mice, Inbred C57BL, Neoplasms, STAT1 Transcription Factor, Male, Female, CP: Cancer, CP: Immunology, IRF1, PD-L1 regulation, TLR signaling, antitumor immunity, cytotoxic T lymphocytes, immune checkpoint blockade, immune evasion, interferon signaling, scRNA-seq, transcription, Biochemistry and Cell Biology, Medical Physiology, Biological sciences

Abstract

Type I interferon (IFN-I) and IFN-γ foster antitumor immunity by facilitating T cell responses. Paradoxically, IFNs may promote T cell exhaustion by activating immune checkpoints. The downstream regulators of these disparate responses are incompletely understood. Here, we describe how interferon regulatory factor 1 (IRF1) orchestrates these opposing effects of IFNs. IRF1 expression in tumor cells blocks Toll-like receptor- and IFN-I-dependent host antitumor immunity by preventing interferon-stimulated gene (ISG) and effector programs in immune cells. In contrast, expression of IRF1 in the host is required for antitumor immunity. Mechanistically, IRF1 binds distinctly or together with STAT1 at promoters of immunosuppressive but not immunostimulatory ISGs in tumor cells. Overexpression of programmed cell death ligand 1 (PD-L1) in Irf1-/- tumors only partially restores tumor growth, suggesting multifactorial effects of IRF1 on antitumor immunity. Thus, we identify that IRF1 expression in tumor cells opposes host IFN-I- and IRF1-dependent antitumor immunity to facilitate immune escape and tumor growth.

Published

2024

2. N-MYC-interacting protein enhances type II interferon signaling by inhibiting STAT1 sumoylation.

Author

Linyuan Feng, Wanwei Li, Xiaowen Li, Xiaotian Li, Yanhong Ran, Xiaoping Yang, Zemin Deng, and Hongjian Li

Abstract

Signaling desensitization is key to limiting signal transduction duration and intensity. Signal transducer and activator of transcription 1 (STAT1) can mediate type II interferon (IFNγ)-induced immune responses, which are enhanced and inhibited by STAT1 phosphorylation and sumoylation, respectively. Here, we identified an N-MYC interacting protein, NMI, which can enhance STAT1 phosphorylation and STAT1-mediated IFNγ immune responses by binding and sequestering the E2 SUMO conjugation enzyme, UBC9, and blocking STAT1 sumoylation. NMI facilitates UBC9 nucleus-to-cytoplasm translocation in response to IFNγ, thereby inhibiting STAT1 sumoylation. STAT1 phosphorylation at Y701 and sumoylation at K703 are mutually exclusive modifications that regulate IFNγ-dependent transcriptional responses. NMI could not alter the phosphorylation level of sumoylation-deficient STAT1 after IFNγ treatment. Thus, IFNγ signaling is modulated by NMI through sequestration of UBC9 in the cytoplasm, leading to inhibition of STAT1 sumoylation. Hence, NMI functions as a switch for STAT1 activation/inactivation cycles by modulating an IFNγ-induced desensitization mechanism. [ABSTRACT FROM AUTHOR]

Published

2023

3. BRD9 regulates interferon-stimulated genes during macrophage activation via cooperation with BET protein BRD4

Author

Ahmed, Nasiha S, Gatchalian, Jovylyn, Ho, Josephine, Burns, Mannix J, Hah, Nasun, Wei, Zong, Downes, Michael, Evans, Ronald M, and Hargreaves, Diana C

Subjects

Biochemistry and Cell Biology, Biological Sciences, Human Genome, Genetics, Infectious Diseases, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Underpinning research, Aetiology, Antiviral Agents, Cell Cycle Proteins, Chromatin Assembly and Disassembly, Humans, Interferon-Stimulated Gene Factor 3, gamma Subunit, Interferon-alpha, Interferons, Macrophage Activation, Promoter Regions, Genetic, Protein Domains, STAT1 Transcription Factor, STAT2 Transcription Factor, Transcription Factors, Transcriptional Activation, inflammation, macrophages, BRD9, bromodomain protein 9, BRD4

Abstract

Macrophages induce a number of inflammatory response genes in response to stimulation with microbial ligands. In response to endotoxin Lipid A, a gene-activation cascade of primary followed by secondary-response genes is induced. Epigenetic state is an important regulator of the kinetics, specificity, and mechanism of gene activation of these two classes. In particular, SWI/SNF chromatin-remodeling complexes are required for the induction of secondary-response genes, but not primary-response genes, which generally exhibit open chromatin. Here, we show that a recently discovered variant of the SWI/SNF complex, the noncanonical BAF complex (ncBAF), regulates secondary-response genes in the interferon (IFN) response pathway. Inhibition of bromodomain-containing protein 9 (BRD9), a subunit of the ncBAF complex, with BRD9 bromodomain inhibitors (BRD9i) or a degrader (dBRD9) led to reduction in a number of interferon-stimulated genes (ISGs) following stimulation with endotoxin lipid A. BRD9-dependent genes overlapped highly with a subset of genes differentially regulated by BET protein inhibition with JQ1 following endotoxin stimulation. We find that the BET protein BRD4 is cobound with BRD9 in unstimulated macrophages and corecruited upon stimulation to ISG promoters along with STAT1, STAT2, and IRF9, components of the ISGF3 complex activated downstream of IFN-alpha receptor stimulation. In the presence of BRD9i or dBRD9, STAT1-, STAT2-, and IRF9-binding is reduced, in some cases with reduced binding of BRD4. These results demonstrate a specific role for BRD9 and the ncBAF complex in ISG activation and identify an activity for BRD9 inhibitors and degraders in dampening endotoxin- and IFN-dependent gene expression.

Published

2022

4. IL-6-Driven pSTAT1 Response Is Linked to T Cell Features Implicated in Early Immune Dysregulation

Author

Lambert, Katharina, Diggins, Kirsten E, Jones, Britta E, Hundhausen, Christian, Maerz, Megan D, Hocking, Anne M, Sanda, Srinath, Greenbaum, Carla J, Linsley, Peter S, Cerosaletti, Karen, and Buckner, Jane H

Subjects

Biomedical and Clinical Sciences, Immunology, Autoimmune Disease, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Apoptosis, Cytokines, Humans, Immune System Diseases, Interleukin-6, STAT1 Transcription Factor, Signal Transduction, T-Lymphocytes, interleukin-6, interleukin-6 receptor, T cells, STAT1, STAT3, apoptosis, autoimmunity, Medical Microbiology, Biochemistry and cell biology, Genetics

Abstract

Elevated levels and enhanced sensing of the pro-inflammatory cytokine interleukin-6 (IL-6) are key features of many autoimmune and inflammatory diseases. To better understand how IL-6 signaling may influence human T cell fate, we investigated the relationships between levels of components of the IL-6R complex, pSTAT responses, and transcriptomic and translational changes in CD4+ and CD8+ T cell subsets from healthy individuals after exposure to IL-6. Our findings highlight the striking heterogeneity in mbIL-6R and gp130 expression and IL-6-driven pSTAT1/3 responses across T cell subsets. Increased mbIL-6R expression correlated with enhanced signaling via pSTAT1 with less impact on pSTAT3, most strikingly in CD4+ naïve T cells. Additionally, IL-6 rapidly induced expression of transcription factors and surface receptors expressed by T follicular helper cells and altered expression of markers of apoptosis. Importantly, many of the features associated with the level of mbIL-6R expression on T cells were recapitulated both in the setting of tocilizumab therapy and when comparing donor CD4+ T cells harboring the genetic variant, IL6R Asp358Ala (rs2228145), known to alter mbIL-6R expression on T cells. Collectively, these findings should be taken into account as we consider the role of IL-6 in disease pathogenesis and translating IL-6 biology into effective therapies for T cell-mediated autoimmune disease.

Published

2022

5. A Functional Precision Medicine Pipeline Combines Comparative Transcriptomics and Tumor Organoid Modeling to Identify Bespoke Treatment Strategies for Glioblastoma.

Author

Reed, Megan, Lyle, A, De Loose, Annick, Maddukuri, Leena, Learned, Katrina, Beale, Holly, Kephart, Ellen, Cheney, Allison, van den Bout, Anouk, Lee, Madison, Hundley, Kelsey, Smith, Ashley, DesRochers, Teresa, Vibat, Cecile, Gokden, Murat, Salama, Sofie, Wardell, Christopher, Eoff, Robert, Vaske, Olena, and Rodriguez, Analiz

Subjects

Li Fraumeni, glioblastoma, organoid, precision medicine, transcriptomics, Adolescent, Adult, Child, Female, Gene Expression Regulation, Neoplastic, Germ-Line Mutation, Glioblastoma, Humans, Janus Kinase 1, Janus Kinase 2, Li-Fraumeni Syndrome, Male, Nitriles, Organoids, Precision Medicine, Pyrazoles, Pyrimidines, RNA-Seq, STAT1 Transcription Factor, STAT2 Transcription Factor, Transcriptome, Young Adult

Abstract

Li Fraumeni syndrome (LFS) is a hereditary cancer predisposition syndrome caused by germline mutations in TP53. TP53 is the most common mutated gene in human cancer, occurring in 30-50% of glioblastomas (GBM). Here, we highlight a precision medicine platform to identify potential targets for a GBM patient with LFS. We used a comparative transcriptomics approach to identify genes that are uniquely overexpressed in the LFS GBM patient relative to a cancer compendium of 12,747 tumor RNA sequencing data sets, including 200 GBMs. STAT1 and STAT2 were identified as being significantly overexpressed in the LFS patient, indicating ruxolitinib, a Janus kinase 1 and 2 inhibitors, as a potential therapy. The LFS patient had the highest level of STAT1 and STAT2 expression in an institutional high-grade glioma cohort of 45 patients, further supporting the cancer compendium results. To empirically validate the comparative transcriptomics pipeline, we used a combination of adherent and organoid cell culture techniques, including ex vivo patient-derived organoids (PDOs) from four patient-derived cell lines, including the LFS patient. STAT1 and STAT2 expression levels in the four patient-derived cells correlated with levels identified in the respective parent tumors. In both adherent and organoid cultures, cells from the LFS patient were among the most sensitive to ruxolitinib compared to patient-derived cells with lower STAT1 and STAT2 expression levels. A spheroid-based drug screening assay (3D-PREDICT) was performed and used to identify further therapeutic targets. Two targeted therapies were selected for the patient of interest and resulted in radiographic disease stability. This manuscript supports the use of comparative transcriptomics to identify personalized therapeutic targets in a functional precision medicine platform for malignant brain tumors.

Published

2021

6. Self-reactivity controls functional diversity of naive CD8+ T cells by co-opting tonic type I interferon.

Author

Ju, Young-Jun, Lee, Sung-Woo, Kye, Yoon-Chul, Lee, Gil-Woo, Kim, Hee-Ok, Yun, Cheol-Heui, and Cho, Jae-Ho

Subjects

Animals, Antigens, Ly, CD5 Antigens, CD8-Positive T-Lymphocytes, Cell Differentiation, Cell Proliferation, Interferon Type I, Mice, Mice, Inbred C57BL, Phenotype, Receptor, Interferon alpha-beta, Receptors, Interferon, STAT1 Transcription Factor, Signal Transduction, Interferon gamma Receptor

Abstract

The strength of the T cell receptor interaction with self-ligands affects antigen-specific immune responses. However, the precise function and underlying mechanisms are unclear. Here, we demonstrate that naive CD8+ T cells with relatively high self-reactivity are phenotypically heterogeneous owing to varied responses to type I interferon, resulting in three distinct subsets, CD5loLy6C-, CD5hiLy6C-, and CD5hiLy6C+ cells. CD5hiLy6C+ cells differ from CD5loLy6C- and CD5hiLy6C- cells in terms of gene expression profiles and functional properties. Moreover, CD5hiLy6C+ cells demonstrate more extensive antigen-specific expansion upon viral infection, with enhanced differentiation into terminal effector cells and reduced memory cell generation. Such features of CD5hiLy6C+ cells are imprinted in a steady-state and type I interferon dependence is observed even for monoclonal CD8+ T cell populations. These findings demonstrate that self-reactivity controls the functional diversity of naive CD8+ T cells by co-opting tonic type I interferon signaling.

Published

2021

7. Histone deacetylase 2 knockout suppresses immune escape of triple-negative breast cancer cells via downregulating PD-L1 expression.

Author

Xu, Pengfei, Xiong, Wei, Lin, Yun, Fan, Liping, Pan, Hongchao, and Li, Yaochen

Subjects

Lymphocytes, Tumor-Infiltrating, Cell Line, Tumor, Animals, Mice, Inbred BALB C, Humans, Mice, Nude, Histones, Tumor Stem Cell Assay, Signal Transduction, Cell Cycle, Cell Proliferation, Cell Movement, Down-Regulation, Gene Expression Regulation, Neoplastic, Base Sequence, Acetylation, Female, STAT1 Transcription Factor, Janus Kinase 2, Interferon-gamma, Promoter Regions, Genetic, Gene Knockout Techniques, Histone Deacetylase 2, Immune Evasion, Triple Negative Breast Neoplasms, B7-H1 Antigen, Breast Cancer, Cancer, 2.1 Biological and endogenous factors, Aetiology, Biochemistry and Cell Biology, Oncology and Carcinogenesis

Abstract

The PD-L1 overexpression is an important event of immune escape and metastasis in triple-negative breast cancer (TNBC), but the molecular mechanism remains to be determined. Interferon gamma (IFNγ) represents a major driving force behind PD-L1 expression in tumor microenvironment, and histone deacetylase 2 (HDAC2) is required for IFN signaling. Here, we investigated the regulation of HDAC2 on the IFNγ-induced PD-L1 expression in TNBC cells. We found the HDAC2 and PD-L1 expression in TNBC was significantly higher than that in non-TNBC, and HDAC2 was positively correlated with PD-L1 expression. HDAC2 promoted PD-L1 induction by upregulating the phosphorylation of JAK1, JAK2, and STAT1, as well as the translocation of STAT1 to the nucleus and the recruitment of STAT1 to the PD-L1 promoter. Meanwhile, HDAC2 was recruited to the PD-L1 promoter by STAT1, and HDAC2 knockout compromised IFNγ-induced upregulation of H3K27, H3K9 acetylation, and the BRD4 recruitment in PD-L1 promoter. In addition, significant inhibition of proliferation, colony formation, migration, and cell cycle of TNBC cells were observed following knockout of HDAC2 in vitro. Furthermore, HDAC2 knockout reduced IFNγ-induced PD-L1 expression, lymphocyte infiltration, and retarded tumor growth and metastasis in the breast cancer mouse models. This study may provide evidence that HDAC2 promotes IFNγ-induced PD-L1 expression, suggesting a way for enhanced antitumor immunity when targeting the HDAC2 in TNBC.

