Your search keyword '"Jeffrey M. Riggs"' showing total 29 results

1. Pathogenic mechanisms of IgE-mediated inflammation in self-destructive autoimmune responses

Author

Rachel Ettinger, Jodi L. Karnell, Jill Henault, Santosh K. Panda, Jeffrey M. Riggs, Roland Kolbeck, and Miguel A. Sanjuan

Subjects

atopic dermatitis, autoimmunity, b cells, basophil, class switch recombination, chronic spontaneous urticaria, ige, interferon, pemphigus bullous, plasmacytoid dendritic cells, systemic lupus erythematosus, Internal medicine, RC31-1245

Abstract

Autoantibodies of the IgG subclass are pathogenic in a number of autoimmune disorders such as systemic lupus erythomatosus. The presence of circulating IgE autoantibodies in autoimmune patients has also been known for almost 40 years. Despite their role in allergies, IgE autoantibodies are not associated with a higher rate of atopy in these patients. However, recently they have been recognized as active drivers of autoimmunity through mechanisms involving the secretion of Type I interferons by plasmacytoid dendritic cells (pDC), the recruitment of basophils to lymph nodes, and the activation of adaptive immune responses through B and T cells. Here, we will review the formation, prevalence, affinity, and roles of the IgE autoantibodies that have been described in autoimmunity. We also present novel evidence supporting that triggering of IgE receptors in pDC induces LC3-associated phagocytosis, a cellular process also known as LAP that is associated with interferon responses. The activation of pDC with immune complexes formed by DNA-specific IgE antibodies also induce potent B-cell differentiation and plasma cell formation, which further define IgE’s role in autoimmune humoral responses.

Published

2017

2. Supplementary Table 1 from Immunomodulation of T- and NK-cell Responses by a Bispecific Antibody Targeting CD28 Homolog and PD-L1

Author

Gianluca Carlesso, Darren J. Schofield, Ronald Herbst, Geetha K. Bhat, Jeffrey M. Riggs, Yvonne Puplampu-Dove, Zenon Zenonos, Gareth Browne, Andrew Garcia, Tamer I. Mahmoud, Hormas Ghadially, Des C. Jones, Taeil Kim, and Madhu Ramaswamy

Abstract

Supplementary Table 1Suppl. Table 1 related to materials and methods

Published

2023

3. Supplementary Figures S1-S7 from Immunomodulation of T- and NK-cell Responses by a Bispecific Antibody Targeting CD28 Homolog and PD-L1

Author

Gianluca Carlesso, Darren J. Schofield, Ronald Herbst, Geetha K. Bhat, Jeffrey M. Riggs, Yvonne Puplampu-Dove, Zenon Zenonos, Gareth Browne, Andrew Garcia, Tamer I. Mahmoud, Hormas Ghadially, Des C. Jones, Taeil Kim, and Madhu Ramaswamy

Abstract

Supplementary Figures S1-S7Supplementary Figures S1-S7

Published

2023

4. Data from Immunomodulation of T- and NK-cell Responses by a Bispecific Antibody Targeting CD28 Homolog and PD-L1

Author

Gianluca Carlesso, Darren J. Schofield, Ronald Herbst, Geetha K. Bhat, Jeffrey M. Riggs, Yvonne Puplampu-Dove, Zenon Zenonos, Gareth Browne, Andrew Garcia, Tamer I. Mahmoud, Hormas Ghadially, Des C. Jones, Taeil Kim, and Madhu Ramaswamy

Abstract

Checkpoint blockade therapies targeting PD-1/PD-L1 and CTLA-4 are clinically successful but also evoke adverse events due to systemic T-cell activation. We engineered a bispecific, mAb targeting CD28 homolog (CD28H), a newly identified B7 family receptor that is constitutively expressed on T and natural killer (NK) cells, with a PD-L1 antibody to potentiate tumor-specific immune responses. The bispecific antibody led to T-cell costimulation, induced NK-cell cytotoxicity of PD-L1–expressing tumor cells, and activated tissue-resident memory CD8+ T cells. Mechanistically, the CD28H agonistic arm of the bispecific antibody reduced PD-L1/PD-1–induced SHP2 phosphorylation while simultaneously augmenting T-cell receptor signaling by activating the MAPK and AKT pathways. This bispecific approach could be used to target multiple immune cells, including CD8+ T cells, tissue-resident memory T cells, and NK cells, in a tumor-specific manner that may lead to induction of durable, therapeutic antitumor responses.

