Your search keyword '"Stephen Ullrich"' showing total 24 results

1. Raxibacumab for the Treatment of Inhalational Anthrax

Author

John Zhong, Thi Sau Migone, Andrew Chen, Al Corey, Stephen Ullrich, Karen Gillum, Janelle Zimmerman, Matt Devalaraja, Daniel C. Sanford, Larry Lo, Sally D. Bolmer, G. Mani Subramanian, Gabriel T. Meister, Letha M. Healey, Jason M. Mott, and Maggie Lewis

Subjects

Adult, Male, Adolescent, medicine.drug_class, Anthrax toxin, Drug Evaluation, Preclinical, Bacteremia, Antibodies, Monoclonal, Humanized, Monoclonal antibody, Placebo, Median lethal dose, Anthrax, Random Allocation, Young Adult, Anti-Infective Agents, Ciprofloxacin, medicine, Clinical endpoint, Animals, Humans, Respiratory Tract Infections, Aerosolization, Aged, Aged, 80 and over, biology, business.industry, Antibodies, Monoclonal, General Medicine, Middle Aged, biology.organism_classification, Antibodies, Bacterial, Survival Analysis, Bacillus anthracis, Macaca fascicularis, Immunoglobulin G, Immunology, Drug Therapy, Combination, Female, Rabbits, Raxibacumab, business, medicine.drug

Abstract

Inhalational anthrax caused by Bacillus anthracis is associated with high mortality primarily due to toxin-mediated injury. Raxibacumab is a human IgG1lambda monoclonal antibody directed against protective antigen, a component of the anthrax toxin.We evaluated the efficacy of raxibacumab as a prophylactic agent and after disease onset in a total of four randomized, placebo-controlled studies conducted in rabbits and monkeys. Animals were exposed to an aerosolized target exposure of B. anthracis spores that was approximately 100 times (in the prophylactic studies) and 200 times (in the therapeutic-intervention studies) the median lethal dose. In the therapeutic-intervention studies, animals were monitored for the onset of symptoms. Animals with detectable protective antigen in serum, a significant increase in temperature, or both received a single intravenous bolus of placebo or raxibacumab at a dose of either 20 mg per kilogram of body weight or 40 mg per kilogram. The primary end point was survival at day 14 (in rabbits) or at day 28 (in monkeys). Safety studies were conducted with intravenous raxibacumab (40 mg per kilogram) in 333 healthy human volunteers.In both rabbits and monkeys, the time to detection of protective antigen correlated with the time to bacteremia (r=0.9, P0.001). In the therapeutic-intervention studies, the survival rate was significantly higher among rabbits that received raxibacumab at a dose of 40 mg per kilogram (44% [8 of 18]) than among rabbits that received placebo (0% [0 of 18]; P=0.003). Raxibacumab treatment also significantly increased survival in monkeys (64% [9 of 14], vs. 0% [0 of 12] with placebo; P0.001). In human subjects, intravenous raxibacumab at a dose of 40 mg per kilogram had a half-life of 20 to 22 days and provided a maximum concentration of the drug in excess of levels that are protective in animals. Concentrations of raxibacumab provide a surrogate end point that should be predictive of clinical benefit.A single dose of raxibacumab improved survival in rabbits and monkeys with symptomatic inhalational anthrax. (ClinicalTrials.gov number, NCT00639678.)

Published

2009

2. Osteostat/Tumor Necrosis Factor Superfamily 18 Inhibits Osteoclastogenesis and Is Selectively Expressed by Vascular Endothelial Cells

Author

Stephen Ullrich, Yun Hee Cho, Liubov Zaritskaya, Charles E. Birse, Paul A. Moore, Clint Lincoln, Bernardetta Nardelli, Wendy Halpern, Yansong Ni, and William J. McAuliffe

Subjects

medicine.medical_specialty, Endothelium, medicine.medical_treatment, Acid Phosphatase, Osteoclasts, Receptors, Cytoplasmic and Nuclear, Biology, Vascular endothelial growth inhibitor, Monocytes, Receptors, Tumor Necrosis Factor, Open Reading Frames, Endocrinology, Osteoprotegerin, Osteoclast, Internal medicine, medicine, Humans, RNA, Messenger, DNA Primers, Glycoproteins, Oligonucleotide Array Sequence Analysis, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, Tartrate-Resistant Acid Phosphatase, Activator (genetics), Cell Membrane, Recombinant Proteins, Cell biology, Isoenzymes, Endothelial stem cell, medicine.anatomical_structure, Cytokine, Tumor Necrosis Factors, Immunology, Tumor necrosis factor alpha, Endothelium, Vascular

Abstract

Vascular endothelial cells (EC) participate in the process of bone formation through the production of factors regulating osteoclast differentiation and function. In this study, we report the selective expression in primary human microvascular EC of Osteostat/TNF superfamily 18, a ligand of the TNF superfamily. Osteostat protein is detectable in human microvascular EC and is highly up-regulated by IFN-α and IFN-β. Moreover, an anti-Osteostat antibody strongly binds to the vascular endothelium in human tissues, demonstrating that the protein is present in the EC layers surrounding blood vessels. Functional in vitro assays were used to define Osteostat involvement in osteoclastogenesis. Both recombinant and membrane-bound Osteostat inhibit differentiation of osteoclasts from monocytic precursor cells. Osteostat suppresses the early stage of osteoclastogenesis via inhibition of macrophage colony-stimulating factor-induced receptor activator of NF-κB (RANK) expression in the osteoclast precursor cells. This effect appears to be specific for the differentiation pathway of the osteoclast lineage, because Osteostat does not inhibit lipopolysaccharide-induced RANK expression in monocytes and dendritic cells, or activation-induced RANK expression in T cells. These findings demonstrate that Osteostat is a novel regulator of osteoclast generation and substantiate the major role played by the endothelium in bone physiology.