Published

2021

8. Human DNA methylation signatures differentiate persistent from resolving MRSA bacteremia.

Author

Chang, Yu-Ling, Rossetti, Maura, Gjertson, David W, Rubbi, Liudmilla, Thompson, Michael, Montoya, Dennis J, Morselli, Marco, Ruffin, Felicia, Hoffmann, Alexander, Pellegrini, Matteo, Fowler, Vance G, Yeaman, Michael R, Reed, Elaine F, and with the MRSA Systems Immunology Group

Subjects

with the MRSA Systems Immunology Group, Humans, Bacteremia, Staphylococcal Infections, CCAAT-Enhancer-Binding Protein-beta, Anti-Bacterial Agents, DNA Methylation, Response Elements, Middle Aged, Female, Male, STAT1 Transcription Factor, p300-CBP Transcription Factors, Methicillin-Resistant Staphylococcus aureus, DNA methylation, MRSA, Staphylococcus aureus, epigenetics, persistence, Human Genome, Hematology, Antimicrobial Resistance, Genetics, Biodefense, Sepsis, Vaccine Related, Infectious Diseases, Emerging Infectious Diseases, Prevention, Infection

Abstract

Persistent methicillin-resistant Staphylococcus aureus (MRSA) bacteremia is life threatening and occurs in up to 30% of MRSA bacteremia cases despite appropriate antimicrobial therapy. Isolates of MRSA that cause antibiotic-persistent methicillin-resistant S. aureus bacteremia (APMB) typically have in vitro antibiotic susceptibilities equivalent to those causing antibiotic-resolving methicillin-resistant S. aureus bacteremia (ARMB). Thus, persistence reflects host-pathogen interactions occurring uniquely in context of antibiotic therapy in vivo. However, host factors and mechanisms involved in APMB remain unclear. We compared DNA methylomes in circulating immune cells from patients experiencing APMB vs. ARMB. Overall, methylation signatures diverged in the distinct patient cohorts. Differentially methylated sites intensified proximate to transcription factor binding sites, primarily in enhancer regions. In APMB patients, significant hypomethylation was observed in binding sites for CCAAT enhancer binding protein-β (C/EBPβ) and signal transducer/activator of transcription 1 (STAT1). In contrast, hypomethylation in ARMB patients localized to glucocorticoid receptor and histone acetyltransferase p300 binding sites. These distinct methylation signatures were enriched in neutrophils and achieved a mean area under the curve of 0.85 when used to predict APMB using a classification model. These findings validated by targeted bisulfite sequencing (TBS-seq) differentiate epigenotypes in patients experiencing APMB vs. ARMB and suggest a risk stratification strategy for antibiotic persistence in patients treated for MRSA bacteremia.

Published

2021

9. Aberrant type 1 immunity drives susceptibility to mucosal fungal infections

Author

Break, Timothy J, Oikonomou, Vasileios, Dutzan, Nicolas, Desai, Jigar V, Swidergall, Marc, Freiwald, Tilo, Chauss, Daniel, Harrison, Oliver J, Alejo, Julie, Williams, Drake W, Pittaluga, Stefania, Lee, Chyi-Chia R, Bouladoux, Nicolas, Swamydas, Muthulekha, Hoffman, Kevin W, Greenwell-Wild, Teresa, Bruno, Vincent M, Rosen, Lindsey B, Lwin, Wint, Renteria, Andy, Pontejo, Sergio M, Shannon, John P, Myles, Ian A, Olbrich, Peter, Ferré, Elise MN, Schmitt, Monica, Martin, Daniel, Core16, Genomics and Computational Biology, Barber, Daniel L, Solis, Norma V, Notarangelo, Luigi D, Serreze, David V, Matsumoto, Mitsuru, Hickman, Heather D, Murphy, Philip M, Anderson, Mark S, Lim, Jean K, Holland, Steven M, Filler, Scott G, Afzali, Behdad, Belkaid, Yasmine, Moutsopoulos, Niki M, and Lionakis, Michail S

Subjects

Autoimmune Disease, Emerging Infectious Diseases, Infectious Diseases, 2.1 Biological and endogenous factors, Aetiology, Infection, Inflammatory and immune system, Adolescent, Adult, Aged, Animals, Candida albicans, Candidiasis, Chronic Mucocutaneous, Disease Models, Animal, Female, Humans, Immunity, Mucosal, Immunologic Surveillance, Interferon-gamma, Interleukins, Janus Kinases, Male, Mice, Mice, Inbred BALB C, Middle Aged, Mouth Mucosa, Polyendocrinopathies, Autoimmune, Receptors, Interleukin-17, STAT1 Transcription Factor, T-Lymphocytes, Young Adult, Genomics and Computational Biology Core, General Science & Technology

Abstract

Human monogenic disorders have revealed the critical contribution of type 17 responses in mucosal fungal surveillance. We unexpectedly found that in certain settings, enhanced type 1 immunity rather than defective type 17 responses can promote mucosal fungal infection susceptibility. Notably, in mice and humans with AIRE deficiency, an autoimmune disease characterized by selective susceptibility to mucosal but not systemic fungal infection, mucosal type 17 responses are intact while type 1 responses are exacerbated. These responses promote aberrant interferon-γ (IFN-γ)- and signal transducer and activator of transcription 1 (STAT1)-dependent epithelial barrier defects as well as mucosal fungal infection susceptibility. Concordantly, genetic and pharmacologic inhibition of IFN-γ or Janus kinase (JAK)-STAT signaling ameliorates mucosal fungal disease. Thus, we identify aberrant T cell-dependent, type 1 mucosal inflammation as a critical tissue-specific pathogenic mechanism that promotes mucosal fungal infection susceptibility in mice and humans.

Published

2021

10. High Dose IFN-β Activates GAF to Enhance Expression of ISGF3 Target Genes in MLE12 Epithelial Cells

Author

Kishimoto, Kensei, Wilder, Catera L, Buchanan, Justin, Nguyen, Minh, Okeke, Chidera, Hoffmann, Alexander, and Cheng, Quen J

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Immunology, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Inflammatory and immune system, Animals, Cell Line, Chromatin Immunoprecipitation Sequencing, Dose-Response Relationship, Immunologic, Epithelial Cells, Gene Expression Regulation, Interferon-Stimulated Gene Factor 3, Interferon-beta, Mice, Promoter Regions, Genetic, Protein Multimerization, RNA-Seq, STAT1 Transcription Factor, interferon, JAK-STAT signaling pathway, signal transduction, gene regulation, ISGF3, GAF, Medical Microbiology, Biochemistry and cell biology

Abstract

Interferon β (IFN-β) signaling activates the transcription factor complex ISGF3 to induce gene expression programs critical for antiviral defense and host immune responses. It has also been observed that IFN-β activates a second transcription factor complex, γ-activated factor (GAF), but the significance of this coordinated activation is unclear. We report that in murine lung epithelial cells (MLE12) high doses of IFN-β indeed activate both ISGF3 and GAF, which bind to distinct genomic locations defined by their respective DNA sequence motifs. In contrast, low doses of IFN-β preferentially activate ISGF3 but not GAF. Surprisingly, in MLE12 cells GAF binding does not induce nearby gene expression even when strongly bound to the promoter. Yet expression of interferon stimulated genes is enhanced when GAF and ISGF3 are both active compared to ISGF3 alone. We propose that GAF may function as a dose-sensitive amplifier of ISG expression to enhance antiviral immunity and establish pro-inflammatory states.

Published

2021

11. Genome-wide aggregated trans-effects on risk of type 1 diabetes: A test of the "omnigenic" sparse effector hypothesis of complex trait genetics.

Author

Iakovliev, Andrii, McGurnaghan, Stuart J., Hayward, Caroline, Colombo, Marco, Lipschutz, Debby, Spiliopoulou, Athina, Colhoun, Helen M., and McKeigue, Paul M.

Subjects

*TYPE 1 diabetes, *GENETICS, *REGULATORY T cells, *GENE expression, *FORKHEAD transcription factors

Abstract

The "omnigenic" hypothesis postulates that the polygenic effects of common SNPs on a typical complex trait are mediated through trans -effects on expression of a relatively sparse set of effector ("core") genes. We tested this hypothesis in a study of 4,964 cases of type 1 diabetes (T1D) and 7,497 controls by using summary statistics to calculate aggregated (excluding the HLA region) trans -scores for gene expression in blood. From associations of T1D with aggregated trans -scores, nine putative core genes were identified, of which three— STAT1 , CTLA4 and FOXP3 —are genes in which variants cause monogenic forms of autoimmune diabetes. Seven of these genes affect the activity of regulatory T cells, and two are involved in immune responses to microbial lipids. Four T1D-associated genomic regions could be identified as master regulators via trans -effects on gene expression. These results support the sparse effector hypothesis and reshape our understanding of the genetic architecture of T1D. [Display omitted] Iakovliev et al. investigate whether the effects of common SNPs on risk of type 1 diabetes are mediated through trans -effects on expression of core genes. By testing for association with genotypic scores that aggregate predicted trans -effects, they identify a set of putative core genes for type 1 diabetes. [ABSTRACT FROM AUTHOR]

Published

2023

12. SARS-CoV-2 Orf6 hijacks Nup98 to block STAT nuclear import and antagonize interferon signaling

Author

Miorin, Lisa, Kehrer, Thomas, Sanchez-Aparicio, Maria Teresa, Zhang, Ke, Cohen, Phillip, Patel, Roosheel S, Cupic, Anastasija, Makio, Tadashi, Mei, Menghan, Moreno, Elena, Danziger, Oded, White, Kris M, Rathnasinghe, Raveen, Uccellini, Melissa, Gao, Shengyan, Aydillo, Teresa, Mena, Ignacio, Yin, Xin, Martin-Sancho, Laura, Krogan, Nevan J, Chanda, Sumit K, Schotsaert, Michael, Wozniak, Richard W, Ren, Yi, Rosenberg, Brad R, Fontoura, Beatriz MA, and García-Sastre, Adolfo

Subjects

Biodefense, Emerging Infectious Diseases, Vaccine Related, Infectious Diseases, Pneumonia, Prevention, Lung, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Active Transport, Cell Nucleus, Animals, Binding Sites, COVID-19, Chlorocebus aethiops, HEK293 Cells, Humans, Interferons, Nuclear Matrix-Associated Proteins, Nuclear Pore, Nuclear Pore Complex Proteins, Nucleocytoplasmic Transport Proteins, Protein Binding, STAT1 Transcription Factor, STAT2 Transcription Factor, Signal Transduction, Vero Cells, Viral Proteins, Immunization, Pneumonia & Influenza, Biotechnology, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, SARS-CoV-2, interferon signaling antagonism, STATs, ORF6, Nup98

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is the causative agent of the ongoing coronavirus disease 2019 (COVID-19) pandemic that is a serious global health problem. Evasion of IFN-mediated antiviral signaling is a common defense strategy that pathogenic viruses use to replicate and propagate in their host. In this study, we show that SARS-CoV-2 is able to efficiently block STAT1 and STAT2 nuclear translocation in order to impair transcriptional induction of IFN-stimulated genes (ISGs). Our results demonstrate that the viral accessory protein Orf6 exerts this anti-IFN activity. We found that SARS-CoV-2 Orf6 localizes at the nuclear pore complex (NPC) and directly interacts with Nup98-Rae1 via its C-terminal domain to impair docking of cargo-receptor (karyopherin/importin) complex and disrupt nuclear import. In addition, we show that a methionine-to-arginine substitution at residue 58 impairs Orf6 binding to the Nup98-Rae1 complex and abolishes its IFN antagonistic function. All together our data unravel a mechanism of viral antagonism in which a virus hijacks the Nup98-Rae1 complex to overcome the antiviral action of IFN.