Published

2023

5. Immunomodulation of T- and NK-cell Responses by a Bispecific Antibody Targeting CD28 Homolog and PD-L1

Author

Madhu Ramaswamy, Taeil Kim, Des C. Jones, Hormas Ghadially, Tamer I. Mahmoud, Andrew Garcia, Gareth Browne, Zenon Zenonos, Yvonne Puplampu-Dove, Jeffrey M. Riggs, Geetha K. Bhat, Ronald Herbst, Darren J. Schofield, and Gianluca Carlesso

Subjects

Killer Cells, Natural, Cancer Research, CD28 Antigens, Cell Line, Tumor, Neoplasms, Immunology, Antibodies, Bispecific, Programmed Cell Death 1 Receptor, Humans, Immunotherapy, CD8-Positive T-Lymphocytes, Lymphocyte Activation, B7-H1 Antigen

Abstract

Checkpoint blockade therapies targeting PD-1/PD-L1 and CTLA-4 are clinically successful but also evoke adverse events due to systemic T-cell activation. We engineered a bispecific, mAb targeting CD28 homolog (CD28H), a newly identified B7 family receptor that is constitutively expressed on T and natural killer (NK) cells, with a PD-L1 antibody to potentiate tumor-specific immune responses. The bispecific antibody led to T-cell costimulation, induced NK-cell cytotoxicity of PD-L1–expressing tumor cells, and activated tissue-resident memory CD8+ T cells. Mechanistically, the CD28H agonistic arm of the bispecific antibody reduced PD-L1/PD-1–induced SHP2 phosphorylation while simultaneously augmenting T-cell receptor signaling by activating the MAPK and AKT pathways. This bispecific approach could be used to target multiple immune cells, including CD8+ T cells, tissue-resident memory T cells, and NK cells, in a tumor-specific manner that may lead to induction of durable, therapeutic antitumor responses.

Published

2021

6. Depleting plasmacytoid dendritic cells reduces local type I interferon responses and disease activity in patients with cutaneous lupus

Author

Jodi L. Karnell, Michael A Smith, William Rees, Victoria P. Werth, Jill Henault, Li Yan, Katherine Ann Vousden, Jeffrey M. Riggs, Miguel A. Sanjuan, Vib Trial Investigators, G. Illei, John N. Ratchford, Yanping Wu, Simone M. Nicholson, Kerry A. Casey, Nanette Mittereder, Michele Gunsior, and Jorn Drappa

Subjects

0301 basic medicine, Chemokine, Autoimmunity, medicine.disease_cause, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Immune system, Interferon, medicine, Lupus Erythematosus, Cutaneous, Humans, 030203 arthritis & rheumatology, Lupus erythematosus, biology, business.industry, hemic and immune systems, General Medicine, Dendritic Cells, medicine.disease, 030104 developmental biology, Immunology, Interferon Type I, biology.protein, Antibody, Chemokines, business, Interferon type I, medicine.drug