Published

2006

3. TL1A Is a TNF-like Ligand for DR3 and TR6/DcR3 and Functions as a T Cell Costimulator

Author

Stephen Ullrich, Ping Feng, Jun Zhang, Cecil Chen, Sunghee Kim, Palanisamy Kanakaraj, Reiner L. Gentz, Jeffrey Carrell, Ding Liu, Gang Hu, Ping Wei, Paul A. Moore, Ernest Boyd, Steve Ruben, Bugen Hu, Laurie Pukac, June S. Hong, Xia Luo, Henrik S. Olsen, Joe X. H. Zhou, Yun Hee Cho, James W. Perry, Su Fang Chen, Jian Ni, Thi Sau Migone, and Li Zhuang

Subjects

Tumor Necrosis Factor Ligand Superfamily Member 15, T-Lymphocytes, T cell, Molecular Sequence Data, Immunology, Receptors, Cell Surface, Biology, Ligands, Lymphocyte Activation, Receptors, Tumor Necrosis Factor, Proinflammatory cytokine, TCIRG1, Mice, medicine, Animals, Humans, Immunology and Allergy, Cytotoxic T cell, Amino Acid Sequence, Receptor, Receptors, Tumor Necrosis Factor, Member 25, Membrane Glycoproteins, Tumor Necrosis Factor-alpha, Receptors, Tumor Necrosis Factor, Member 6b, Cell biology, Infectious Diseases, medicine.anatomical_structure, Tumor necrosis factor alpha, Decoy receptor 3, Sequence Alignment, Death receptor 3, Interleukin-1

Abstract

DR3 is a death domain-containing receptor that is upregulated during T cell activation and whose overexpression induces apoptosis and NF-kappaB activation in cell lines. Here we show that an endothelial cell-derived TNF-like factor, TL1A, is a ligand for DR3 and decoy receptor TR6/DcR3 and that its expression is inducible by TNF and IL-1alpha. TL1A induces NF-kappaB activation and apoptosis in DR3-expressing cell lines, while TR6-Fc protein antagonizes these signaling events. Interestingly, in T cells, TL1A acts as a costimulator that increases IL-2 responsiveness and secretion of proinflammatory cytokines both in vitro and in vivo. Our data suggest that interaction of TL1A with DR3 promotes T cell expansion during an immune response, whereas TR6 has an opposing effect.

Published

2002

4. BLyS BINDS TO B CELLS WITH HIGH AFFINITY AND INDUCES ACTIVATION OF THE TRANSCRIPTION FACTORS NF-κB AND ELF-1

Author

Theodora W. Salcedo, Stephen Ullrich, Bernardetta Nardelli, Yuxiang Gan, Thi-Sau Migone, Henrik S. Olsen, Yuling Li, Palanisamy Kanakaraj, David M. Hilbert, Judith Giri, Erika Cochrane, and Thomas Kaufman

Subjects

Immunology, In Vitro Techniques, Biochemistry, Iodine Radioisotopes, chemistry.chemical_compound, B-Cell Activating Factor, Humans, Immunology and Allergy, Binding site, Protein Structure, Quaternary, B-cell activating factor, Receptor, Molecular Biology, Transcription factor, B-Lymphocytes, Binding Sites, biology, Tumor Necrosis Factor-alpha, Kinase, NF-kappa B, Membrane Proteins, NF-κB, Hematology, Molecular biology, Recombinant Proteins, In vitro, DNA-Binding Proteins, Kinetics, Cross-Linking Reagents, chemistry, biology.protein, Antibody, Protein Binding, Signal Transduction, Transcription Factors

Abstract

B lymphocyte stimulator (BLyS) is a novel member of the TNF family of proteins expressed by myeloid cells as membrane-bound and soluble forms. BLyS was shown to act specifically on B cells, inducing proliferation and immunoglobulin production both in vitro and in vivo. The present study was undertaken to characterize binding of radiolabeled BLyS to its cognate receptor on human B lymphocytes and examine intracellular events initiated by BLyS binding. Similar to other TNF family members, BLyS is present in solution as a homotrimer as determined by gel filtration chromatography and light scattering analysis. BLyS binding to B cells is specific as other TNF family members tested did not compete for 125 I-BLyS binding. Analysis of equilibrium binding of 125 I-labeled BLyS to purified human tonsillar B cells demonstrated saturable binding. Scatchard analysis of the binding data revealed a single class of high-affinity binding on human B cells with approximately 2600 binding sites per cell and an apparent dissociation constant (K D ) of about 0.1 nM. In addition we report that BLyS binding to B cells results in the activation of NF-κB and the Ets family transcription factor, ELF-1, and in the induction of mRNA for Polo-like kinase (PLK).

Published

2001

5. Tumor Necrosis Factor (TNF) Receptor Superfamily Member TACI Is a High Affinity Receptor for TNF Family Members APRIL and BLyS

Author

Yuxiang Gan, Jeff Carrell, Paul A. Moore, Donna Dimke, Steve Ruben, David W. Lafleur, Youmei Wu, Ping Feng, Palanisamy Kanakaraj, Thi Sau Migone, Kevin P. Baker, Ping Wei, Stephen Ullrich, Bernardetta Nardelli, Yun Hee Cho, Kara Taylor, Andy Garcia, Dana Bressette, Thomas Kaufman, Elisa Gollatz, and Henrik S. Olsen

Subjects

DNA, Complementary, Time Factors, Recombinant Fusion Proteins, Transmembrane Activator and CAML Interactor Protein, Ligands, Transfection, Polymerase Chain Reaction, Biochemistry, Receptors, Tumor Necrosis Factor, Cell Line, Humans, RNA, Messenger, Receptor, BAFF receptor, B-cell activating factor, Molecular Biology, Gene Library, B-Lymphocytes, Dose-Response Relationship, Drug, Reverse Transcriptase Polymerase Chain Reaction, Tumor Necrosis Factor-alpha, Chemistry, Transmembrane activator and CAML interactor, Cell Membrane, Neuropeptides, HEK 293 cells, Membrane Proteins, Nuclear Proteins, Cell Biology, Flow Cytometry, Fusion protein, Molecular biology, Kinetics, Cancer research, Tumor necrosis factor alpha, Signal transduction, B-Cell Activation Factor Receptor, Protein Binding, Signal Transduction

Abstract

An expression cloning approach was employed to identify the receptor for B-lymphocyte stimulator (BLyS) and identified the tumor necrosis factor receptor superfamily member TACI as a BLyS-binding protein. Expression of TACI in HEK293T cells confers on the cells the ability to bind BLyS with subnanomolar affinity. Furthermore, a TACI-Fc fusion protein recognizes both the cleaved, soluble form of BLyS as well as the membrane BLyS present on the cell surface of a recombinant cell line. TACI mRNA is found predominantly in B-cells and correlates with BLyS binding in a panel of B-cell lines. We also demonstrate that TACI interacts with nanomolar affinity with the BLyS-related tumor necrosis factor homologue APRIL for which no clear in vivo role has been described. BLyS and APRIL are capable of signaling through TACI to mediate NF-kappaB responses in HEK293 cells. We conclude that TACI is a receptor for BLyS and APRIL and discuss the implications for B-cell biology.