Published

2020

13. Type I Interferon Regulates a Coordinated Gene Network to Enhance Cytotoxic T Cell–Mediated Tumor Killing

Author

Fan, Jun-Bao, Miyauchi, Sayuri, Xu, Hui-Zhong, Liu, Dan, Kim, Leo JY, Burkart, Christoph, Cheng, Hua, Arimoto, Kei-ichiro, Yan, Ming, Zhou, Yu, Győrffy, Balázs, Knobeloch, Klaus-Peter, Rich, Jeremy N, Cang, Hu, Fu, Xiang-Dong, and Zhang, Dong-Er

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Oncology and Carcinogenesis, Cancer, Breast Cancer, Genetics, Women's Health, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Animals, Breast Neoplasms, Cell Proliferation, Female, Gene Expression Regulation, Neoplastic, Gene Regulatory Networks, Humans, Interferon Type I, Mice, STAT1 Transcription Factor, STAT2 Transcription Factor, T-Lymphocytes, Transcription Factors, Ubiquitin-Activating Enzymes, Ubiquitins, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Type I interferons (IFN), which activate many IFN-stimulated genes (ISG), are known to regulate tumorigenesis. However, little is known regarding how various ISGs coordinate with one another in developing antitumor effects. Here, we report that the ISG UBA7 is a tumor suppressor in breast cancer. UBA7 encodes an enzyme that catalyzes the covalent conjugation of the ubiquitin-like protein product of another ISG (ISG15) to cellular proteins in a process known as "ISGylation." ISGylation of other ISGs, including STAT1 and STAT2, synergistically facilitates production of chemokine-receptor ligands to attract cytotoxic T cells. These gene-activation events are further linked to clustering and nuclear relocalization of STAT1/2 within IFN-induced promyelocytic leukemia (PML) bodies. Importantly, this coordinated ISG-ISGylation network plays a central role in suppressing murine breast cancer growth and metastasis, which parallels improved survival in patients with breast cancer. These findings reveal a cooperative IFN-inducible gene network in orchestrating a tumor-suppressive microenvironment. SIGNIFICANCE: We report a highly cooperative ISG network, in which UBA7-mediated ISGylation facilitates clustering of transcription factors and activates an antitumor gene-expression program. These findings provide mechanistic insights into immune evasion in breast cancer associated with UBA7 loss, emphasizing the importance of a functional ISG-ISGylation network in tumor suppression.This article is highlighted in the In This Issue feature, p. 327.

Published

2020

14. Cellular Signaling Analysis shows antiviral, ribavirin-mediated ribosomal signaling modulation.

Author

Nolan, Garry, Sanchez, David, Ding, Xianting, Krutzik, Peter, Ghaffari, Amir, Zhaozhi, Yixiu, Miranda, Daniel, Cheng, Genhong, and Ho, Chih-Ming

Subjects

Animals, Antiviral Agents, Biomarkers, Cell Line, Cytokines, Disease Models, Animal, Drug Discovery, Herpes Simplex, Herpesvirus 1, Human, Host-Pathogen Interactions, Humans, Mice, Ribavirin, Ribosomal Protein S6 Kinases, Ribosomes, STAT1 Transcription Factor, Signal Transduction, Virus Replication

Abstract

As antiviral drug resistance develops and new viruses emerge there is a pressing need to develop strategies to rapidly develop antiviral therapeutics. Here we use phospho-specific flow cytometry to assess perturbations of many different cellular signaling pathways during treatment with drug combinations that are highly effective in blocking Herpes simplex virus type 1 (HSV-1) infection. We discovered two antiviral drug combinations act on distinct signaling pathways, either STAT1 or S6 phosphorylation, to block HSV-1 infection. We focused on upregulation of S6 phosphorylation by HSV-1 infection, and our subsequent finding that ribavirin antagonizes this upregulation of S6 phosphorylation. We go on to show that the S6 kinase inhibitor SL0101 blocks HSV-1 replication in vitro and in an in vivo animal model of HSV-1 infection. Overall, we have used an unbiased analysis of cellular signaling pathways during treatment by antiviral drug combinations to discover a novel antiviral drug target against HSV-1 infection. The outcomes of the approach we present highlight the importance of analyzing how antiviral drugs modulate cellular and pathogen-induced signaling as a method to discover new drug therapy targets.

Published

2019

15. Cellular Signaling Analysis shows antiviral, ribavirin-mediated ribosomal signaling modulation

Author

Ding, Xianting, Krutzik, Peter O, Ghaffari, Amir Ali, Zhaozhi, Yixiu, Miranda, Daniel, Cheng, Genhong, Ho, Chih-Ming, Nolan, Garry P, and Sanchez, David Jesse

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Biological Sciences, Sexually Transmitted Infections, Infectious Diseases, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Infection, Good Health and Well Being, Animals, Antiviral Agents, Biomarkers, Cell Line, Cytokines, Disease Models, Animal, Drug Discovery, Herpes Simplex, Herpesvirus 1, Human, Host-Pathogen Interactions, Humans, Mice, Ribavirin, Ribosomal Protein S6 Kinases, Ribosomes, STAT1 Transcription Factor, Signal Transduction, Virus Replication, Microbiology, Pharmacology and Pharmaceutical Sciences, Virology, Medical microbiology, Pharmacology and pharmaceutical sciences

Abstract

As antiviral drug resistance develops and new viruses emerge there is a pressing need to develop strategies to rapidly develop antiviral therapeutics. Here we use phospho-specific flow cytometry to assess perturbations of many different cellular signaling pathways during treatment with drug combinations that are highly effective in blocking Herpes simplex virus type 1 (HSV-1) infection. We discovered two antiviral drug combinations act on distinct signaling pathways, either STAT1 or S6 phosphorylation, to block HSV-1 infection. We focused on upregulation of S6 phosphorylation by HSV-1 infection, and our subsequent finding that ribavirin antagonizes this upregulation of S6 phosphorylation. We go on to show that the S6 kinase inhibitor SL0101 blocks HSV-1 replication in vitro and in an in vivo animal model of HSV-1 infection. Overall, we have used an unbiased analysis of cellular signaling pathways during treatment by antiviral drug combinations to discover a novel antiviral drug target against HSV-1 infection. The outcomes of the approach we present highlight the importance of analyzing how antiviral drugs modulate cellular and pathogen-induced signaling as a method to discover new drug therapy targets.

Published

2019

16. Inflammaging: Age and Systemic, Cellular, and Nuclear Inflammatory Biology in Older Adults

Author

Piber, Dominique, Olmstead, Richard, Cho, Joshua Hyong-Jin, Witarama, Tuff, Perez, Christian, Dietz, Nicholas, Seeman, Teresa E, Breen, Elizabeth C, Cole, Steve W, and Irwin, Michael R

Subjects

Cancer, Aging, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Age Factors, Aged, Aged, 80 and over, C-Reactive Protein, Cross-Sectional Studies, Cytokines, Female, Gene Expression Regulation, Humans, Independent Living, Inflammation, Inflammation Mediators, Linear Models, Male, Middle Aged, Multivariate Analysis, Risk Assessment, STAT1 Transcription Factor, STAT3 Transcription Factor, STAT5 Transcription Factor, Signal Transduction, Tumor Necrosis Factor-alpha, Tumor Suppressor Proteins, STAT signaling, NF-kappa B, C-reactive protein, Proinflammatory cytokines, NF-κB, Clinical Sciences, Gerontology

Abstract

Systemic inflammation is associated with increasing age. Yet, there are limited data about the association between age and systemic inflammation within older adults, and whether older age is also associated with cellular and nuclear signaling markers of inflammation. In community-dwelling older adults (N = 262, 60-88 years), systemic levels of C-reactive protein, interleukin-6, and soluble tumor necrosis factor receptor II; levels of toll-like receptor-4-stimulated monocytic production of interleukin-6 and tumor necrosis factor α; and resting nuclear levels of activated nuclear factor kappa B and signal transducer and activator of transcription (STAT1, STAT3, STAT5) were evaluated. Adjusting for demographic and clinical factors, multivariate linear regression tested the association between age and each inflammatory marker. Age was positively associated with increased levels of interleukin-6 and soluble tumor necrosis factor receptor II (p's < .05) and with increases in STAT1, STAT3, and STAT5 activation (p's < .05). However, no relationship was found between age and C-reactive protein, toll-like receptor-4-stimulated interleukin-6/tumor necrosis factor alpha α production, or nuclear factor kappa B. Within a community-dwelling sample of older adults, older age is associated with increases in STAT activation, along with increases of systemic inflammatory cytokines. In older adults, heterogeneity in age-related increases in inflammatory disease risk may be related to individual variability in inflammation.

Published

2019

17. miR-486 is modulated by stretch and increases ventricular growth.

Author

Lange, Stephan, Banerjee, Indroneal, Carrion, Katrina, Serrano, Ricardo, Habich, Louisa, Kameny, Rebecca, Lengenfelder, Luisa, Dalton, Nancy, Meili, Rudolph, Börgeson, Emma, Peterson, Kirk, Ricci, Marco, Lincoln, Joy, Ghassemian, Majid, Fineman, Jeffery, Del Álamo, Juan, and Nigam, Vishal

Subjects

Cardiology, Cardiovascular disease, Cell Biology, Noncoding RNAs, Proteomics, Animals, Animals, Newborn, Biomechanical Phenomena, Cell Proliferation, Cells, Cultured, Heart Ventricles, Humans, Hypoplastic Left Heart Syndrome, Mechanotransduction, Cellular, Mice, MicroRNAs, Myocytes, Cardiac, STAT1 Transcription Factor, Sheep

Abstract

Perturbations in biomechanical stimuli during cardiac development contribute to congenital cardiac defects such as hypoplastic left heart syndrome (HLHS). This study sought to identify stretch-responsive pathways involved in cardiac development. miRNA-Seq identified miR-486 as being increased in cardiomyocytes exposed to cyclic stretch in vitro. The right ventricles (RVs) of patients with HLHS experienced increased stretch and had a trend toward higher miR-486 levels. Sheep RVs dilated from excessive pulmonary blood flow had 60% more miR-486 compared with control RVs. The left ventricles of newborn mice treated with miR-486 mimic were 16.9%-24.6% larger and displayed a 2.48-fold increase in cardiomyocyte proliferation. miR-486 treatment decreased FoxO1 and Smad signaling while increasing the protein levels of Stat1. Stat1 associated with Gata-4 and serum response factor (Srf), 2 key cardiac transcription factors with protein levels that increase in response to miR-486. This is the first report to our knowledge of a stretch-responsive miRNA that increases the growth of the ventricle in vivo.

Published

2019

18. PHLPP1 counter-regulates STAT1-mediated inflammatory signaling.

Author

Cohen Katsenelson, Ksenya, Stender, Joshua D, Kawashima, Agnieszka T, Lordén, Gema, Uchiyama, Satoshi, Nizet, Victor, Glass, Christopher K, and Newton, Alexandra C

Subjects

Animals, Mice, Escherichia coli Infections, Disease Models, Animal, Inflammation, Signal Transduction, Gene Expression Regulation, STAT1 Transcription Factor, Phosphoprotein Phosphatases, Immunity, Innate, PHLPP1, STAT1, biochemistry, chemical biology, immunology, inflammation, mouse, phosphatase, transcription factors, Biochemistry and Cell Biology

Abstract

Inflammation is an essential aspect of innate immunity but also contributes to diverse human diseases. Although much is known about the kinases that control inflammatory signaling, less is known about the opposing phosphatases. Here we report that deletion of the gene encoding PH domain Leucine-rich repeat Protein Phosphatase 1 (PHLPP1) protects mice from lethal lipopolysaccharide (LPS) challenge and live Escherichia coli infection. Investigation of PHLPP1 function in macrophages reveals that it controls the magnitude and duration of inflammatory signaling by dephosphorylating the transcription factor STAT1 on Ser727 to inhibit its activity, reduce its promoter residency, and reduce the expression of target genes involved in innate immunity and cytokine signaling. This previously undescribed function of PHLPP1 depends on a bipartite nuclear localization signal in its unique N-terminal extension. Our data support a model in which nuclear PHLPP1 dephosphorylates STAT1 to control the magnitude and duration of inflammatory signaling in macrophages.

Published

2019

19. PHLPP1 counter-regulates STAT1-mediated inflammatory signaling

Author

Katsenelson, Ksenya Cohen, Stender, Joshua D, Kawashima, Agnieszka T, Lordén, Gema, Uchiyama, Satoshi, Nizet, Victor, Glass, Christopher K, and Newton, Alexandra C

Subjects

Biochemistry and Cell Biology, Biological Sciences, Infectious Diseases, Biodefense, Genetics, Emerging Infectious Diseases, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Inflammatory and immune system, Animals, Disease Models, Animal, Escherichia coli Infections, Gene Expression Regulation, Immunity, Innate, Inflammation, Mice, Phosphoprotein Phosphatases, STAT1 Transcription Factor, Signal Transduction, PHLPP1, STAT1, biochemistry, chemical biology, immunology, inflammation, mouse, phosphatase, transcription factors, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Inflammation is an essential aspect of innate immunity but also contributes to diverse human diseases. Although much is known about the kinases that control inflammatory signaling, less is known about the opposing phosphatases. Here we report that deletion of the gene encoding PH domain Leucine-rich repeat Protein Phosphatase 1 (PHLPP1) protects mice from lethal lipopolysaccharide (LPS) challenge and live Escherichia coli infection. Investigation of PHLPP1 function in macrophages reveals that it controls the magnitude and duration of inflammatory signaling by dephosphorylating the transcription factor STAT1 on Ser727 to inhibit its activity, reduce its promoter residency, and reduce the expression of target genes involved in innate immunity and cytokine signaling. This previously undescribed function of PHLPP1 depends on a bipartite nuclear localization signal in its unique N-terminal extension. Our data support a model in which nuclear PHLPP1 dephosphorylates STAT1 to control the magnitude and duration of inflammatory signaling in macrophages.