Abstract

Plasmacytoid dendritic cells (pDCs) not only are specialized in their capacity to secrete large amounts of type I interferon (IFN) but also serve to enable both innate and adaptive immune responses through expression of additional proinflammatory cytokines, chemokines, and costimulatory molecules. Persistent activation of pDCs has been demonstrated in a number of autoimmune diseases. To evaluate the potential benefit of depleting pDCs in autoimmunity, a monoclonal antibody targeting the pDC-specific marker immunoglobulin-like transcript 7 was generated. This antibody, known as VIB7734, which was engineered for enhanced effector function, mediated rapid and potent depletion of pDCs through antibody-dependent cellular cytotoxicity. In cynomolgus monkeys, treatment with VIB7734 reduced pDCs in blood below the lower limit of normal by day 1 after the first dose. In two phase 1 studies in patients with autoimmune diseases, VIB7734 demonstrated an acceptable safety profile, comparable to that of placebo. In individuals with cutaneous lupus, VIB7734 profoundly reduced both circulating and tissue-resident pDCs, with a 97.6% median reduction in skin pDCs at study day 85 in VIB7734-treated participants. Reductions in pDCs in the skin correlated with a decrease in local type I IFN activity as well as improvements in clinical disease activity. Biomarker analysis suggests that responsiveness to pDC depletion therapy may be greater among individuals with high baseline type I IFN activity, supporting a central role for pDCs in type I IFN production in autoimmunity and further development of VIB7734 in IFN-associated diseases.

Published

2020

7. SLE Plasma Profiling Identifies Unique Signatures of Lupus Nephritis and Discoid Lupus

Author

Dominic Sinibaldi, Ethan Grant, Rachel Ettinger, Melissa Parker, Michael A Smith, Kerry A. Casey, Michelle Petri, Devon K. Taylor, Miguel A. Sanjuan, Jodi L. Karnell, Jill Henault, Jeffrey M. Riggs, and Roland Kolbeck

Subjects

Adult, Male, 0301 basic medicine, Immunoglobulin A, Lupus nephritis, lcsh:Medicine, Inflammation, Disease, Kidney, Article, Cohort Studies, 03 medical and health sciences, Lupus Erythematosus, Discoid, Systemic lupus erythematosus, 0302 clinical medicine, immune system diseases, medicine, Humans, Lupus Erythematosus, Systemic, lcsh:Science, skin and connective tissue diseases, Autoantibodies, 030203 arthritis & rheumatology, Multidisciplinary, biology, business.industry, lcsh:R, Autoantibody, Diagnostic markers, Middle Aged, medicine.disease, Lupus Nephritis, Blood proteins, 030104 developmental biology, Immunology, biology.protein, lcsh:Q, Female, Antibody, medicine.symptom, business, Biomarkers

Abstract

Systemic lupus erythematosus (SLE) impacts multiple organ systems, although the causes of many individual SLE pathologies are poorly understood. This study was designed to elucidate organ-specific inflammation by identifying proteins that correlate with SLE organ involvement and to evaluate established biomarkers of disease activity across a diverse patient cohort. Plasma proteins and autoantibodies were measured across seven SLE manifestations. Comparative analyses between pathologies and correlation with the SLE Disease Activity Index (SLEDAI) were used to identify proteins associated with organ-specific and composite disease activity. Established biomarkers of composite disease activity, SLE-associated antibodies, type I interferon (IFN), and complement C3, correlated with composite SLEDAI, but did not significantly associate with many individual SLE pathologies. Two clusters of proteins were associated with renal disease in lupus nephritis samples. One cluster included markers of infiltrating leukocytes and the second cluster included markers of tissue remodelling. In patients with discoid lupus, a distinct signature consisting of elevated immunoglobulin A autoantibodies and interleukin-23 was observed. Our findings indicate that proteins from blood samples can be used to identify protein signatures that are distinct from established SLE biomarkers and SLEDAI and could be used to conveniently monitor multiple inflammatory pathways present in different organ systems.