Published

2000

6. A Novel Cytokine Receptor-Ligand Pair

Author

Henrik S. Olsen, Yun Hee Cho, Kevin Connolly, Wei Wang, Yanggu Shi, Jeffrey Carrell, Kirsten A. Wilkinson, Jun Zhang, Carrie L. Fisher, Irina Knyazev, Vermettya Hodge, Karen Wathen, Viktor Kao, Steve Ruben, Melisa C. Barber, Krzysztof J. Grzegorzewski, Stephen Ullrich, and Reinhard Ebner

Subjects

Chinese hamster ovary cell, medicine.medical_treatment, Cell Biology, Biology, Biochemistry, Molecular biology, Transmembrane protein, Proinflammatory cytokine, Biological pathway, Cytokine, Secretory protein, Complementary DNA, medicine, Cytokine receptor, Molecular Biology

Abstract

As part of a large scale effort to discover novel secreted proteins, a cDNA encoding a novel cytokine was identified. Alignments of the sequence of the new protein, designated IL-17B, suggest it to be a homolog of the recently described T cell-derived cytokine, IL-17. By Northern analysis, EST distribution and real-time quantitative polymerase chain reaction analysis, mRNA was detected in many cell types. A novel type I transmembrane protein, identified in an EST data base by homology to IL-17R, was found to bind specifically IL-17B, as determined by surface plasmon resonance analysis, flow cytometry, and co-immunoprecipitation experiments. Readily detectable transcription of IL-17BR was restricted to human kidney, pancreas, liver, brain, and intestines and only a few of the many cell lines tested. By using a rodent ortholog of IL-17BR as a probe, IL-17BR message was found to be drastically up-regulated during intestinal inflammation elicited by indomethacin treatment in rats. In addition, intraperitoneal injection of IL-17B purified from Chinese hamster ovary cells caused marked neutrophil migration in normal mice, in a specific and dose-dependent manner. Together these results suggest that IL-17B may be a novel proinflammatory cytokine acting on a restricted set of target cell types. They also demonstrate the strength of genomic approaches in the unraveling of novel biological pathways.

Published

2000

7. Abstract A05: Targeting the EMT-immunosuppression loop in lung cancer as a strategy to prevent metastasis

Author

Limo Chen, Yanyan Lou, John Heymach, Ignacio Wistuba, Stephen Ullrich, Xiao-Feng Qin, and Don Gibbons

Subjects

Cancer Research, Oncology

Abstract

This abstract is being presented as a short talk in the scientific program. A full abstract is printed in the Proffered Abstracts section (PR01) of the Conference Proceedings. Citation Format: Limo Chen, Yanyan Lou, John Heymach, Ignacio Wistuba, Stephen Ullrich, Xiao-Feng Qin, Don Gibbons. Targeting the EMT-immunosuppression loop in lung cancer as a strategy to prevent metastasis. [abstract]. In: Proceedings of the AACR Special Conference on Tumor Metastasis; 2015 Nov 30-Dec 3; Austin, TX. Philadelphia (PA): AACR; Cancer Res 2016;76(7 Suppl):Abstract nr A05.

Published

2016

8. Immune Modulation by Dermal Exposure to Jet Fuel

Author

Gerardo Ramos and Stephen Ullrich

Published

2010

9. Inhibition by brefeldin A of presentation of exogenous protein antigens to MHC class II-restricted T cells

Author

Serge Y. Fuchs, Luciano Adorini, Stephen Ullrich, and Ettore Appella

Subjects

Ovalbumin, T-Lymphocytes, Antigen presentation, CD1, Antigen-Presenting Cells, Cyclopentanes, In Vitro Techniques, Cell Line, Mice, Antigen, MHC class I, Animals, Antigens, Antigen-presenting cell, MHC class II, Brefeldin A, Multidisciplinary, biology, Antigen processing, Histocompatibility Antigens Class II, MHC restriction, Molecular biology, Cell Compartmentation, Cell biology, Solubility, biology.protein, Muramidase, Peptides

Abstract

Peptides bound to class I or class II major histocompatibility complex (MHC)-encoded molecules are ligands for the antigen-specific T-cell receptor of T-cells carrying the CD8 and CD4 antigens, respectively. MHC class I-restricted T cells generally recognize peptides derived from processing of endogenously synthesized cellular antigens, whereas class II-restricted T cells usually recognize peptides derived from exogenous antigens entering antigen presenting cells. Accordingly, two separate pathways of antigen processing and presentation have been proposed. The fungal metabolite brefeldin A (BFA), an inhibitor of protein transport from the endoplasmic reticulum, inhibits presentation of endogenous antigens for MHC-restricted T-cell recognition. The selectivity of BFA activity has been inferred to reflect presentation of a given antigen processed through the cytosolic or the endocytic route. Here we show that BFA also greatly inhibits the presentation of exogenous protein antigens by MHC class II molecules to T cells, indicating a broader effect of this drug on antigen presentation and an additional similarity between the two processing pathways. As cycloheximide, a protein synthesis inhibitor, also inhibits presentation of protein antigens to class II-restricted T cells, the data indicate that peptides generated by processing of exogenous proteins binds to newly synthesized class II molecules for presentation to T cells.

Published

1990

10. The remarkable flexibility of the human antibody repertoire; isolation of over one thousand different antibodies to a single protein, BLyS

Author

Sarah Helen Main, Ralph Minter, Bryan M. Edwards, Stephen Ullrich, Jane Wilton, Elizabeth Williams, Gil H. Choi, Vivian R. Albert, Tristan J. Vaughan, Leila Du Fou, Steven C. Barash, and Steve Ruben

Subjects

Phage display, Molecular Sequence Data, Biology, Immunoglobulin light chain, Antibodies, Immune system, Antibody Repertoire, Antigen, Structural Biology, Peptide Library, B-Cell Activating Factor, Humans, Point Mutation, Amino Acid Sequence, Molecular Biology, Peptide sequence, Phylogeny, Genetics, Tumor Necrosis Factor-alpha, Membrane Proteins, Antibody Diversity, Molecular biology, Complementarity Determining Regions, biology.protein, Immunoglobulin Light Chains, Antibody, Immunoglobulin Heavy Chains

Abstract

It is well established that the humoral immune response can generate antibodies to many different antigens. The antibody diversity required to achieve this is believed to be substantial. However, the extent to which the immune repertoire can generate structural diversity against a single target antigen has never been addressed. Here, we have used phage display to demonstrate the extraordinary capacity of the human antibody repertoire. Over 1000 antibodies, all different in amino acid sequence, were generated to a single protein, B-lymphocyte stimulator (BLyS protein). This is a highly diverse panel of antibodies as exemplified by the extensive heavy and light chain germline usage: 42/49 functional heavy chain germlines and 19/33 V(lambda) and 13/35 V(kappa) light chain germlines were all represented in the panel of antibodies. Moreover, a high level of sequence diversity was observed in the V(H) CDR3 domains of these antibodies, with 568 different amino acid sequences identified. Thus we have demonstrated that specific recognition of a single antigen can be achieved from many different VDJ combinations, illustrating the remarkable problem-solving ability of the human immune repertoire. When studied in a biochemical assay, around 500 (40%) of these antibodies inhibited the binding of BLyS to its receptors on B-cell lines. The most potent antibodies inhibited BLyS binding with sub-nanomolar IC(50) values and with sub-nanomolar affinities. Such antibodies provide excellent choices as candidates for the treatment of BLyS-associated autoimmune diseases.