Published

2019

20. LNK suppresses interferon signaling in melanoma.

Author

Ding, Ling-Wen, Sun, Qiao-Yang, Edwards, Jarem J, Fernández, Lucia Torres, Ran, Xue-Bin, Zhou, Si-Qin, Scolyer, Richard A, Wilmott, James S, Thompson, John F, Doan, Ngan, Said, Jonathan W, Venkatachalam, Nachiyappan, Xiao, Jin-Fen, Loh, Xin-Yi, Pein, Maren, Xu, Liang, Mullins, David W, Yang, Henry, Lin, De-Chen, and Koeffler, H Phillip

Subjects

Cell Line, Tumor, Animals, Mice, Inbred C57BL, Mice, Inbred NOD, Humans, Mice, Mice, SCID, Melanoma, Skin Neoplasms, Intracellular Signaling Peptides and Proteins, Proteins, Interferons, Xenograft Model Antitumor Assays, Apoptosis, STAT1 Transcription Factor, HEK293 Cells, Cell Cycle Checkpoints, Membrane Proteins, Cell Line, Tumor, Inbred C57BL, Inbred NOD, SCID

Abstract

LNK (SH2B3) is a key negative regulator of JAK-STAT signaling which has been extensively studied in malignant hematopoietic diseases. We found that LNK is significantly elevated in cutaneous melanoma; this elevation is correlated with hyperactive signaling of the RAS-RAF-MEK pathway. Elevated LNK enhances cell growth and survival in adverse conditions. Forced expression of LNK inhibits signaling by interferon-STAT1 and suppresses interferon (IFN) induced cell cycle arrest and cell apoptosis. In contrast, silencing LNK expression by either shRNA or CRISPR-Cas9 potentiates the killing effect of IFN. The IFN-LNK signaling is tightly regulated by a negative feedback mechanism; melanoma cells exposed to IFN upregulate expression of LNK to prevent overactivation of this signaling pathway. Our study reveals an unappreciated function of LNK in melanoma and highlights the critical role of the IFN-STAT1-LNK signaling axis in this potentially devastating disease. LNK may be further explored as a potential therapeutic target for melanoma immunotherapy.

Published

2019

21. Application of Flow Cytometry in the Diagnostics Pipeline of Primary Immunodeficiencies Underlying Disseminated Talaromyces marneffei Infection in HIV-Negative Children

Author

Lee, Pamela P, Lao-araya, Mongkol, Yang, Jing, Chan, Koon-Wing, Ma, Haiyan, Pei, Lim-Cho, Kui, Lin, Mao, Huawei, Yang, Wanling, Zhao, Xiaodong, Trakultivakorn, Muthita, and Lau, Yu-Lung

Subjects

Pediatric, Biodefense, Infectious Diseases, Rare Diseases, HIV/AIDS, Prevention, Vaccine Related, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Infection, Inflammatory and immune system, Good Health and Well Being, Adolescent, Adult, CD40 Ligand, Child, Child, Preschool, Female, Flow Cytometry, Humans, Immunoglobulin Isotypes, Infant, Lymphocyte Count, Male, Mycoses, Primary Immunodeficiency Diseases, STAT1 Transcription Factor, Sensitivity and Specificity, Talaromyces, Taloromyces marneffei, flow cytometry, X-linked hyper-IgM syndrome, CD40L, STAT1, interferon gamma receptor deficiency, Immunology, Medical Microbiology

Abstract

Talaromyces (Penicillium) marneffei is an AIDS-defining infection in Southeast Asia and is associated with high mortality. It is rare in non-immunosuppressed individuals, especially children. Little is known about host immune response and genetic susceptibility to this endemic fungus. Genetic defects in the interferon-gamma (IFN-γ)/STAT1 signaling pathway, CD40/CD40 ligand- and IL12/IL12-receptor-mediated crosstalk between phagocytes and T-cells, and STAT3-mediated Th17 differentiation have been reported in HIV-negative children with talaromycosis and other endemic mycoses such as histoplasmosis, coccidioidomycosis, and paracoccidioidomycosis. There is a need to design a diagnostic algorithm to evaluate such patients. In this article, we review a cohort of pediatric patients with disseminated talaromycosis referred to the Asian Primary Immunodeficiency Network for genetic diagnosis of PID. Using these illustrative cases, we propose a diagnostics pipeline that begins with immunoglobulin pattern (IgG, IgA, IgM, and IgE) and enumeration of lymphocyte subpopulations (T-, B-, and NK-cells). The former could provide clues for hyper-IgM syndrome and hyper-IgE syndrome. Flow cytometric evaluation of CD40L expression should be performed for patients suspected to have X-linked hyper-IgM syndrome. Defects in interferon-mediated JAK-STAT signaling are evaluated by STAT1 phosphorylation studies by flow cytometry. STAT1 hyperphosphorylation in response to IFN-α or IFN-γ and delayed dephosphorylation is diagnostic for gain-of-function STAT1 disorder, while absent STAT1 phosphorylation in response to IFN-γ but normal response to IFN-α is suggestive of IFN-γ receptor deficiency. This simple and rapid diagnostic algorithm will be useful in guiding genetic studies for patients with disseminated talaromycosis requiring immunological investigations.

Published

2019

22. Combating viral contaminants in CHO cells by engineering innate immunity

Author

Chiang, Austin WT, Li, Shangzhong, Kellman, Benjamin P, Chattopadhyay, Gouri, Zhang, Yaqin, Kuo, Chih-Chung, Gutierrez, Jahir M, Ghazi, Faezeh, Schmeisser, Hana, Ménard, Patrice, Bjørn, Sara Petersen, Voldborg, Bjørn G, Rosenberg, Amy S, Puig, Montserrat, and Lewis, Nathan E

Subjects

Infectious Diseases, Biodefense, Biotechnology, Prevention, Emerging Infectious Diseases, Vaccine Related, Genetics, Infection, Animals, Biomarkers, CHO Cells, Cricetulus, Drug Resistance, Genetic Engineering, Host-Pathogen Interactions, Immunity, Innate, Industrial Microbiology, Interferon Type I, Poly I-C, RNA Viruses, STAT1 Transcription Factor, Signal Transduction, Virus Replication

Abstract

Viral contamination in biopharmaceutical manufacturing can lead to shortages in the supply of critical therapeutics. To facilitate the protection of bioprocesses, we explored the basis for the susceptibility of CHO cells to RNA virus infection. Upon infection with certain ssRNA and dsRNA viruses, CHO cells fail to generate a significant interferon (IFN) response. Nonetheless, the downstream machinery for generating IFN responses and its antiviral activity is intact in these cells: treatment of cells with exogenously-added type I IFN or poly I:C prior to infection limited the cytopathic effect from Vesicular stomatitis virus (VSV), Encephalomyocarditis virus (EMCV), and Reovirus-3 virus (Reo-3) in a STAT1-dependent manner. To harness the intrinsic antiviral mechanism, we used RNA-Seq to identify two upstream repressors of STAT1: Gfi1 and Trim24. By knocking out these genes, the engineered CHO cells exhibited activation of cellular immune responses and increased resistance to the RNA viruses tested. Thus, omics-guided engineering of mammalian cell culture can be deployed to increase safety in biotherapeutic protein production among many other biomedical applications.

Published

2019

23. STAT2 dependent Type I Interferon response promotes dysbiosis and luminal expansion of the enteric pathogen Salmonella Typhimurium

Author

Wilson, R Paul, Tursi, Sarah A, Rapsinski, Glenn J, Medeiros, Nicole J, Le, Long S, Kotredes, Kevin P, Patel, Sajan, Liverani, Elisabetta, Sun, Shuang, Zhu, Wenhan, Kilpatrick, Laurie, Winter, Sebastian E, Gamero, Ana M, and Tükel, Çagla

Subjects

Microbiology, Biological Sciences, Biomedical and Clinical Sciences, Vaccine Related, Digestive Diseases, Emerging Infectious Diseases, Prevention, Foodborne Illness, Infectious Diseases, Biodefense, Aetiology, 2.1 Biological and endogenous factors, Infection, Animals, Cells, Cultured, Dysbiosis, Female, Gastroenteritis, Inflammation, Interferon Type I, Intestines, Mice, Mice, Inbred C57BL, Mice, Knockout, Neutrophils, STAT1 Transcription Factor, STAT2 Transcription Factor, Salmonella Infections, Salmonella typhimurium, Immunology, Medical Microbiology, Virology, Medical microbiology

Abstract

The mechanisms by which the gut luminal environment is disturbed by the immune system to foster pathogenic bacterial growth and survival remain incompletely understood. Here, we show that STAT2 dependent type I IFN signaling contributes to the inflammatory environment by disrupting hypoxia enabling the pathogenic S. Typhimurium to outgrow the microbiota. Stat2-/- mice infected with S. Typhimurium exhibited impaired type I IFN induced transcriptional responses in cecal tissue and reduced bacterial burden in the intestinal lumen compared to infected wild-type mice. Although inflammatory pathology was similar between wild-type and Stat2-/- mice, we observed decreased hypoxia in the gut tissue of Stat2-/- mice. Neutrophil numbers were similar in wild-type and Stat2-/- mice, yet Stat2-/- mice showed reduced levels of myeloperoxidase activity. In vitro, the neutrophils from Stat2-/- mice produced lower levels of superoxide anion upon stimulation with the bacterial ligand N-formylmethionyl-leucyl-phenylalanine (fMLP) in the presence of IFNα compared to neutrophils from wild-type mice, indicating that the neutrophils were less functional in Stat2-/- mice. Cytochrome bd-II oxidase-mediated respiration enhances S. Typhimurium fitness in wild-type mice, while in Stat2-/- deficiency, this respiratory pathway did not provide a fitness advantage. Furthermore, luminal expansion of S. Typhimurium in wild-type mice was blunted in Stat2-/- mice. Compared to wild-type mice which exhibited a significant perturbation in Bacteroidetes abundance, Stat2-/- mice exhibited significantly less perturbation and higher levels of Bacteroidetes upon S. Typhimurium infection. Our results highlight STAT2 dependent type I IFN mediated inflammation in the gut as a novel mechanism promoting luminal expansion of S. Typhimurium.

Published

2019

24. miR-30a Remodels Subcutaneous Adipose Tissue Inflammation to Improve Insulin Sensitivity in Obesity

Author

Koh, Eun-Hee, Chernis, Natasha, Saha, Pradip K, Xiao, Liuling, Bader, David A, Zhu, Bokai, Rajapakshe, Kimal, Hamilton, Mark P, Liu, Xia, Perera, Dimuthu, Chen, Xi, York, Brian, Trauner, Michael, Coarfa, Cristian, Bajaj, Mandeep, Moore, David D, Deng, Tuo, McGuire, Sean E, and Hartig, Sean M

Subjects

Biomedical and Clinical Sciences, Diabetes, Obesity, Biotechnology, Nutrition, Genetics, Aetiology, 2.1 Biological and endogenous factors, Metabolic and endocrine, Oral and gastrointestinal, Cardiovascular, Adipose Tissue, White, Animals, Diabetes Mellitus, Type 2, Diet, High-Fat, Energy Metabolism, Insulin Resistance, Liver, Mice, MicroRNAs, STAT1 Transcription Factor, Subcutaneous Fat, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

Chronic inflammation accompanies obesity and limits subcutaneous white adipose tissue (WAT) expandability, accelerating the development of insulin resistance and type 2 diabetes mellitus. MicroRNAs (miRNAs) influence expression of many metabolic genes in fat cells, but physiological roles in WAT remain poorly characterized. Here, we report that expression of the miRNA miR-30a in subcutaneous WAT corresponds with insulin sensitivity in obese mice and humans. To examine the hypothesis that restoration of miR-30a expression in WAT improves insulin sensitivity, we injected adenovirus (Adv) expressing miR-30a into the subcutaneous fat pad of diabetic mice. Exogenous miR-30a expression in the subcutaneous WAT depot of obese mice coupled improved insulin sensitivity and increased energy expenditure with decreased ectopic fat deposition in the liver and reduced WAT inflammation. High-throughput proteomic profiling and RNA-Seq suggested that miR-30a targets the transcription factor STAT1 to limit the actions of the proinflammatory cytokine interferon-γ (IFN-γ) that would otherwise restrict WAT expansion and decrease insulin sensitivity. We further demonstrated that miR-30a opposes the actions of IFN-γ, suggesting an important role for miR-30a in defending adipocytes against proinflammatory cytokines that reduce peripheral insulin sensitivity. Together, our data identify a critical molecular signaling axis, elements of which are involved in uncoupling obesity from metabolic dysfunction.

Published

2018

25. Crk Adaptor Proteins Regulate NK Cell Expansion and Differentiation during Mouse Cytomegalovirus Infection

Author

Nabekura, Tsukasa, Chen, Zhiying, Schroeder, Casey, Park, Taeju, Vivier, Eric, Lanier, Lewis L, and Liu, Dongfang

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Infectious Diseases, Underpinning research, 1.1 Normal biological development and functioning, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Animals, Cell Differentiation, Cell Proliferation, Cytomegalovirus Infections, Interferon-alpha, Interleukin-12, Killer Cells, Natural, Mice, Mice, Inbred C57BL, Mice, Knockout, Muromegalovirus, NK Cell Lectin-Like Receptor Subfamily A, Proto-Oncogene Proteins c-crk, STAT1 Transcription Factor, STAT4 Transcription Factor, Signal Transduction, Biochemistry and cell biology

Abstract

Natural killer cells are critical in the immune response to infection and malignancy. Prior studies have demonstrated that Crk family proteins can influence cell apoptosis, proliferation, and cell transformation. In this study, we investigated the role of Crk family proteins in mouse NK cell differentiation and host defense using a mouse CMV infection model. The number of NK cells, maturational state, and the majority of the NKR repertoire was similar in Crk x Crk-like (CrkL)-double-deficient and wild type NK cells. However, Crk family proteins were required for optimal activation, IFN-γ production, expansion, and differentiation of Ly49H+ NK cells, as well as host defense during mouse CMV infection. The diminished function of Crk x CrkL-double-deficient NK cells correlated with decreased phosphorylation of STAT4 and STAT1 in response to IL-12 and IFN-α stimulation, respectively. Together, our findings analyzing NK cell-specific Crk-deficient mice provide insights into the role of Crk family proteins in NK cell function and host defense.