Published

2019

8. Abstract 4438: A bispecific antibody targeting CD28H and PDL-1 is a novel and potent immunomodulator of T cell responses

Author

Desmond Jones, Tamer Mahmoud, Madhu Ramaswamy, Susan Wilson, Gianluca Carlesso, Jeffrey M. Riggs, Andrew Garcia, Hormas Ghadially, Darren J. Schofield, and Taeil Kim

Subjects

Cancer Research, education.field_of_study, biology, medicine.drug_class, CD3, medicine.medical_treatment, T cell, Innate lymphoid cell, Population, Immunotherapy, Monoclonal antibody, Cytokine, medicine.anatomical_structure, Oncology, biology.protein, medicine, Cancer research, education, CD8

Abstract

The success of immune checkpoint inhibitors CTLA4 and PD-1 monoclonal antibody, both FDA approved cancer therapies, specifically counteracts inhibitory pathways to activate antigen-specific T cells. However, their success is limited by the fact that not all patients respond to immunotherapy and a variety of adverse events due to non specific and systemic T cell activation limits their administration. A newly identified B7 family receptor, CD28H/TMIGD2, is constitutively expressed on T, pDCs and innate lymphoid cells including NK and ILCs. CD28H is also detected in TILs including the CD8+ tissue resident memory T cells (TRM), a T cell subset that correlates with better prognosis and response to immune checkpoint inhibitor therapy. Functionally, CD28H provides costimulatory function to T cells in the context of TCR signaling events during activation. We engineered a bispecific antibody (Bis mAb) targeting CD28H and PDL1 aimed to augment T cell costimulation and NK activation. The CD28H-PDL1 Bis mAb potentiates T cell proliferative and cytokine responses in antigen-specific human T cell assays and induces human NK -mediated redirected killing of PDL1+ tumor cells. In T cells, the mechanism of action of the Bis mAb requires intracellular signaling domain of the CD28H which downmodulates SHP phosphorylation upon CD3 activation. Intriguingly, we found that the Bis mAb increases induction of CD8 TRM cells in vitro. In human TILs, where CD28H is mostly expressed on CD8 TRM in tumors, the Bis mAb enables higher cytokine responses over PDL1 mAb alone. Given the recent relevance of TRM cells as an important pool of anti-tumor T cell immunity, the rationale for targeting this population via CD28H in the context of blocking PDL1 may prove to be a therapeutic tool for enhancing responses to checkpoint inhibitor therapy. Citation Format: Madhu Ramaswamy, Taeil Kim, Desmond Jones, Hormas Ghadially, Tamer Mahmoud, Andrew Garcia, Susan Wilson, Jeffrey Riggs, Darren Schofield, GIanluca Carlesso. A bispecific antibody targeting CD28H and PDL-1 is a novel and potent immunomodulator of T cell responses [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 4438.

Published

2020

9. Pathogenic mechanisms of IgE-mediated inflammation in self-destructive autoimmune responses

Author

Jill Henault, Roland Kolbeck, Santosh K. Panda, Jeffrey M. Riggs, Rachel Ettinger, Jodi L. Karnell, and Miguel A. Sanjuan

Subjects

0301 basic medicine, T-Lymphocytes, Immunology, Inflammation, Autoimmunity, Basophil, Immunoglobulin E, medicine.disease_cause, Lymphocyte Activation, Autoimmune Diseases, Atopy, 03 medical and health sciences, 0302 clinical medicine, Immune system, Interferon, medicine, Immunology and Allergy, Animals, Humans, Gene Rearrangement, B-Lymphocyte, Autoantibodies, B-Lymphocytes, biology, business.industry, Autoantibody, hemic and immune systems, medicine.disease, Immunoglobulin Class Switching, 030104 developmental biology, medicine.anatomical_structure, Antibody Formation, biology.protein, Disease Susceptibility, medicine.symptom, business, 030215 immunology, medicine.drug

Abstract

Autoantibodies of the IgG subclass are pathogenic in a number of autoimmune disorders such as systemic lupus erythomatosus. The presence of circulating IgE autoantibodies in autoimmune patients has also been known for almost 40 years. Despite their role in allergies, IgE autoantibodies are not associated with a higher rate of atopy in these patients. However, recently they have been recognized as active drivers of autoimmunity through mechanisms involving the secretion of Type I interferons by plasmacytoid dendritic cells (pDC), the recruitment of basophils to lymph nodes, and the activation of adaptive immune responses through B and T cells. Here, we will review the formation, prevalence, affinity, and roles of the IgE autoantibodies that have been described in autoimmunity. We also present novel evidence supporting that triggering of IgE receptors in pDC induces LC3-associated phagocytosis, a cellular process also known as LAP that is associated with interferon responses. The activation of pDC with immune complexes formed by DNA-specific IgE antibodies also induce potent B-cell differentiation and plasma cell formation, which further define IgE's role in autoimmune humoral responses.