Published

2003

11. BLyS and APRIL form biologically active heterotrimers that are expressed in patients with systemic immune-based rheumatic diseases

Author

Stephen Ullrich, Rodger Smith, Kevin P. Baker, Viktor Roschke, David M. Hilbert, Svetlana Sosnovtseva, Christopher D. Ward, Thi-Sau Migone, Bernardetta Nardelli, William Stohl, June S. Hong, and Vivian R. Albert

Subjects

Immunology, Tumor Necrosis Factor Ligand Superfamily Member 13, Lymphocyte Activation, Transfection, Arthritis, Reactive, Atacicept, Receptors, Tumor Necrosis Factor, Cell Line, Arthritis, Rheumatoid, Mice, Immune system, Heterotrimeric G protein, Rheumatic Diseases, medicine, Tumor Cells, Cultured, Immunology and Allergy, Animals, Humans, Lupus Erythematosus, Systemic, Spondylitis, Ankylosing, Receptor, BAFF receptor, B-cell activating factor, Cells, Cultured, B-Lymphocytes, Mice, Inbred BALB C, Lupus erythematosus, business.industry, Tumor Necrosis Factor-alpha, Arthritis, Psoriatic, Membrane Proteins, medicine.disease, Polymyositis, Tumor necrosis factor alpha, Female, business, B-Cell Activation Factor Receptor

Abstract

BLyS and APRIL are two members of the TNF superfamily that are secreted by activated myeloid cells and have costimulatory activity on B cells. BLyS and APRIL share two receptors, TACI and BCMA, whereas a third receptor, BAFF-R, specifically binds BLyS. Both BLyS and APRIL have been described as homotrimeric molecules, a feature common to members of the TNF superfamily. In this study, we show that APRIL and BLyS can form active heterotrimeric molecules when coexpressed and that circulating heterotrimers are present in serum samples from patients with systemic immune-based rheumatic diseases. These findings raise the possibility that active BLyS/APRIL heterotrimers may play a role in rheumatic and other autoimmune diseases and that other members of the TNF ligand superfamily may also form active soluble heterotrimers.

Published

2002

12. Modulation of T-cell responses to alloantigens by TR6/DcR3

Author

Theodora W. Salcedo, Ping Feng, Jiangping Wu, Theresa Gregorio, Jun Zhang, Stephen Ullrich, Yuling Li, Xiaochun Wan, Shijie Qi, Huifang Chen, Bugen Hu, Paul A. Moore, and Yun Hee Cho

Subjects

Isoantigens, Tumor Necrosis Factor Ligand Superfamily Member 14, T cell, Recombinant Fusion Proteins, T-Lymphocytes, Immunoblotting, Mice, Transgenic, Receptors, Cell Surface, Biology, Fas ligand, Receptors, Tumor Necrosis Factor, Article, Cell Line, Mice, Immune system, medicine, Cytotoxic T cell, Animals, Humans, Receptor, Mice, Inbred BALB C, Membrane Glycoproteins, Interleukin-6, Tumor Necrosis Factor-alpha, HEK 293 cells, Receptors, Tumor Necrosis Factor, Member 6b, Lymphokine, Granulocyte-Macrophage Colony-Stimulating Factor, Interferon-alpha, Membrane Proteins, General Medicine, Flow Cytometry, Molecular biology, Precipitin Tests, Interleukin-10, Mice, Inbred C57BL, medicine.anatomical_structure, Heart Transplantation, Tumor necrosis factor alpha, Female, Spleen

Abstract

TR6 (DcR3) is a new member of the TNF receptor (TNFR) family that lacks a transmembrane domain in its sequence, indicating that it is a secreted molecule. TR6 can bind to FasL and prevent FasL-induced apoptosis; it can also associate with LIGHT, another TNF family member. The role of TR6 in immune responses was investigated in this study. According to flow cytometry, recombinant human TR6-Fc binds to human LIGHT expressed on 293 cells or on activated human T cells and competes with the LIGHT receptor TR2 for the binding to LIGHT on these cells. Human TR6 could cross-react with mouse LIGHT in immunoprecipitation. TR6-Fc also downregulates cytotoxic T lymphocyte activity in vitro and graft-versus-host responses in mice. Moreover, TR6-Fc modulates lymphokine production by alloantigen-stimulated mouse T cells. TR6-Fc ameliorated rejection response to mouse heart allograft. These results indicate that TR6 can dampen T-cell responses to alloantigens. Such regulatory effects of TR6 probably occur via interference with interaction between pairs of related TNF and TNFR family members, LIGHT/TR2 being one of the possible candidate pairs.

Published

2001

13. Preparation and characterization of recombinant tissue inhibitor of metalloproteinase 4 (TIMP-4)

Author

Mingsheng Wang, Yiliang E. Liu, Jeffery L. Su, Stephen Ullrich, Preston Alexander, Shijie Sheng, Y. Eric Shi, Qing-Xiang Amy Sang, John M. Greene, and Hui Li

Subjects

Breast Neoplasms, Matrix metalloproteinase, Biochemistry, law.invention, Western blot, law, medicine, Humans, Neoplasm Invasiveness, Molecular Biology, Glycoproteins, Gel electrophoresis, chemistry.chemical_classification, medicine.diagnostic_test, Chemistry, Tissue Inhibitor of Metalloproteinases, Cell Biology, Tissue inhibitor of metalloproteinase, Molecular biology, Recombinant Proteins, Cancer cell, Recombinant DNA, Female, Glycoprotein, Extracellular Matrix Degradation

Abstract

TIMP-4, a novel human tissue inhibitor of metalloproteinase, was identified and cloned (Greene, J., Wang, M., Raymond, L. A., Liu, Y. E., Rosen, C., and Shi, Y. E. (1996) J. Biol. Chem. 271, 30375-30380). In this report, the production and characterization of recombinant TIMP-4 (rTIMP4p) are described. rTIMP4p, expressed in baculovirus-infected insect cells, was purified to homogeneity by a combination of cation exchange, hydrophobic, and size-exclusion chromatographies. The purified protein migrated as a single 23-kDa band in SDS-polyacrylamide gel electrophoresis and in Western blot using a specific anti-TIMP-4 antibody. Inhibition of matrix metalloproteinase (MMP) activities by rTIMP4p was demonstrated in five MMPs. Enzymatic kinetic studies revealed IC50 values (concentration at 50% inhibition) of 19, 3, 45, 8, and 83 nM for MMP-1, MMP-2, MMP-3, MMP-7, and MMP-9, respectively. Purified rTIMP4p demonstrated a strong inhibitory effect on the invasion of human breast cancer cells across reconstituted basement membranes. Thus, TIMP-4 is a new enzymatic inhibitor in MMP-mediated extracellular matrix degradation and may have therapeutic potential in treating cancer malignant progression.