Published

2018

26. Pathobiology of the 129:Stat1−/− mouse model of human age-related ER-positive breast cancer with an immune infiltrate-excluded phenotype

Author

Mori, Hidetoshi, Chen, Jane Q, Cardiff, Robert D, Pénzváltó, Zsófia, Hubbard, Neil E, Schuetter, Louis, Hovey, Russell C, Trott, Josephine F, and Borowsky, Alexander D

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Breast Cancer, Cancer, 2.1 Biological and endogenous factors, Aetiology, Age Factors, Animals, Breast Neoplasms, Chemotaxis, Leukocyte, Disease Models, Animal, Female, Humans, Immunohistochemistry, Incidence, Macrophages, Mammary Neoplasms, Experimental, Mice, Mice, 129 Strain, Mice, Knockout, Phenotype, Receptors, Estrogen, STAT1 Transcription Factor, Estrogen receptor, Luminal breast cancer, Stat1-knockout mouse, Pathobiology, Tumor microenvironment, Tumor immunology, Oncology & Carcinogenesis, Oncology and carcinogenesis

Abstract

BackgroundStat1 gene-targeted knockout mice (129S6/SvEvTac-Stat1 tm1Rds) develop estrogen receptor-positive (ER+), luminal-type mammary carcinomas at an advanced age. There is evidence for both host environment as well as tumor cell-intrinsic mechanisms to initiate tumorigenesis in this model. In this report, we summarize details of the systemic and mammary pathology at preneoplastic and tumor-bearing time points. In addition, we investigate tumor progression in the 129:Stat1 -/- host compared with wild-type 129/SvEv, and we describe the immune cell reaction to the tumors.MethodsMice housed and treated according to National Institutes of Health guidelines and Institutional Animal Care and Use Committee-approved methods were evaluated by histopathology, and their tissues were subjected to immunohistochemistry with computer-assisted quantitative image analysis. Tumor cell culture and conditioned media from cell culture were used to perform macrophage (RAW264.7) cell migration assays, including the 129:Stat1 -/--derived SSM2 cells as well as control Met1 and NDL tumor cells and EpH4 normal cells.ResultsTumorigenesis in 129:Stat1 -/- originates from a population of FoxA1+ large oval pale cells that initially appear and accumulate along the mammary ducts in segments or regions of the gland prior to giving rise to mammary intraepithelial neoplasias. Progression to invasive carcinoma is accompanied by a marked local stromal and immune cell response composed predominantly of T cells and macrophages. In conditioned media experiments, cells derived from 129:Stat1 -/- tumors secrete both chemoattractant and chemoinhibitory factors, with greater attraction in the extracellular vesicular fraction and inhibition in the soluble fraction. The result appears to be recruitment of the immune reaction to the periphery of the tumor, with exclusion of immune cell infiltration into the tumor.Conclusions129:Stat1 -/- is a unique model for studying the critical origins and risk reduction strategies in age-related ER+ breast cancer. In addition, it can be used in preclinical trials of hormonal and targeted therapies as well as immunotherapies.

Published

2017

27. Gain-of-function STAT1 mutation and visceral leishmaniasis

Author

Paula Teixeira Lyra, Ana Carla Augusto Moura Falcão, Rafael Amora Cruz, Antonio Victor Campos Coelho, Edvaldo da Silva Souza, Luiz Claudio Arraes de Alencar, and João Bosco Oliveira

Subjects

STAT1 transcription factor, Germ-line mutation, Sequence analysis, DNA, Leishmaniasis, visceral, Lymphohistiocytosis, hemophagocytic, Medicine

Abstract

ABSTRACT Gain-of-function mutations in the STAT1 gene have been initially associated with chronic mucocutaneous candidiasis. However, further research has shown that STAT1 GOF variants may increase susceptibility to infection by other intracellular pathogens. This report describes the first case of disseminated leishmaniasis associated with a STAT1 GOF mutation in a pediatric patient who did not have chronic mucocutaneous candidiasis. The patient was a four-year-old boy presenting with fever, severe asthenia, hepatosplenomegaly, pancytopenia, and liver failure. Bone marrow aspirate revealed hemophagocytosis and Leishmania parasites. Treatment consisted primarily of liposomal amphotericin B, as per the Hemophagocytic Lymphohistiocytosis 2004 protocol. After eight weeks of treatment, the patient did not improve and was submitted to diagnostic splenectomy. Activated macrophages and nodular spleen necrosis secondary to the visceral leishmaniasis were detected. Unfortunately, the patient died in the second week after splenectomy due to overwhelming systemic infection. DNA sequencing revealed a pathogenic (p. R274Q) GOF mutation in STAT1.

Published

2022

28. EZH2-mediated upregulation of ROS1 oncogene promotes oral cancer metastasis

Author

Shih, C-H, Chang, Y-J, Huang, W-C, Jang, T-H, Kung, H-J, Wang, W-C, Yang, M-H, Lin, M-C, Huang, S-F, Chou, S-W, Chang, E, Chiu, H, Shieh, T-Y, Chen, Y-J, Wang, L-H, and Chen, L

Subjects

Orphan Drug, Lung, Cancer, Genetics, Dental/Oral and Craniofacial Disease, Lung Cancer, Rare Diseases, 2.1 Biological and endogenous factors, Aetiology, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Animals, Biomarkers, Tumor, Carcinoma, Squamous Cell, Cell Line, Tumor, Cell Proliferation, Chemokine CXCL1, Down-Regulation, Enhancer of Zeste Homolog 2 Protein, ErbB Receptors, Gene Expression Regulation, Neoplastic, Histones, Humans, Lung Neoplasms, Male, Methylation, Mice, Molecular Targeted Therapy, Mouth Neoplasms, Protein-Tyrosine Kinases, Proto-Oncogene Proteins, STAT1 Transcription Factor, Up-Regulation, Xenograft Model Antitumor Assays, Zinc Finger Protein GLI1, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Current anti-epidermal growth factor receptor (EGFR) therapy for oral cancer does not provide satisfactory efficacy due to drug resistance or reduced EGFR level. As an alternative candidate target for therapy, here we identified an oncogene, ROS1, as an important driver for oral squamous cell carcinoma (OSCC) metastasis. Among tumors from 188 oral cancer patients, upregulated ROS1 expression strongly correlated with metastasis to lung and lymph nodes. Mechanistic studies uncover that the activated ROS1 results from highly expressed ROS1 gene instead of gene rearrangement, a phenomenon distinct from other cancers. Our data further reveal a novel mechanism that reduced histone methyltransferase EZH2 leads to a lower trimethylation of histone H3 lysine 27 suppressive modification, relaxes chromatin, and promotes the accessibility of the transcription factor STAT1 to the enhancer and the intron regions of ROS1 target genes, CXCL1 and GLI1, for upregulating their expressions. Down-regulation of ROS1 in highly invasive OSCC cells, nevertheless, reduces cell proliferation and inhibits metastasis to lung in the tail-vein injection and the oral cavity xenograft models. Our findings highlight ROS1 as a candidate biomarker and therapeutic target for OSCC. Finally, we demonstrate that co-targeting of ROS1 and EGFR could potentially offer an effective oral cancer therapy.

Published

2017

29. T cell protein tyrosine phosphatase prevents STAT1 induction of claudin‐2 expression in intestinal epithelial cells

Author

Krishnan, Moorthy and McCole, Declan F

Subjects

Biochemistry and Cell Biology, Medical Physiology, Biomedical and Clinical Sciences, Biological Sciences, Genetics, Digestive Diseases, Underpinning research, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Aetiology, Oral and gastrointestinal, Cell Line, Claudin-2, Epithelial Cells, Humans, Intestinal Mucosa, Promoter Regions, Genetic, Protein Tyrosine Phosphatase, Non-Receptor Type 2, STAT1 Transcription Factor, Tight Junctions, tight junction, inflammatory bowel disease, barrier function, interferon-gamma, protein tyrosine phosphatase, interferon-γ, General Science & Technology

Abstract

T cell protein tyrosine phosphatase (TCPTP) dephosphorylates a number of substrates, including JAK-STAT (signal transducer and activator of transcription) signaling proteins, which are activated by interferon (IFN)-γ, a major proinflammatory cytokine involved in conditions such as inflammatory bowel disease. A critical function of the intestinal epithelium is formation of a selective barrier to luminal contents. The structural units of the epithelium that regulate barrier function are the tight junctions (TJs), and the protein composition of the TJ determines the tightness of the barrier. Claudin-2 is a TJ protein that increases permeability to cations and reduces transepithelial electrical resistance (TER). We previously showed that transient knockdown (KD) of TCPTP permits increased expression of claudin-2 by IFN-γ. Here, we demonstrate that the decreased TER in TCPTP-deficient epithelial cells is alleviated by STAT1 KD. Moreover, increased claudin-2 in TCPTP-deficient cells requires enhanced STAT1 activation and STAT1 binding to the CLDN2 promoter. We also show that mutation of this STAT-binding site prevents elevated CLDN2 promoter activity in TCPTP-deficient epithelial cells. In summary, we demonstrate that TCPTP protects the intestinal epithelial barrier by restricting STAT-induced claudin-2 expression. This is a potential mechanism by which loss-of-function mutations in the gene encoding TCPTP may contribute to barrier defects in chronic intestinal inflammatory disease.

Published

2017

30. Systems approach to uncover signaling networks in primary immunodeficiency diseases

Author

Choi, Jeff, Fernandez, Rosemary, Maecker, Holden T, and Butte, Manish J

Subjects

Biomedical and Clinical Sciences, Immunology, Adolescent, Adult, Cytokines, Cytological Techniques, Humans, Immunologic Deficiency Syndromes, STAT1 Transcription Factor, STAT3 Transcription Factor, Signal Transduction, Systems Biology, Young Adult, Allergy

Abstract

This broad, unbiased approach of studying signaling across all circulating immune cells in healthy subjects allowed identification of disrupted signaling networks in patients with primary immunodeficiencies.

Published

2017

31. Diptoindonesin G promotes ERK-mediated nuclear translocation of p-STAT1 (Ser727) and cell differentiation in AML cells.

Author

Gao, Jian, Fan, Minmin, Xiang, Gang, Wang, Jujuan, Zhang, Xiong, Guo, Wenjie, Wu, Xuefeng, Sun, Yang, Gu, Yanhong, Ge, Huiming, Tan, Renxiang, Qiu, Hongxia, Shen, Yan, and Xu, Qiang

Subjects

Animals, Antineoplastic Agents, Benzofurans, Caspase 3, Caspase Inhibitors, Cell Differentiation, Cell Line, Tumor, Cell Nucleus, Cell Proliferation, Chemokine CXCL10, Extracellular Signal-Regulated MAP Kinases, HL-60 Cells, Humans, Intracellular Signaling Peptides and Proteins, Leukemia, Myeloid, Acute, Mice, Mice, Inbred NOD, Mice, SCID, Phosphorylation, STAT1 Transcription Factor, Up-Regulation

Abstract

Exploration of a new differentiation therapy that extends the range of differentiation for treating acute myeloid leukemia (AML) is attractive to researchers and clinicians. Here we report that diptoindonesin G (Dip G), a natural resveratrol aneuploid, exerts antiproliferative activity by inducing G2/M phase arrest and cell differentiation in AML cell lines and primary AML cells. Gene-profiling experiments showed that treating human leukemia HL-60 cells with Dip G was associated with a remarkable upregulation of STAT1 target gene expression, including IFIT3 and CXCL10. Mechanistically, Dip G activated ERK, which caused phosphorylation of STAT1 at Ser727 and selectively enhanced the interaction of p-STAT1 (Ser727) and p-ERK, further promoting their nuclear translocation. The nuclear translocation of p-STAT1 and p-ERK enhanced the transactivation of STAT1-targeted genes in AML cells. Furthermore, in vivo treatment of HL-60 xenografts demonstrated that Dip G significantly inhibited tumor growth and reduced tumor weight by inducing cell differentiation. Taken together, these results shed light on an essential role for ERK-mediated nuclear translocation of p-STAT1 (Ser727) and its full transcriptional activity in Dip G-induced differentiation of AML cells. Furthermore, these results demonstrate that Dip G could be used as a differentiation-inducing agent for AML therapy, particularly for non-acute promyelocytic leukemia therapy.