Published

2017

10. Early, transient depletion of plasmacytoid dendritic cells ameliorates autoimmunity in a lupus model

Author

William Vermi, Miguel A. Sanjuan, Sarah L. Rowland, Jeffrey M. Riggs, Susan Gilfillan, Emil R. Unanue, Roland Kolbeck, Marco Colonna, and Mattia Bugatti

Subjects

0303 health sciences, Lupus erythematosus, Systemic lupus erythematosus, Immunology, Alpha interferon, hemic and immune systems, Glomerulonephritis, Biology, medicine.disease_cause, medicine.disease, 3. Good health, Autoimmunity, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, biology.protein, Immunology and Allergy, Antibody, 030304 developmental biology, 030215 immunology

Abstract

Plasmacytoid dendritic cells (pDCs) have long been implicated in the pathogenesis of lupus. However, this conclusion has been largely based on a correlative link between the copious production of IFN-α/β by pDCs and the IFN-α/β “signature” often seen in human lupus patients. The specific contribution of pDCs to disease in vivo has not been investigated in detail. For this reason, we generated a strain of BXSB lupus-prone mice in which pDCs can be selectively depleted in vivo. Early, transient ablation of pDCs before disease initiation resulted in reduced splenomegaly and lymphadenopathy, impaired expansion and activation of T and B cells, reduced antibodies against nuclear autoantigens and improved kidney pathology. Amelioration of pathology coincided with decreased transcription of IFN-α/β–induced genes in tissues. PDC depletion had an immediate impact on the activation of immune cells, and importantly, the beneficial effects on pathology were sustained even though pDCs later recovered, indicating an early pDC contribution to disease. Together, our findings demonstrate a critical function for pDCs during the IFN-α/β–dependent initiation of autoimmune lupus and point to pDCs as an attractive therapeutic target for the treatment of SLE.

Published

2014

11. Characterisation of anifrolumab, a fully human anti-interferon receptor antagonist antibody for the treatment of systemic lupus erythematosus

Author

Erika Farmer, Kamelia Zerrouki, Inna Vainshtein, Meina Liang, Jeffrey M. Riggs, Bhargavi Rajan, Chris Morehouse, Kevin Schifferli, Kimberly Rosenthal, Richard N. Hanna, Divya Sagar, Melissa de los Reyes, Roland Kolbeck, Miguel A. Sanjuan, Gary P. Sims, and Jodi L. Karnell

Subjects

0301 basic medicine, Immunology, Plasmacytoid dendritic cell, Proinflammatory cytokine, Flow cytometry, 03 medical and health sciences, systemic lupus erythematosus, Interferon, Plasma cell differentiation, Clinical Trials and Drug Discovery, Medicine, STAT1, B cell, Antibody-dependent cell-mediated cytotoxicity, treatment, biology, medicine.diagnostic_test, business.industry, dmards (biologic), interferon, General Medicine, cytokines, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Cancer research, business, medicine.drug