Published

1997

14. STRL22 is a receptor for the CC chemokine MIP-3alpha

Author

Jeffrey Y. Su, Brent L. Kreider, Fang Liao, Joshua M. Farber, Ralph Alderson, and Stephen Ullrich

Subjects

Receptors, CCR6, Molecular Sequence Data, Biophysics, C-C chemokine receptor type 6, Biochemistry, Cell Line, CCL17, Humans, CCL15, Receptors, Cytokine, CCL13, Molecular Biology, Chemokine CCL20, Chemistry, Cell Biology, Macrophage Inflammatory Proteins, Molecular biology, CCL20, Chemokines, CC, Immunology, Cytokines, Receptors, Chemokine, Chemokines, CC chemokine receptors, CCL23, CCL21

Abstract

STRL22 is a human seven transmembrane domain orphan receptor related to known chemokine receptors and expressed in peripheral blood lymphocytes, tumor infiltrating lymphocytes and lymphoid tissues. MIP-3alpha/LARC/Exodus is a CC chemokine that is chemotactic for lymphocytes and that is expressed in activated cells, including monocytes, T cells, endothelial cells, and fibroblasts, and in liver, lung, and some lymphoid tissues. We report here that STRL22-transfected human embryonic kidney 293 cells demonstrated specific binding for MIP-3alpha and that MIP-3alpha, but no other chemokines, produced a calcium flux in the STRL22-transfected cells. We show that MIP-3alpha, unlike other chemokines, produced a calcium flux in freshly-isolated peripheral blood lymphocytes and we show that MIP-3alpha also produced a signal in tumor infiltrating lymphocytes that express STRL22. Since STRL22 is the sixth functional CC chemokine receptor identified, it should be re-named CCR6.

Published

1997

15. Fusion Toxin BLyS-Gelonin Inhibits Growth of Malignant Human B Cell Lines In Vitro and In Vivo

Author

Ipsita Mukherjee, Troy A. Luster, Luke Oh, Jeffrey Gill, Robin Humphreys, Yun Hee Cho, Stephen Ullrich, Lizbeth Kelly, Jeffrey Carrell, Andy Garcia, Thi-Sau Migone, and Christopher D. Ward

Subjects

B Cells, Mouse, Receptor expression, Cancer Treatment, lcsh:Medicine, Mice, SCID, Mice, Fusion Toxin, Molecular Cell Biology, Basic Cancer Research, B-Cell Activating Factor, Cytotoxic T cell, Lymphoid Organs, Gelonin, lcsh:Science, Cancers and neoplasms, Cellular Stress Responses, Non-Hodgkin lymphoma, Multidisciplinary, Animal Models, Flow Cytometry, Acute Lymphoblastic Leukemia, medicine.anatomical_structure, Oncology, Ribosome Inactivating Proteins, Type 1, Medicine, Lymphomas, Female, Cellular Types, Immunohistochemical Analysis, Research Article, Lymphoma, B-Cell, Cell Survival, Immune Cells, Recombinant Fusion Proteins, Immunology, Blotting, Western, B-cell receptor, Cytokine Therapy, Biology, Cell Line, Model Organisms, Hematopoietic Growth Factors, Cell surface receptor, Leukemias, medicine, Animals, Humans, B-cell activating factor, B cell, Blood Cells, lcsh:R, Xenograft Model Antitumor Assays, Molecular biology, Immune System, Hematologic cancers and related disorders, Immunologic Techniques, lcsh:Q, Cytometry

Abstract

B lymphocyte stimulator (BLyS) is a member of the TNF superfamily of cytokines. The biological activity of BLyS is mediated by three cell surface receptors: BR3/BAFF-R, TACI and BCMA. The expression of these receptors is highly restricted to B cells, both normal and malignant. A BLyS-gelonin fusion toxin (BLyS-gel) was generated consisting of the recombinant plant-derived toxin gelonin fused to the N-terminus of BLyS and tested against a large and diverse panel of B-NHL cell lines. Interestingly, B-NHL subtypes mantle cell lymphoma (MCL), diffuse large B cell lymphoma (DLBCL) and B cell precursor-acute lymphocytic leukemia (BCP-ALL) were preferentially sensitive to BLyS-gel mediated cytotoxicity, with low picomolar EC(50) values. BLyS receptor expression did not guarantee sensitivity to BLyS-gel, even though the construct was internalized by both sensitive and resistant cells. Resistance to BLyS-gel could be overcome by treatment with the endosomotropic drug chloroquine, suggesting BLyS-gel may become trapped within endosomal/lysosomal compartments in resistant cells. BLyS-gel induced cell death was caspase-independent and shown to be at least partially mediated by the "ribotoxic stress response." This response involves activation of p38 MAPK and JNK/SAPK, and BLyS-gel mediated cytotoxicity was inhibited by the p38/JNK inhibitor SB203580. Finally, BLyS-gel treatment was shown to localize to sites of disease, rapidly reduce tumor burden, and significantly prolong survival in xenograft mouse models of disseminated BCP-ALL, DLBCL, and MCL. Together, these findings suggest BLyS has significant potential as a targeting ligand for the delivery of cytotoxic "payloads" to malignant B cells.