Published

2017

32. Isocitrate dehydrogenase mutations suppress STAT1 and CD8+ T cell accumulation in gliomas

Author

Kohanbash, Gary, Carrera, Diego A, Shrivastav, Shruti, Ahn, Brian J, Jahan, Naznin, Mazor, Tali, Chheda, Zinal S, Downey, Kira M, Watchmaker, Payal B, Beppler, Casey, Warta, Rolf, Amankulor, Nduka A, Herold-Mende, Christel, Costello, Joseph F, and Okada, Hideho

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Genetics, Neurosciences, Immunization, Cancer, Brain Cancer, Rare Diseases, Brain Disorders, Good Health and Well Being, Animals, Brain Neoplasms, CD8-Positive T-Lymphocytes, Cancer Vaccines, Cell Line, Tumor, Chemokines, Chemotaxis, Glioma, Humans, Isocitrate Dehydrogenase, Lymphocytes, Tumor-Infiltrating, Mice, Inbred C57BL, Neoplasm Transplantation, STAT1 Transcription Factor, T-Lymphocytes, Cytotoxic, Vaccination, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Mutations in the isocitrate dehydrogenase genes IDH1 and IDH2 are among the first genetic alterations observed during the development of lower-grade glioma (LGG). LGG-associated IDH mutations confer gain-of-function activity by converting α-ketoglutarate to the oncometabolite R-2-hydroxyglutarate (2HG). Clinical samples and gene expression data from The Cancer Genome Atlas (TCGA) demonstrate reduced expression of cytotoxic T lymphocyte-associated genes and IFN-γ-inducible chemokines, including CXCL10, in IDH-mutated (IDH-MUT) tumors compared with IDH-WT tumors. Given these findings, we have investigated the impact of IDH mutations on the immunological milieu in LGG. In immortalized normal human astrocytes (NHAs) and syngeneic mouse glioma models, the introduction of mutant IDH1 or treatment with 2HG reduced levels of CXCL10, which was associated with decreased production of STAT1, a regulator of CXCL10. Expression of mutant IDH1 also suppressed the accumulation of T cells in tumor sites. Reductions in CXCL10 and T cell accumulation were reversed by IDH-C35, a specific inhibitor of mutant IDH1. Furthermore, IDH-C35 enhanced the efficacy of vaccine immunotherapy in mice bearing IDH-MUT gliomas. Our findings demonstrate a mechanism of immune evasion in IDH-MUT gliomas and suggest that specific inhibitors of mutant IDH may improve the efficacy of immunotherapy in patients with IDH-MUT gliomas.

Published

2017

33. Zinc deficiency affects the STAT1/3 signaling pathways in part through redox-mediated mechanisms.

Author

Supasai, S, Aimo, L, Adamo, AM, Mackenzie, GG, and Oteiza, PI

Subjects

Central Nervous System, Brain, Animals, Humans, Rats, Zinc, Thioctic Acid, Tyrosine, Signal Transduction, Gene Expression Regulation, Developmental, Protein Transport, Oxidation-Reduction, Oxidative Stress, Phosphorylation, STAT1 Transcription Factor, STAT3 Transcription Factor, Transcriptional Activation, Pediatric, Rare Diseases, Nutrition, Neurosciences, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Pharmacology and Pharmaceutical Sciences

Abstract

Zinc deficiency affects the development of the central nervous system (CNS) through mechanisms only partially understood. We previously showed that zinc deficiency causes CNS oxidative stress, damaging microtubules and impairing protein nuclear shuttling. STAT1 and STAT3 transcription factors, which require nuclear import for their functions, play major roles in CNS development. Thus, we investigated whether zinc deficiency disrupts STAT1 and STAT3 signaling pathways in the developing fetal CNS, characterizing the involvement of oxidative stress and the cytoskeleton in the adverse effects. Maternal (gestation day 0-19) marginal zinc deficiency (MZD) reduced STAT1 and STAT3 tyrosine phosphorylation and their nuclear translocation in the embryonic day 19 (E19) rat brain. Similar effects were observed in zinc depleted IMR-32 neuroblastoma cells, with an associated decrease in STAT1- and STAT3-dependent gene transactivation. Zinc deficiency caused oxidative stress (increased 4-hydroxynonenal-protein adducts) in E19 brain and IMR-32 cells, which was prevented in cells by supplementation with 0.5mM α-lipoic acid (LA). In zinc depleted IMR-32 cells, the low tyrosine phosphorylation of STAT1, but not that of STAT3, recovered upon incubation with LA. STAT1 and STAT3 nuclear transports were also restored by LA. Accordingly, chemical disruption of the cytoskeleton partially reduced STAT1 and STAT3 nuclear levels. In summary, the redox-dependent tyrosine phosphorylation, and oxidant-mediated disruption of the cytoskeleton are involved in the deleterious effects of zinc deficit on STAT1 and STAT3 activation and nuclear translocation. Therefore, disruption of the STAT1 and STAT3 signaling pathways may in part explain the deleterious effects of maternal MZD on fetal brain development.

Published

2017

34. Exogenous IL-33 Restores Dendritic Cell Activation and Maturation in Established Cancer.

Author

Dominguez, Donye, Ye, Cong, Geng, Zhe, Chen, Siqi, Fan, Jie, Qin, Lei, Long, Alan, Wang, Long, Zhang, Zhuoli, Zhang, Yi, Fang, Deyu, Kuzel, Timothy M, and Zhang, Bin

Subjects

Dendritic Cells, CD8-Positive T-Lymphocytes, Tumor Cells, Cultured, Animals, Mice, Inbred C57BL, Mice, Neoplasms, Experimental, Proto-Oncogene Proteins B-raf, Recombinant Proteins, Cytotoxicity, Immunologic, STAT1 Transcription Factor, PTEN Phosphohydrolase, Myeloid Differentiation Factor 88, Interleukin-33, Interleukin-1 Receptor-Like 1 Protein, CD40 Antigens, Biotechnology, Vaccine Related, Immunization, Cancer, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Immunology

Abstract

The role of IL-33, particularly in tumor growth and tumor immunity, remains ill-defined. We show that exogenous IL-33 can induce robust antitumor effect through a CD8+ T cell-dependent mechanism. Systemic administration of rIL-33 alone was sufficient to inhibit growth of established tumors in transplant and de novo melanoma tumorigenesis models. Notably, in addition to a direct action on CD8+ T cell expansion and IFN-γ production, rIL-33 therapy activated myeloid dendritic cells (mDCs) in tumor-bearing mice, restored antitumor T cell activity, and increased Ag cross-presentation within the tumor microenvironment. Furthermore, combination therapy consisting of rIL-33 and agonistic anti-CD40 Abs demonstrated synergistic antitumor activity. Specifically, MyD88, an essential component of the IL-33 signaling pathway, was required for the IL-33-mediated increase in mDC number and upregulation in expression of costimulatory molecules. Importantly, we identified that the IL-33 receptor ST2, MyD88, and STAT1 cooperate to induce costimulatory molecule expression on mDCs in response to rIL-33. Thus, our study revealed a novel IL-33-ST2-MyD88-STAT1 axis that restores mDC activation and maturation in established cancer and, thereby, the magnitude of antitumor immune responses, suggesting a potential use of rIL-33 as a new immunotherapy option to treat established cancer.

Published

2017

35. T lymphocyte SHP2-deficiency triggers anti-tumor immunity to inhibit colitis-associated cancer in mice.

Author

Liu, Wen, Guo, Wenjie, Shen, Lihong, Chen, Zhen, Luo, Qiong, Luo, Xiaolin, Feng, GenSheng, Shu, Yongqian, Gu, Yanhong, Xu, Qiang, and Sun, Yang

Subjects

IFN-γ, SHP2, antitumor immunity, colitis-associated cancer, cytotoxic T lymphocyte, Animals, Azoxymethane, CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Cells, Cultured, Colitis, Colonic Neoplasms, Cytotoxicity, Immunologic, Dextran Sulfate, Disease Models, Animal, Fas Ligand Protein, Granzymes, Inflammation Mediators, Interferon-gamma, Lymphocytes, Tumor-Infiltrating, Mice, Knockout, Perforin, Phosphorylation, Protein Tyrosine Phosphatase, Non-Receptor Type 11, STAT1 Transcription Factor, Signal Transduction, Time Factors, Tumor Microenvironment

Abstract

Nonresolving inflammation is involved in the initiation and progression process of tumorigenesis. Src homology 2 domain-containing tyrosine phosphatase 2 (SHP2) is known to inhibit acute inflammation but its role in chronic inflammation-associated cancer remains unclear. The role of SHP2 in T cells in dextran sulfate sodium (DSS)-induced colitis and azoxymethane-DSS-induced colitis-associated carcinogenesis was examined using SHP2CD4-/- conditional knockout mice. SHP2 deficiency in T cells aggravated colitis with increased level of pro-inflammatory cytokines including IFN-γ and IL-17A. In contrast, the SHP2CD4-/- mice developed much fewer and smaller tumors than wild type mice with higher level of IFN-γ and enhanced cytotoxicity of CD8+ T cells in the tumor and peritumoral areas. At the molecular level, STAT1 was hyper-phosphorylated in T cells lacking SHP2, which may account for the increased Th1 differentiation and IFN-γ secretion. IFN-γ neutralization or IFN-γ receptor knockout but not IL-17A neutralization, abrogated the anti-tumor effect of SHP2 knockout with lowered levels of perforin 1, FasL and granzyme B. Finally, the expression of granzyme B was negatively correlated with the malignancy of colon cancer in human patients. In conclusion, these findings suggest a new strategy to treat colitis-associated cancer via targeting SHP2.

Published

2017

36. Metronomic chemotherapy prevents therapy-induced stromal activation and induction of tumor-initiating cells

Author

Chan, Tze-Sian, Hsu, Chung-Chi, Pai, Vincent C, Liao, Wen-Ying, Huang, Shenq-Shyang, Tan, Kok-Tong, Yen, Chia-Jui, Hsu, Shu-Ching, Chen, Wei-Yu, Shan, Yan-Shen, Li, Chi-Rong, Lee, Michael T, Jiang, Kuan-Ying, Chu, Jui-Mei, Lien, Gi-Shih, Weaver, Valerie M, and Tsai, Kelvin K

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Stem Cell Research, Biotechnology, Stem Cell Research - Nonembryonic - Human, Cancer, Rare Diseases, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Administration, Metronomic, Breast Neoplasms, Female, Fibroblasts, Humans, MCF-7 Cells, NF-kappa B, Receptors, Interleukin-8B, STAT1 Transcription Factor, Stromal Cells, U937 Cells, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences

Abstract

Although traditional chemotherapy kills a fraction of tumor cells, it also activates the stroma and can promote the growth and survival of residual cancer cells to foster tumor recurrence and metastasis. Accordingly, overcoming the host response induced by chemotherapy could substantially improve therapeutic outcome and patient survival. In this study, resistance to treatment and metastasis has been attributed to expansion of stem-like tumor-initiating cells (TICs). Molecular analysis of the tumor stroma in neoadjuvant chemotherapy-treated human desmoplastic cancers and orthotopic tumor xenografts revealed that traditional maximum-tolerated dose chemotherapy, regardless of the agents used, induces persistent STAT-1 and NF-κB activity in carcinoma-associated fibroblasts. This induction results in the expression and secretion of ELR motif-positive (ELR+) chemokines, which signal through CXCR-2 on carcinoma cells to trigger their phenotypic conversion into TICs and promote their invasive behaviors, leading to paradoxical tumor aggression after therapy. In contrast, the same overall dose administered as a low-dose metronomic chemotherapy regimen largely prevented therapy-induced stromal ELR+ chemokine paracrine signaling, thus enhancing treatment response and extending survival of mice carrying desmoplastic cancers. These experiments illustrate the importance of stroma in cancer therapy and how its impact on treatment resistance could be tempered by altering the dosing schedule of systemic chemotherapy.

Published

2016

37. Mapping the Fetomaternal Peripheral Immune System at Term Pregnancy.

Author

Fragiadakis, Gabriela, Baca, Quentin, Gherardini, Pier, Ganio, Edward, Gaudilliere, Dyani, Tingle, Martha, Lancero, Hope, McNeil, Leslie, Spitzer, Matthew, Wong, Ronald, Shaw, Gary, Darmstadt, Gary, Sylvester, Karl, Winn, Virginia, Carvalho, Brendan, Lewis, David, Stevenson, David, Nolan, Garry, Aghaeepour, Nima, Angst, Martin, and Gaudilliere, Brice

Subjects

CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Extracellular Signal-Regulated MAP Kinases, Female, Humans, Immunity, Innate, Killer Cells, Natural, Placenta, Pregnancy, Pregnancy Proteins, STAT1 Transcription Factor

Abstract

Preterm labor and infections are the leading causes of neonatal deaths worldwide. During pregnancy, immunological cross talk between the mother and her fetus is critical for the maintenance of pregnancy and the delivery of an immunocompetent neonate. A precise understanding of healthy fetomaternal immunity is the important first step to identifying dysregulated immune mechanisms driving adverse maternal or neonatal outcomes. This study combined single-cell mass cytometry of paired peripheral and umbilical cord blood samples from mothers and their neonates with a graphical approach developed for the visualization of high-dimensional data to provide a high-resolution reference map of the cellular composition and functional organization of the healthy fetal and maternal immune systems at birth. The approach enabled mapping of known phenotypical and functional characteristics of fetal immunity (including the functional hyperresponsiveness of CD4+ and CD8+ T cells and the global blunting of innate immune responses). It also allowed discovery of new properties that distinguish the fetal and maternal immune systems. For example, examination of paired samples revealed differences in endogenous signaling tone that are unique to a mother and her offspring, including increased ERK1/2, MAPK-activated protein kinase 2, rpS6, and CREB phosphorylation in fetal Tbet+CD4+ T cells, CD8+ T cells, B cells, and CD56loCD16+ NK cells and decreased ERK1/2, MAPK-activated protein kinase 2, and STAT1 phosphorylation in fetal intermediate and nonclassical monocytes. This highly interactive functional map of healthy fetomaternal immunity builds the core reference for a growing data repository that will allow inferring deviations from normal associated with adverse maternal and neonatal outcomes.