Abstract

Objective We investigated the mechanistic and pharmacological properties of anifrolumab, a fully human, effector-null, anti-type I interferon (IFN) alpha receptor 1 (IFNAR1) monoclonal antibody in development for SLE. Methods IFNAR1 surface expression and internalisation on human monocytes before and after exposure to anifrolumab were assessed using confocal microscopy and flow cytometry. The effects of anifrolumab on type I IFN pathway activation were assessed using signal transducer and activator of transcription 1 (STAT1) phosphorylation, IFN-stimulated response element–luciferase reporter cell assays and type I IFN gene signature induction. The ability of anifrolumab to inhibit plasmacytoid dendritic cell (pDC) function and plasma cell differentiation was assessed by flow cytometry and ELISA. Effector-null properties of anifrolumab were assessed in antibody-dependent cell-mediated cytotoxicity (ADCC) and complement-dependent cytotoxicity (CDC) assays with B cells. Results Anifrolumab reduced cell surface IFNAR1 by eliciting IFNAR1 internalisation. Anifrolumab blocked type I IFN-dependent STAT1 phosphorylation and IFN-dependent signalling induced by recombinant and pDC-derived type I IFNs and serum of patients with SLE . Anifrolumab suppressed type I IFN production by blocking the type I IFN autoamplification loop and inhibited proinflammatory cytokine induction and the upregulation of costimulatory molecules on stimulated pDCs. Blockade of IFNAR1 suppressed plasma cell differentiation in pDC/B cell co-cultures. Anifrolumab did not exhibit CDC or ADCC activity. Conclusions Anifrolumab potently inhibits type I IFN-dependent signalling, including the type I IFN autoamplification loop, and is a promising therapeutic for patients with SLE and other diseases that exhibit chronic dysfunctional type I IFN signalling.

Published

2018

12. Self-reactive IgE exacerbates interferon responses associated with autoimmunity

Author

Ronald Herbst, Tomas Mustelin, Marcus R. Clark, Lorraine Clarke, Deepak B. Khatry, Liat Izhak, Jill Henault, Kerry A. Casey, Michelle Petri, Rachel Ettinger, Lena Shirinian, Roland Kolbeck, Vladimir M. Liarski, Jodi L. Karnell, Linda Xu, Jeffrey M. Riggs, Miguel A. Sanjuan, Michael A Smith, and Jianqing Li

Subjects

0301 basic medicine, Male, Immunology, Plasma Cells, Inflammation, Autoimmunity, Antigen-Antibody Complex, Immunoglobulin E, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, Immune system, Phagocytosis, Phagosomes, medicine, Immunology and Allergy, Humans, Lupus Erythematosus, Systemic, Autoantibodies, B-Lymphocytes, Lupus erythematosus, biology, TLR9, Dendritic Cells, medicine.disease, Lupus Nephritis, Research Highlight, 3. Good health, 030104 developmental biology, chemistry, Antibodies, Antinuclear, Immunoglobulin G, Toll-Like Receptor 9, biology.protein, Leukocytes, Mononuclear, Cytokines, Female, Interferons, Antibody, medicine.symptom, Histamine

Abstract

Canonically, immunoglobulin E (IgE) mediates allergic immune responses by triggering mast cells and basophils to release histamine and type 2 helper cytokines. Here we found that in human systemic lupus erythematosus (SLE), IgE antibodies specific for double-stranded DNA (dsDNA) activated plasmacytoid dendritic cells (pDCs), a type of cell of the immune system linked to viral defense, which led to the secretion of substantial amounts of interferon-α (IFN-α). The concentration of dsDNA-specific IgE found in patient serum correlated with disease severity and greatly potentiated pDC function by triggering phagocytosis via the high-affinity FcɛRI receptor for IgE, followed by Toll-like receptor 9 (TLR9)-mediated sensing of DNA in phagosomes. Our findings expand the known pathogenic mechanisms of IgE-mediated inflammation beyond those found in allergy and demonstrate that IgE can trigger interferon responses capable of exacerbating self-destructive autoimmune responses.