Published

2012

16. Abstract 3861: Fusion toxin BLyS-gelonin inhibits growth of B-NHL cell lines in vitro and in vivo

Author

Ipsita Mukherjee, Jeffrey Carrell, Jeffrey Gill, Christopher D. Ward, Yun Hee Cho, Troy A. Luster, Robin Humphreys, Stephen Ullrich, Andy Garcia, and Thi-Sau Migone

Subjects

Cancer Research, Cell, Biology, Molecular biology, medicine.anatomical_structure, Oncology, Cell surface receptor, Cell culture, Fusion Toxin, medicine, Gelonin, B-cell activating factor, Receptor, B cell

Abstract

B lymphocyte stimulator (BLyS) is a member of the TNF superfamily of cytokines. BLyS is expressed by cells of myeloid origin and is one of many soluble factors that regulate human B-cell activation. The biological activity of BLyS is mediated by three cell surface receptors: B-cell-activating factor-receptor (BAFF-R/BR3), transmembrane activator and calcium modulator and cyclophilin ligand interactor (TACI) and B-cell maturation antigen (BCMA). These receptors are expressed by normal and malignant B-cells at various stages of development. To target malignant B cells expressing BLyS receptors, the recombinant plant-derived toxin gelonin was fused to the N-terminus of BLyS to generate the fusion toxin BLyS-gel. Gelonin is an N-glycosidase that removes a critical adenine from eukaryotic 28S rRNA, disrupting ribosome function and inhibiting protein synthesis. Importantly, gelonin is not toxic to cells unless coupled with a targeting moiety that can enter the cell. BLyS-gel was used to treat a panel of nearly 50 malignant non-Hodgkin lymphoma (NHL) cell lines expressing BLyS receptors. NHL subtypes mantle cell lymphoma (MCL), diffuse large B cell lymphoma (DLBCL) and B cell precursor-acute lymphocytic leukemia (BCP-ALL) were preferentially sensitive to BLyS-gel mediated cytotoxicity, with EC50 values in the low picomolar range. BLyS-gel cytotoxicity was mediated primarily by BR3 and TACI in sensitive cell lines; however, cell surface expression of these BLyS receptors did not necessarily confer sensitivity to BLyS-gel. The internalization of BLyS-gel was confirmed in both sensitive and resistant cell lines, indicating resistance was not due to a lack of internalization. As expected, BLyS-gel treatment inhibited protein synthesis in sensitive, but not resistant cell lines. In most cell lines, cell death seemed to be mediated by the “ribotoxic stress response.” This response involves activation of p38 MAPK and JNK/SAPK, and BLyS-gel mediated cytotoxicity was inhibited by the p38/JNK inhibitor SB203580. Finally, BLyS-gel treatment significantly prolonged survival in three distinct disseminated xenograft models (BCP-ALL, DLBCL & MCL) in SCID mice, and BLyS-gel was shown to specifically localize to sites of disease. Together, these findings suggest BLyS has potential as a targeting ligand for the therapeutic delivery of toxins and/or drugs directly to malignant B cells. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr 3861. doi:1538-7445.AM2012-3861

Published

2012

17. Phosphorylation at Ser-15 and Ser-392 in mutant p53 molecules from human tumors is altered compared to wild-type p53

Author

Stephen Ullrich, E Appella, W E Mercer, Carl W. Anderson, Michele Fiscella, Kazuyasu Sakaguchi, and Susan P. Lees-Miller

Subjects

Phosphopeptides, Multidisciplinary, Tumor suppressor gene, Cell growth, Mutant, Molecular Sequence Data, Wild type, Biology, Molecular biology, Transactivation, Transcription (biology), Neoplasms, Mutation, Serine, Tumor Cells, Cultured, Phosphorylation, Humans, Protein phosphorylation, Amino Acid Sequence, Tumor Suppressor Protein p53, Research Article

Abstract

The product of the p53 gene suppresses cell growth and plays a critical role in suppressing development of human tumors. p53 protein binds DNA, activates transcription, and can be phosphorylated at N- and C-terminal sites. Previously, wild-type p53 was shown to be hyperphosphorylated compared to mutant p53 during p53-mediated growth arrest in vivo. Here we show that Ser-15 and Ser-9 in the N-terminal transactivation domain of wild-type human p53 are phosphorylated in vivo in cells derived from the human glioblastoma line T98G. In [Ile237]p53 and [Ala143]p53, two natural p53 mutants from human tumors that are defective for activation of transcription, phosphorylation at Ser-15 was reduced and phosphorylation at Ser-392 was increased compared to wild-type p53. No change was observed at Ser-9. [His273]p53, a third mutant, had a phosphorylation state similar to that of wild-type p53. We suggest that phosphorylation of Ser-15 may depend on the ability of p53 to adopt a wild-type conformation and may contribute to p53's ability to block cell growth.

Published

1993

18. Cell cycle effects of microinjected antisense oligodeoxynucleotides to p34cdc2 kinase

Author

Hansjuerg Alder, W. Edward Mercer, Stephen Ullrich, D Lin, and Michelle T. Shields

Subjects

Time Factors, Microinjections, Molecular Sequence Data, Stimulation, Cycloheximide, General Biochemistry, Genetics and Molecular Biology, S Phase, chemistry.chemical_compound, History and Philosophy of Science, Sense (molecular biology), CDC2 Protein Kinase, Protein biosynthesis, Tumor Cells, Cultured, Humans, Microinjection, Cell Nucleus, Base Sequence, General Neuroscience, Cell Cycle, G1 Phase, Glioma, Cell cycle, Oligonucleotides, Antisense, Cell biology, Cell Compartmentation, chemistry, Oligodeoxyribonucleotides, Cytoplasm, Restriction point

Abstract

In this study the effect of antisense oligomers targeted against the mRNA transcripts of p34cdc2 kinase on G1 progression into S-phase was examined. For this purpose, antisense, sense, or nonsense oligomers were introduced directly into the cytoplasm of T98G cells grown in monolayer cultures by glass-capillary microinjection. The microinjection of antisense oligomers (but not sense or nonsense oligomers) into growth-arrested cells before serum stimulation inhibited G1 progression into S-phase. This inhibition was correlated with a reduction in the steady-state levels of nuclear p34cdc2 protein. Microinjection of antisense oligomers into cells at 2 and 6 hours after serum stimulation also resulted in a marked inhibition in the ability of cells to enter S-phase. The inhibitory effect decreased when cells were microinjected at 12 hours after serum stimulation. When cells were microinjected at 18 and 24 hours after serum stimulation, only a slight inhibition was observed. As the antisense oligomers were introduced directly into the cytoplasm of cells at each of the time points examined, the observed differences in the inhibitory effects of the antisense oligomers at later times after serum stimulation cannot be explained by differences in uptake. An alternative explanation is that after a certain threshold level of nuclear p34cdc2 protein is reached in late G1 phase; no further increase is necessary, because the cells become committed to enter S-phase. In yeast, p34cdc2 appears to play an important role in the G1/S-phase transition at a control point in late G1 phase called START (reviewed by Lewin). In mammalian cells a control point that could be equivalent to START is the "restriction point" which is defined as the time after which inhibition of protein synthesis fails to block entry into S-phase (reviewed by Pardee). The effects observed with antisense oligomers to p34cdc2 kinase are strikingly similar to what is observed when low concentrations of the drug cycloheximide are added to these cells at different times after serum stimulation; entry into S-phase is significantly inhibited when cycloheximide is added up to 12 hours postimulation. Thus, the results reported in this study are in agreement with the idea that p34cdc2 kinase plays a role in the G1/S phase transition in mammalian cells. Finally, introduction of antisense oligomers directly into the cytoplasm of cells grown in monolayer cultures by glass-capillary microinjection appears to be a viable alternative to simply adding the oligomers to the culture medium.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1992