Published

2016

38. Type I IFN promotes NK cell expansion during viral infection by protecting NK cells against fratricide

Author

Madera, Sharline, Rapp, Moritz, Firth, Matthew A, Beilke, Joshua N, Lanier, Lewis L, and Sun, Joseph C

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Biodefense, Vaccine Related, Prevention, Aetiology, 2.1 Biological and endogenous factors, Infection, Animals, Apoptosis, Cell Proliferation, Herpesviridae Infections, Interferon Type I, Killer Cells, Natural, Lymphocyte Activation, Mice, Mice, Inbred C57BL, Mice, Knockout, Muromegalovirus, NK Cell Lectin-Like Receptor Subfamily K, Perforin, Receptor, Interferon alpha-beta, STAT1 Transcription Factor, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences

Abstract

Type I interferon (IFN) is crucial in host antiviral defense. Previous studies have described the pleiotropic role of type I IFNs on innate and adaptive immune cells during viral infection. Here, we demonstrate that natural killer (NK) cells from mice lacking the type I IFN-α receptor (Ifnar(-/-)) or STAT1 (which signals downstream of IFNAR) are defective in expansion and memory cell formation after mouse cytomegalovirus (MCMV) infection. Despite comparable proliferation, Ifnar(-/-) NK cells showed diminished protection against MCMV infection and exhibited more apoptosis compared with wild-type NK cells. Furthermore, we show that Ifnar(-/-) NK cells express increased levels of NK group 2 member D (NKG2D) ligands during viral infection and are susceptible to NK cell-mediated fratricide in a perforin- and NKG2D-dependent manner. Adoptive transfer of Ifnar(-/-) NK cells into NK cell-deficient mice reverses the defect in survival and expansion. Our study reveals a novel type I IFN-dependent mechanism by which NK cells evade mechanisms of cell death after viral infection.

Published

2016

39. Targeted deep sequencing identifies rare loss-of-function variants in IFNGR1 for risk of atopic dermatitis complicated by eczema herpeticum

Author

Gao, Li, Bin, Lianghua, Rafaels, Nicholas M, Huang, Lili, Potee, Joseph, Ruczinski, Ingo, Beaty, Terri H, Paller, Amy S, Schneider, Lynda C, Gallo, Rich, Hanifin, Jon M, Beck, Lisa A, Geha, Raif S, Mathias, Rasika A, Barnes, Kathleen C, and Leung, Donald YM

Subjects

Human Genome, Genetic Testing, Prevention, Genetics, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Adolescent, Adult, Aged, Aged, 80 and over, Cell Line, Child, Child, Preschool, Dermatitis, Atopic, Female, Genes, Reporter, Genetic Predisposition to Disease, Genotype, High-Throughput Nucleotide Sequencing, Humans, Infant, Interferon-gamma, Kaposi Varicelliform Eruption, Male, Middle Aged, Polymorphism, Single Nucleotide, Receptors, Interferon, Risk, STAT1 Transcription Factor, Young Adult, IFNGR1, genetic variants, atopic dermatitis, eczema herpeticum, Immunology, Allergy

Abstract

BackgroundA subset of atopic dermatitis is associated with increased susceptibility to eczema herpeticum (ADEH+). We previously reported that common single nucleotide polymorphisms (SNPs) in the IFN-γ (IFNG) and IFN-γ receptor 1 (IFNGR1) genes were associated with the ADEH+ phenotype.ObjectiveWe sought to interrogate the role of rare variants in interferon pathway genes for the risk of ADEH+.MethodsWe performed targeted sequencing of interferon pathway genes (IFNG, IFNGR1, IFNAR1, and IL12RB1) in 228 European American patients with AD selected according to their eczema herpeticum status, and severity was measured by using the Eczema Area and Severity Index. Replication genotyping was performed in independent samples of 219 European American and 333 African American subjects. Functional investigation of loss-of-function variants was conducted by using site-directed mutagenesis.ResultsWe identified 494 single nucleotide variants encompassing 105 kb of sequence, including 145 common, 349 (70.6%) rare (minor allele frequency

Published

2015

40. Gain-of-function STAT1 mutation and visceral leishmaniasis.

Author

Teixeira Lyra, Paula, Augusto Moura Falcão, Ana Carla, Amora Cruz, Rafael, Campos Coelho, Antonio Victor, da Silva Souza, Edvaldo, Arraes de Alencar, Luiz Claudio, and Bosco Oliveira, João

Subjects

*GAIN-of-function mutations, *TRANSCRIPTION factors, *CHRONIC diseases, *VISCERAL leishmaniasis, *BONE marrow, *CHILD patients, *LIPOSOMES, *AMPHOTERICIN B, *DNA

Abstract

Gain-of-function mutations in the STAT1 gene have been initially associated with chronic mucocutaneous candidiasis. However, further research has shown that STAT1 GOF variants may increase susceptibility to infection by other intracellular pathogens. This report describes the first case of disseminated leishmaniasis associated with a STAT1 GOF mutation in a pediatric patient who did not have chronic mucocutaneous candidiasis. The patient was a four-yearold boy presenting with fever, severe asthenia, hepatosplenomegaly, pancytopenia, and liver failure. Bone marrow aspirate revealed hemophagocytosis and Leishmania parasites. Treatment consisted primarily of liposomal amphotericin B, as per the Hemophagocytic Lymphohistiocytosis 2004 protocol. After eight weeks of treatment, the patient did not improve and was submitted to diagnostic splenectomy. Activated macrophages and nodular spleen necrosis secondary to the visceral leishmaniasis were detected. Unfortunately, the patient died in the second week after splenectomy due to overwhelming systemic infection. DNA sequencing revealed a pathogenic (p. R274Q) GOF mutation in STAT1. [ABSTRACT FROM AUTHOR]

Published

2022

41. STAT2-dependent induction of RNA adenosine deaminase ADAR1 by type I interferon differs between mouse and human cells in the requirement for STAT1.

Author

George, Cyril X and Samuel, Charles E

Subjects

Cell Line, Animals, Humans, Mice, Adenosine Deaminase, Interferon Type I, RNA, Messenger, Gene Expression Regulation, Protein Binding, STAT1 Transcription Factor, STAT2 Transcription Factor, Promoter Regions, Genetic, Transcriptional Activation, Gene Knockout Techniques, Adenosine deaminase acting on RNA, Innate immunity, Interferon, Signal transducers and activators of transcription, Genetics, 1.1 Normal biological development and functioning, Aetiology, Underpinning research, 2.1 Biological and endogenous factors, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology

Abstract

Expression of adenosine deaminase acting on RNA1 (ADAR1) is driven by alternative promoters. Promoter PA, activated by interferon (IFN), produces transcripts that encode the inducible p150 ADAR1 protein, whereas PB specifies the constitutively expressed p110 protein. We show using Stat1(-/-), Stat2(-/-) and IRF9(-/-) MEFs that induction of ADAR1 p150 occurs by STAT2- and IRF9-dependent signaling that is enhanced by, but not obligatorily dependent upon, STAT1. Chromatin immunoprecipitation analysis demonstrated STAT2 at the PA promoter in IFN-treated Stat1(-/-) cells, whereas IFN-treated wild-type cells showed both STAT1 and STAT2 bound at PA. By contrast, with human 2fTGH cells and mutants U3A or U6A, ADAR1 induction by IFN was dependent upon both STAT1 and STAT2. These results suggest that transcriptional activation of Adar1 by IFN occurs in the absence of STAT1 by a non-canonical STAT2-dependent pathway in mouse but not human cells.

Published

2015

42. HCS Campaign to Identify Selective Inhibitors of IL-6-Induced STAT3 Pathway Activation in Head and Neck Cancer Cell Lines

Author

Johnston, Paul A, Sen, Malabika, Hua, Yun, Camarco, Daniel P, Shun, Tong Ying, Lazo, John S, Wilson, Gabriela Mustata, Resnick, Lynn O, LaPorte, Matthew G, Wipf, Peter, Huryn, Donna M, and Grandis, Jennifer R

Subjects

Biomedical and Clinical Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Oncology and Carcinogenesis, Rare Diseases, Dental/Oral and Craniofacial Disease, Cancer, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Carcinoma, Squamous Cell, Cell Line, Tumor, Head and Neck Neoplasms, High-Throughput Screening Assays, Humans, Interferon-gamma, Interleukin-6, STAT1 Transcription Factor, STAT3 Transcription Factor, Signal Transduction, Squamous Cell Carcinoma of Head and Neck, Physical Chemistry (incl. Structural), Pharmacology and Pharmaceutical Sciences, Medicinal & Biomolecular Chemistry, Pharmacology and pharmaceutical sciences, Medicinal and biomolecular chemistry

Abstract

Signal transducer and activator of transcription factor 3 (STAT3) is hyperactivated in head and neck squamous cell carcinomas (HNSCC). Cumulative evidence indicates that IL-6 production by HNSCC cells and/or stromal cells in the tumor microenvironment activates STAT3 and contributes to tumor progression and drug resistance. A library of 94,491 compounds from the Molecular Library Screening Center Network (MLSCN) was screened for the ability to inhibit interleukin-6 (IL-6)-induced pSTAT3 activation. For contractual reasons, the primary high-content screening (HCS) campaign was conducted over several months in 3 distinct phases; 1,068 (1.1%) primary HCS actives remained after cytotoxic or fluorescent outliers were eliminated. One thousand one hundred eighty-seven compounds were cherry-picked for confirmation; actives identified in the primary HCS and compounds selected by a structural similarity search of the remaining MLSCN library using hits identified in phases I and II of the screen. Actives were confirmed in pSTAT3 IC50 assays, and an IFNγ-induced pSTAT1 activation assay was used to prioritize selective inhibitors of STAT3 activation that would not inhibit STAT1 tumor suppressor functions. Two hundred three concentration-dependent inhibitors of IL-6-induced pSTAT3 activation were identified and 89 of these also produced IC50s against IFN-γ-induced pSTAT1 activation. Forty-nine compounds met our hit criteria: they reproducibly inhibited IL-6-induced pSTAT3 activation by ≥70% at 20 μM; their pSTAT3 activation IC50s were ≤25 μM; they were ≥2-fold selective for pSTAT3 inhibition over pSTAT1 inhibition; a cross target query of PubChem indicated that they were not biologically promiscuous; and they were ≥90% pure. Twenty-six chemically tractable hits that passed filters for nuisance compounds and had acceptable drug-like and ADME-Tox properties by computational evaluation were purchased for characterization. The hit structures were distributed among 5 clusters and 8 singletons. Twenty-four compounds inhibited IL-6-induced pSTAT3 activation with IC50s ≤20 μM and 13 were ≥3-fold selective versus inhibition of pSTAT1 activation. Eighteen hits inhibited the growth of HNSCC cell lines with average IC50s ≤ 20 μM. Four chemical series were progressed into lead optimization: the guanidinoquinazolines, the triazolothiadiazines, the amino alcohols, and an oxazole-piperazine singleton.

Published

2015

43. Sleep loss activates cellular inflammation and signal transducer and activator of transcription (STAT) family proteins in humans

Author

Irwin, Michael R, Witarama, Tuff, Caudill, Marissa, Olmstead, Richard, and Breen, Elizabeth Crabb

Subjects

Clinical Research, Sleep Research, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Adult, Aged, Female, Humans, Inflammation, Interleukin-6, Leukocytes, Mononuclear, Male, Middle Aged, Monocytes, STAT1 Transcription Factor, STAT3 Transcription Factor, STAT5 Transcription Factor, Sleep Deprivation, Tumor Necrosis Factor-alpha, Sleep, Immunology, Sleep deprivation, Tumor necrosis factor-alpha, Signal transducer and activator of transcription, Flow cytometry, Tumor necrosis factor-α, Neurosciences, Psychology, Neurology & Neurosurgery

Abstract

Sleep disturbance and short sleep duration are associated with inflammation and related disorders including cardiovascular disease, arthritis, diabetes mellitus, and certain cancers. This study was undertaken to test the effects of experimental sleep loss on spontaneous cellular inflammation and activation of signal transducer and activator of transcription (STAT) family proteins, which together promote an inflammatory microenvironment. In 24 healthy adults (16 females; 8 males), spontaneous production of IL-6 and TNF-α in monocytes and spontaneous intranuclear expression of activated STAT1, STAT3, and STAT5 in peripheral blood mononuclear cells (PBMC), monocyte-, and lymphocyte populations were measured in the morning after uninterrupted baseline sleep, partial sleep deprivation (PSD, sleep period from 3a.m. to 7a.m.), and recovery sleep. Relative to baseline, spontaneous monocytic expression of IL-6 and TNF-α was significantly greater after PSD (P

Published

2015

44. Lupus Risk Variant Increases pSTAT1 Binding and Decreases ETS1 Expression

Author

Lu, Xiaoming, Zoller, Erin E, Weirauch, Matthew T, Wu, Zhiguo, Namjou, Bahram, Williams, Adrienne H, Ziegler, Julie T, Comeau, Mary E, Marion, Miranda C, Glenn, Stuart B, Adler, Adam, Shen, Nan, Nath, Swapan K, Stevens, Anne M, Freedman, Barry I, Tsao, Betty P, Jacob, Chaim O, Kamen, Diane L, Brown, Elizabeth E, Gilkeson, Gary S, Alarcón, Graciela S, Reveille, John D, Anaya, Juan-Manuel, James, Judith A, Sivils, Kathy L, Criswell, Lindsey A, Vilá, Luis M, Alarcón-Riquelme, Marta E, Petri, Michelle, Scofield, R Hal, Kimberly, Robert P, Ramsey-Goldman, Rosalind, Bin Joo, Young, Choi, Jeongim, Bae, Sang-Cheol, Boackle, Susan A, Graham, Deborah Cunninghame, Vyse, Timothy J, Guthridge, Joel M, Gaffney, Patrick M, Langefeld, Carl D, Kelly, Jennifer A, Greis, Kenneth D, Kaufman, Kenneth M, Harley, John B, and Kottyan, Leah C

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Biotechnology, Lupus, Autoimmune Disease, Human Genome, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Alleles, Animals, Asian People, Bayes Theorem, Genetic Predisposition to Disease, Genotype, Haplotypes, Humans, Lupus Erythematosus, Systemic, Mice, Protein Binding, Proto-Oncogene Protein c-ets-1, STAT1 Transcription Factor, Medical and Health Sciences, Genetics & Heredity, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Genetic variants at chromosomal region 11q23.3, near the gene ETS1, have been associated with systemic lupus erythematosus (SLE), or lupus, in independent cohorts of Asian ancestry. Several recent studies have implicated ETS1 as a critical driver of immune cell function and differentiation, and mice deficient in ETS1 develop an SLE-like autoimmunity. We performed a fine-mapping study of 14,551 subjects from multi-ancestral cohorts by starting with genotyped variants and imputing to all common variants spanning ETS1. By constructing genetic models via frequentist and Bayesian association methods, we identified 16 variants that are statistically likely to be causal. We functionally assessed each of these variants on the basis of their likelihood of affecting transcription factor binding, miRNA binding, or chromatin state. Of the four variants that we experimentally examined, only rs6590330 differentially binds lysate from B cells. Using mass spectrometry, we found more binding of the transcription factor signal transducer and activator of transcription 1 (STAT1) to DNA near the risk allele of rs6590330 than near the non-risk allele. Immunoblot analysis and chromatin immunoprecipitation of pSTAT1 in B cells heterozygous for rs6590330 confirmed that the risk allele increased binding to the active form of STAT1. Analysis with expression quantitative trait loci indicated that the risk allele of rs6590330 is associated with decreased ETS1 expression in Han Chinese, but not other ancestral cohorts. We propose a model in which the risk allele of rs6590330 is associated with decreased ETS1 expression and increases SLE risk by enhancing the binding of pSTAT1.