19. Negative growth regulation in a glioblastoma tumor cell line that conditionally expresses human wild-type p53

Author

Amin M, G J Sauve, E Appella, M T Shields, J W Romano, W E Mercer, and Stephen Ullrich

Subjects

DNA Replication, Cell division, Biology, Transfection, Dexamethasone, Cell Line, Transcriptional regulation, Tumor Cells, Cultured, Humans, RNA, Messenger, RNA, Neoplasm, Oncogene Proteins, Multidisciplinary, Cell growth, Mouse mammary tumor virus, Cell Cycle, Wild type, Nuclear Proteins, Glioma, Cell cycle, biology.organism_classification, Blotting, Northern, Phosphoproteins, Molecular biology, Blotting, Southern, Cell culture, Tumor Suppressor Protein p53, Cell Division, Thymidine, Research Article

Abstract

To investigate the effect that human wild-type p53 (wt-p53) expression has on cell proliferation we constructed a recombinant plasmid, pM47, in which wt-p53 cDNA is under transcriptional control of the hormone-inducible mouse mammary tumor virus promoter linked to the dominant biochemical selection marker gene Eco gpt. The pM47 plasmid was introduced into T98G cells derived from a human glioblastoma multiforme tumor, and a stable clonal cell line, GM47.23, was derived that conditionally expressed wt-p53 following exposure to dexamethasone. We show that induction of wt-p53 expression in exponentially growing cells inhibits cell cycle progression and that the inhibitory effect is reversible upon removal of the inducer or infection with simian virus 40. Moreover, when growth-arrested cells are stimulated to proliferate, induction of wt-p53 expression inhibits G0/G1 progression into S phase and the cells accumulate with a DNA content equivalent to cells arrested in the G0/G1 phase of the cell cycle. Taken together, these studies suggest that wt-p53 may play a negative role in growth regulation.

Published

1990

20. A mouse tumor-specific transplantation antigen is a heat shock-related protein

Author

Mark C. Willingham, Lloyd W. Law, Ettore Appella, Stephen Ullrich, and Elizabeth A. Robinson

Subjects

Cytoplasm, Immunofluorescence, Mice, chemistry.chemical_compound, Antigen, Antigens, Neoplasm, Heat shock protein, medicine, Animals, Amino Acid Sequence, Isoelectric Point, Amino Acids, Peptide sequence, Heat-Shock Proteins, Multidisciplinary, medicine.diagnostic_test, biology, Cell Membrane, Neoplasms, Experimental, Meth, Molecular biology, Hsp90, Tumor antigen, Molecular Weight, Transplantation, Biochemistry, chemistry, Antigens, Surface, biology.protein, Research Article, Methylcholanthrene

Abstract

A tumor-specific transplantation antigen has been purified to homogeneity from the cytosol of a methylcholanthrene-induced tumor, Meth A. The purified antigen is highly immunogenic and specific against challenge with Meth A, providing greater than 95% inhibition of tumor growth in immunized syngeneic mice. Immunofluorescence analysis of Meth A showed that the antigen is a highly abundant cytosolic protein but that it is also present at the cell surface and, therefore, accessible to the host's immune system. The antigen consists of two polypeptide isoforms present in equimolar amounts, having similar masses (84 and 86 kDa), pI values (4.95 and 4.90), and amino acid compositions. Both are phosphoproteins, and neither is glycosylated. The NH2-terminal sequences of the two isoforms are identical except that each chain contains a portion of unique sequence. Comparison of the NH2-terminal and CNBr-fragment sequence data to the sequences of the yeast and Drosophila heat shock proteins (Hsp90 and Hsp83, respectively) reveals that 73 of 91 residues compared are identical. In addition, an anti-Meth A tumor antigen serum that defects the isoforms from a variety of tumors also immunoprecipitates proteins of identical mass and pI from both normal and heat-shocked mouse embryo cells.

Published

1986

21. Murine 86- and 84-kDa Heat Shock Proteins, cDNA Sequences, Chromosome Assignments, and Evolutionary Origins

Author

Stephen Ullrich, Christine A. Kozak, Elizabeth A. Robinson, Ettore Appella, and S K Moore

Subjects

Genetics, chemistry.chemical_classification, Untranslated region, Nucleic acid sequence, Cell Biology, Biology, Biochemistry, Homology (biology), Amino acid, chemistry, Heat shock protein, Complementary DNA, Coding region, Molecular Biology, Gene

Abstract

The two forms of the approximately 90-kDa murine heat shock protein, referred to as HSP86 and HSP84, are coded for by separate but related genes. A full-length nucleotide sequence of the cDNA coding for HSP86 from a chemically induced tumor, Meth A, was determined. Sequences from a number of peptides from HSP86 were found to be in complete agreement with the nucleotide sequence. The HSP84 sequence from the same tumor was also completed. HSP86 and HSP84 are acidic polypeptides 733 and 724 amino acids long with calculated molecular weights of 84,796 and 83,290, respectively. The two proteins are 86% homologous. HSP86 was found to contain internal peptide repeats of Glu-Lys-Glu within a region of highly charged amino acid residues. The coding regions of the cDNAs were 76% homologous; however, this homology did not extend to the 5'- and 3'-untranslated regions. The 5'-untranslated region of hsp86 cDNA was considerably longer than that of hsp84 cDNA and, unlike that of hsp84, contained extraneous ATG triplets. Hsp86-related sequences were assigned to chromosomes 12, 11, and 3. An evolutionary tree constructed from HSP90-related protein sequences indicated that HSP86 and HSP84 were likely to have diverged more than 500 million years ago. The findings presented herein suggest that HSP86 and HSP84 may have different functions.

Published

1989

22. Transcriptional and Translational Analysis of the Murine 84- and 86-kDa Heat Shock Proteins

Author

Stephen Ullrich, S K Moore, and Ettore Appella

Subjects

Messenger RNA, Cell culture, Transcription (biology), Complementary DNA, Heat shock protein, Protein biosynthesis, Cell Biology, Northern blot, Biology, Molecular Biology, Biochemistry, Molecular biology, In vitro

Abstract

The mammalian 85-90-kDa heat shock protein(s) (hsp) have been shown to exist as two species of 84 and 86 kDa (Ullrich, S. J., Robinson, E. A., Law, L. W., Willingham, M., and Appella, E. (1986) Proc. Natl. Acad. Sci. U. S. A. 83, 3121-3125). Two cDNA clones corresponding to the two forms have been isolated which specifically hybridize to either a 2.85- or a 3.0-kilobase pair transcript corresponding to hsp 84 and 86, respectively (Moore, S. K., Kozak, C., Robinson, E. A., Ullrich, S. J., and Appella, E. (1987) Gene (Amst.) 56, 29-40, and this paper). The regulation of these hsp were examined in nontransformed NIH-3T3 and chemically transformed Meth A cells. The basal level of the hsp 84 mRNA transcript was approximately 2.5-fold greater than the hsp 86 transcript, with a corresponding ratio of hsp 84 to hsp 86 protein synthesis of approximately 2.5:1. After a transient heat shock (10 min, 44 degrees C), the rate of transcription of hsp 84 and 86 increased approximately 4.5- and approximately 7-fold, respectively, within 0.5 h and remained elevated for approximately 2 h. Northern blot analysis performed on NIH-3T3 and Meth A cells, during recovery from a transient heat shock, indicated that in both cells mRNA levels of both hsp increased rapidly, peaking at 5 h post-heat shock; hsp 84 and 86 transcripts were 1.5- and 2-fold higher than in non-heat-shocked cells, respectively. The increased rate of hsp synthesis after heat shock correlated with the increased levels of each transcript in both cell lines. In the transformed Meth A cells the basal mRNA, hsp synthesis, and steady state levels of each hsp in vitro were 2-3-fold higher than in the nontransformed NIH-3T3 cells. In Meth A tumors in vivo, the steady state level of hsp 84 was reduced compared to in vitro levels. Thus, in normal and in transformed murine cells, both hsp are heat-inducible, transcriptionally and translationally, with the transformed cells expressing higher levels of synthesis of both hsp 84 and 86. The data suggest that hsp 84 and 86 syntheses are primarily transcriptionally regulated.

Published

1989

23. Cloning and nucleotide sequence of the murine hsp84 cDNA and chromosome assignment of related sequences

Author

Ettore Appella, Elizabeth A. Robinson, Christine A. Kozak, Stephen Ullrich, and Stephen K. Moore

Subjects

Polyadenylation, Molecular Sequence Data, Molecular cloning, Biology, Homology (biology), law.invention, Mice, law, Complementary DNA, Genetics, Coding region, Animals, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Gene, Heat-Shock Proteins, Base Sequence, Nucleic acid sequence, Chromosome Mapping, General Medicine, DNA, Molecular biology, Recombinant DNA, RNA, Poly A

Abstract

The nucleotide (nt) sequence of mouse 84-kDa heat shock protein (Hsp) cDNA has been determined using a combination of molecular cloning and oligodeoxynucleotide priming on poly(A) + RNA. The cDNA was 2.5 kb long, not including the poly(A) tail. It contained a 5′ leader of about 94 nt that was G + C-rich, and a 243-nt 3′-untranslated region that was A + T-rich in the vicinity of the polyadenylation signal. Gene hsp84 codes for an acidic polypeptide of 724 amino acid (aa) residues. Mouse Hsp84 had 81% and 63% aa homology to Drosophila melunogaster Hsp82 and yeast Hsp90, respectively. The nucleotide sequence had 74% and 59% homology to Drosophila and yeast hsp sequences, respectively, in the coding regions of these genes. This homology did not extend to the 5′- and 3′-untranslated regions. Chromosomal analysis indicated that hsp84 -related sequences are on at least three different chromosomes.

Published

1987

24. Regulatory effect of IFN-κ, a novel type I IFN, on cytokine production by cells of the innate immune system

Author

Paul A. Moore, Giampiero Girolomoni, Stephen Ullrich, David W. Lafleur, Bernardetta Nardelli, Mark Semenuk, Cristina Albanesi, Yun Hee Cho, Liubov Zaritskaya, and Devanshi Shah

Subjects

Adult, medicine.medical_treatment, Immunology, Biology, Monocytes, Interferon-gamma, Immune system, Adjuvants, Immunologic, medicine, Immunology and Allergy, Humans, Myeloid Cells, Cells, Cultured, Skin, Inflammation, Immunity, Cellular, Innate immune system, Heparin, Monocyte, CCL18, Dendritic cell, Blood Proteins, Dendritic Cells, Interleukin-12, Immunity, Innate, Lymphocyte Subsets, Cell biology, Cytokine, medicine.anatomical_structure, Interleukin 15, Interferon Type I, Cytokines, Cytokine secretion, Carrier Proteins, Antimicrobial Cationic Peptides, Protein Binding

Abstract

IFN-kappa is a recently identified type I IFN that exhibits both structural and functional homology with the other type I IFN subclasses. In this study, we have investigated the effect of IFN-kappa on cells of the innate immune system by comparing cytokine release following treatment of human cells with either IFN-kappa or two recombinant IFN subtypes, IFN-beta and IFN-alpha2a. Although IFN-alpha2a failed to stimulate monocyte cytokine secretion, IFN-kappa, like IFN-beta, induced the release of several cytokines from both monocytes and dendritic cells, without the requirement of a costimulatory signal. IFN-kappa was particularly effective in inhibiting inducible IL-12 release from monocytes. Unlike IFN-beta, IFN-kappa did not induce release of IFN-gamma by PBL. Expression of the IFN-kappa mRNA was observed in resting dendritic cells and monocytes, and it was up-regulated by IFN-gamma stimulation in monocytes, while IFN-beta mRNA was minimally detectable under the same conditions. Monocyte and dendritic cell expression of IFN-kappa was also confirmed in vivo in chronic lesions of psoriasis vulgaris and atopic dermatitis. Finally, biosensor-based binding kinetic analysis revealed that IFN-kappa, like IFN-beta, binds strongly to heparin (K(d): 2.1 nM), suggesting that the cytokine can be retained close to the local site of production. The pattern of cytokines induced by IFN-kappa in monocytes, coupled with the unique induction of IFN-kappa mRNA by IFN-gamma, indicates a potential role for IFN-kappa in the regulation of immune cell functions.