Published

2015

45. Regulation of inflammatory transcription factors by heat shock protein 70 in primary cultured astrocytes exposed to oxygen–glucose deprivation

Author

Kim, JY, Yenari, MA, and Lee, JE

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Genetics, Biotechnology, 1.1 Normal biological development and functioning, Underpinning research, Animals, Astrocytes, Brain Ischemia, Encephalitis, Glucose, HSP70 Heat-Shock Proteins, Heat-Shock Response, I-kappa B Proteins, JNK Mitogen-Activated Protein Kinases, MAP Kinase Signaling System, Mice, Inbred ICR, NF-kappa B, Oxygen, Phosphorylation, Primary Cell Culture, STAT1 Transcription Factor, Transcription Factor AP-1, ischemic injury, inflammation, 70-kDa heat shock protein, transcription factors, phosphorylation, Cognitive Sciences, Neurology & Neurosurgery, Biological psychology

Abstract

Inflammation is an important event in ischemic injury. These immune responses begin with the expression of pro-inflammatory genes modulating transcription factors, such as nuclear factor-κB (NF-κB), activator protein-1 (AP-1), and signal transducers and activator of transcription-1 (STAT-1). The 70-kDa heat shock protein (Hsp70) can both induce and arrest inflammatory reactions and lead to improved neurological outcome in experimental brain injury and ischemia. Since Hsp70 are induced under heat stress, we investigated the link between Hsp70 neuroprotection and phosphorylation of inhibitor of κB (IκB), c-Jun N-terminal kinases (JNK) and p38 through co-immunoprecipitation and enzyme-linked immunosorbent assay (ELISA) assay. Transcription factors and pro-inflammatory genes were quantified by immunoblotting, electrophoretic-mobility shift assay and reverse transcription-polymerase chain reaction assays. The results showed that heat stress led to Hsp70 overexpression which rendered neuroprotection after ischemia-like injury. Overexpression Hsp70 also interrupts the phosphorylation of IκB, JNK and p38 and blunts DNA binding of their transcription factors (NF-κB, AP-1 and STAT-1), effectively downregulating the expression of pro-inflammatory genes in heat-pretreated astrocytes. Taken together, these results suggest that overexpression of Hsp70 may protect against brain ischemia via an anti-inflammatory mechanism by interrupting the phosphorylation of upstream of transcription factors.

Published

2015

46. Positive feedback regulation of type I interferon by the interferon‐stimulated gene STING

Author

Ma, Feng, Li, Bing, Yu, Yongxin, Iyer, Shankar S, Sun, Mingyu, and Cheng, Genhong

Subjects

Genetics, HIV/AIDS, Underpinning research, 1.1 Normal biological development and functioning, Inflammatory and immune system, Animals, Binding Sites, Cell Line, Immunity, Innate, Interferon Type I, Interferons, Male, Membrane Proteins, Mice, Mice, Knockout, Promoter Regions, Genetic, Receptor, Interferon alpha-beta, STAT1 Transcription Factor, CDN, cGAMP, IFN, ISG, STING, Biochemistry and Cell Biology, Developmental Biology

Abstract

Stimulator of interferon genes (STING) is an important regulator of the innate immune response to cytoplasmic DNA. However, regulation of STING itself is largely unknown. Here, we show that STING transcription is induced by innate immune activators, such as cyclic dinucleotides (CDNs), through an IFNAR1- and STAT1-dependent pathway. We also identify a STAT1 binding site in the STING promoter that contributes to the activation of STING transcription. Furthermore, we show that induction of STING mediates the positive feedback regulation of CDN-triggered IFN-I. Thus, our study demonstrates that STING is an interferon-stimulated gene (ISG) and its induction is crucial for the IFN-I positive feedback loop.

Published

2015

47. Abnormal Mammary Development in 129:STAT1-Null Mice is Stroma-Dependent.

Author

Chen, Jane Q, Mori, Hidetoshi, Cardiff, Robert D, Trott, Josephine F, Hovey, Russell C, Hubbard, Neil E, Engelberg, Jesse A, Tepper, Clifford G, Willis, Brandon J, Khan, Imran H, Ravindran, Resmi K, Chan, Szeman R, Schreiber, Robert D, and Borowsky, Alexander D

Subjects

Epithelium, Mammary Glands, Animal, Stromal Cells, Animals, Mice, Knockout, Mice, Breast Neoplasms, Disease Models, Animal, Hormones, Cytokines, Cluster Analysis, Gene Expression Profiling, Female, STAT1 Transcription Factor, Isografts, Mammary Glands, Animal, Knockout, Disease Models, General Science & Technology

Abstract

Female 129:Stat1-null mice (129S6/SvEvTac-Stat1(tm1Rds) homozygous) uniquely develop estrogen-receptor (ER)-positive mammary tumors. Herein we report that the mammary glands (MG) of these mice have altered growth and development with abnormal terminal end buds alongside defective branching morphogenesis and ductal elongation. We also find that the 129:Stat1-null mammary fat pad (MFP) fails to sustain the growth of 129S6/SvEv wild-type and Stat1-null epithelium. These abnormalities are partially reversed by elevated serum progesterone and prolactin whereas transplantation of wild-type bone marrow into 129:Stat1-null mice does not reverse the MG developmental defects. Medium conditioned by 129:Stat1-null epithelium-cleared MFP does not stimulate epithelial proliferation, whereas it is stimulated by medium conditioned by epithelium-cleared MFP from either wild-type or 129:Stat1-null females having elevated progesterone and prolactin. Microarrays and multiplexed cytokine assays reveal that the MG of 129:Stat1-null mice has lower levels of growth factors that have been implicated in normal MG growth and development. Transplanted 129:Stat1-null tumors and their isolated cells also grow slower in 129:Stat1-null MG compared to wild-type recipient MG. These studies demonstrate that growth of normal and neoplastic 129:Stat1-null epithelium is dependent on the hormonal milieu and on factors from the mammary stroma such as cytokines. While the individual or combined effects of these factors remains to be resolved, our data supports the role of STAT1 in maintaining a tumor-suppressive MG microenvironment.

Published

2015

48. The Interferon Signaling Antagonist Function of Yellow Fever Virus NS5 Protein Is Activated by Type I Interferon

Author

Laurent-Rolle, Maudry, Morrison, Juliet, Rajsbaum, Ricardo, Macleod, Jesica M Levingston, Pisanelli, Giuseppe, Pham, Alissa, Ayllon, Juan, Miorin, Lisa, Martínez-Romero, Carles, tenOever, Benjamin R, and García-Sastre, Adolfo

Subjects

Biochemistry and Cell Biology, Biological Sciences, Emerging Infectious Diseases, Infectious Diseases, Biodefense, Vaccine Related, Prevention, Infection, Amino Acid Motifs, Animals, Cell Line, GTP-Binding Proteins, Host-Pathogen Interactions, Humans, Interferon-beta, Phosphorylation, Protein Binding, STAT1 Transcription Factor, STAT2 Transcription Factor, Signal Transduction, Viral Nonstructural Proteins, Yellow Fever, Yellow fever virus, Microbiology, Medical Microbiology, Immunology, Biochemistry and cell biology, Medical microbiology

Abstract

To successfully establish infection, flaviviruses have to overcome the antiviral state induced by type I interferon (IFN-I). The nonstructural NS5 proteins of several flaviviruses antagonize IFN-I signaling. Here we show that yellow fever virus (YFV) inhibits IFN-I signaling through a unique mechanism that involves binding of YFV NS5 to the IFN-activated transcription factor STAT2 only in cells that have been stimulated with IFN-I. This NS5-STAT2 interaction requires IFN-I-induced tyrosine phosphorylation of STAT1 and the K63-linked polyubiquitination at a lysine in the N-terminal region of YFV NS5. We identified TRIM23 as the E3 ligase that interacts with and polyubiquitinates YFV NS5 to promote its binding to STAT2 and trigger IFN-I signaling inhibition. Our results demonstrate the importance of YFV NS5 in overcoming the antiviral action of IFN-I and offer a unique example of a viral protein that is activated by the same host pathway that it inhibits.

Published

2014

49. Unanchored K48-Linked Polyubiquitin Synthesized by the E3-Ubiquitin Ligase TRIM6 Stimulates the Interferon-IKKε Kinase-Mediated Antiviral Response

Author

Rajsbaum, Ricardo, Versteeg, Gijs A, Schmid, Sonja, Maestre, Ana M, Belicha-Villanueva, Alan, Martínez-Romero, Carles, Patel, Jenish R, Morrison, Juliet, Pisanelli, Giuseppe, Miorin, Lisa, Laurent-Rolle, Maudry, Moulton, Hong M, Stein, David A, Fernandez-Sesma, Ana, tenOever, Benjamin R, and García-Sastre, Adolfo

Subjects

Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Animals, Antiviral Agents, Cells, Cultured, Enzyme Activation, Humans, I-kappa B Kinase, Interferon Type I, Janus Kinase 1, Mice, Phosphorylation, Polyubiquitin, RNA Interference, RNA, Small Interfering, STAT1 Transcription Factor, Signal Transduction, Tripartite Motif Proteins, Ubiquitin-Conjugating Enzymes, Ubiquitin-Protein Ligases

Abstract

Type I interferons (IFN-I) are essential antiviral cytokines produced upon microbial infection. IFN-I elicits this activity through the upregulation of hundreds of IFN-I-stimulated genes (ISGs). The full breadth of ISG induction demands activation of a number of cellular factors including the IκB kinase epsilon (IKKε). However, the mechanism of IKKε activation upon IFN receptor signaling has remained elusive. Here we show that TRIM6, a member of the E3-ubiquitin ligase tripartite motif (TRIM) family of proteins, interacted with IKKε and promoted induction of IKKε-dependent ISGs. TRIM6 and the E2-ubiquitin conjugase UbE2K cooperated in the synthesis of unanchored K48-linked polyubiquitin chains, which activated IKKε for subsequent STAT1 phosphorylation. Our work attributes a previously unrecognized activating role of K48-linked unanchored polyubiquitin chains in kinase activation and identifies the UbE2K-TRIM6-ubiquitin axis as critical for IFN signaling and antiviral response.

Published

2014

50. Otopetrin 1 Protects Mice From Obesity-Associated Metabolic Dysfunction Through Attenuating Adipose Tissue Inflammation

Author

Wang, Guo-Xiao, Cho, Kae Won, Uhm, Maeran, Hu, Chun-Rui, Li, Siming, Cozacov, Zoharit, Xu, Acer E, Cheng, Ji-Xin, Saltiel, Alan R, Lumeng, Carey N, and Lin, Jiandie D

Subjects

Biomedical and Clinical Sciences, Liver Disease, Digestive Diseases, Diabetes, Obesity, Nutrition, Prevention, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Cardiovascular, Metabolic and endocrine, Stroke, Oral and gastrointestinal, Adipose Tissue, Adipose Tissue, White, Animals, Diet, High-Fat, Homeostasis, Inflammation, Insulin Resistance, Interferon-gamma, Male, Membrane Proteins, Mice, STAT1 Transcription Factor, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

Chronic low-grade inflammation is emerging as a pathogenic link between obesity and metabolic disease. Persistent immune activation in white adipose tissue (WAT) impairs insulin sensitivity and systemic metabolism, in part, through the actions of proinflammatory cytokines. Whether obesity engages an adaptive mechanism to counteract chronic inflammation in adipose tissues has not been elucidated. Here we identified otopetrin 1 (Otop1) as a component of a counterinflammatory pathway that is induced in WAT during obesity. Otop1 expression is markedly increased in obese mouse WAT and is stimulated by tumor necrosis factor-α in cultured adipocytes. Otop1 mutant mice respond to high-fat diet with pronounced insulin resistance and hepatic steatosis, accompanied by augmented adipose tissue inflammation. Otop1 attenuates interferon-γ (IFN-γ) signaling in adipocytes through selective downregulation of the transcription factor STAT1. Using a tagged vector, we found that Otop1 physically interacts with endogenous STAT1. Thus, Otop1 defines a unique target of cytokine signaling that attenuates obesity-induced adipose tissue inflammation and plays an adaptive role in maintaining metabolic homeostasis in obesity.

Published

2014