Published

2015

13. Determinants of the Host Range Restriction of Replication of Bovine Parainfluenza Virus Type 3 in Rhesus Monkeys Are Polygenic

Author

Peter L. Collins, William R. Elkins, Mario H. Skiadopoulos, Alexander Schmidt, Brian R. Murphy, Jeffrey M. Riggs, Marisa St. Claire, and Sonja R. Surman

Subjects

DNA, Complementary, Immunology, Biology, Virus Replication, Microbiology, Cell Line, law.invention, Open Reading Frames, law, Virology, Vaccines and Antiviral Agents, Animals, Humans, ORFS, Gene, Pathogen, Parainfluenza Virus 3, Bovine, Chimera, Point mutation, Temperature, Macaca mulatta, Parainfluenza Virus 3, Human, Open reading frame, Viral replication, Insect Science, Recombinant DNA, biology.protein, Antibody

Abstract

The Kansas strain of bovine parainfluenza virus type 3 (BPIV3) is 100- to 1,000-fold restricted in replication in the respiratory tracts of nonhuman primates compared to human PIV3 (HPIV3), an important pathogen of infants and young children. BPIV3 is also restricted in replication in human infants and children, yet it is immunogenic and is currently being evaluated in clinical trials as a vaccine candidate to protect against illness caused by HPIV3. We have examined the genetic basis for the host range attenuation phenotype of BPIV3 by exchanging each open reading frame (ORF) of a recombinant wild-type HPIV3 with the analogous ORF from BPIV3, with the caveats that the multiple ORFs of the P gene were exchanged as a single unit and that the HN and F genes were exchanged as a single unit. Recombinant chimeric bovine-human PIV3s were recovered from cDNA, and the levels of viral replication in vitro and in the respiratory tract of rhesus monkeys were determined. Recombinant chimeric HPIV3s bearing the BPIV3 N or P ORF were highly attenuated in the upper and lower respiratory tracts of monkeys, whereas those bearing the BPIV3 M or L ORF or the F and HN genes were only moderately attenuated. This indicates that the genetic determinants of the host range restriction of replication of BPIV3 for primates are polygenic, with the major determinants being the N and P ORFs. Monkeys immunized with these bovine-human chimeric viruses, including the more highly attenuated ones, developed higher levels of HPIV3 hemagglutination-inhibiting serum antibodies than did monkeys immunized with BPIV3 and were protected from challenge with wild-type HPIV3. Furthermore, host range determinants could be combined with attenuating point mutations to achieve an increased level of attenuation. Thus, chimeric recombinant bovine-human PIV3 viruses that manifest different levels of attenuation in rhesus monkeys are available for evaluation as vaccine candidates to protect infants from the severe lower respiratory tract disease caused by HPIV3.

Published

2003

14. Sendai Virus, a Murine Parainfluenza Virus Type 1, Replicates to a Level Similar to Human PIV1 in the Upper and Lower Respiratory Tract of African Green Monkeys and Chimpanzees

Author

Daniel Kolakofsky, Mario H. Skiadopoulos, Peter L. Collins, Brian R. Murphy, Marisa St. Claire, Machiko Nishio, William R. Elkins, Jeffrey M. Riggs, Sonja R. Surman, and Dominique Garcin

Subjects

Pan troglodytes, Respiratory System, Parainfluenza Virus 1, Human/immunology/physiology, Respirovirus Infections/immunology/prevention & control, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Respirovirus Infections, Sendai virus, Sendai virus/immunology/physiology, Species Specificity, Neutralization Tests, Virology, Chlorocebus aethiops, medicine, Animals, Antibodies, Viral/analysis, Vector (molecular biology), Viral Vaccines/administration & dosage, ddc:616, biology, Transmission (medicine), Pan troglodytes/virology, Viral Vaccines, biology.organism_classification, Parainfluenza Virus 1, Human, Disease Models, Animal, Human Parainfluenza Virus, medicine.anatomical_structure, Respiratory System/virology, Viral replication, Immunology, Viral disease, African Green Monkey, Cercopithecus aethiops/virology, Respiratory tract

Abstract

Human parainfluenza virus type 1 (HPIV1), a major cause of croup in infants and young children, accounts for 6% of hospitalizations for pediatric respiratory tract disease. The antigenically related Sendai virus, referred to here as murine PIV1 (MPIV1), is being considered for use as a live-attenuated vaccine to protect against HPIV1 (J. L. Hurwitz, K. F. Soike, M. Y., Sangster, A. Portner, R. E. Sealy, D. H. Dawson, and C. Coleclough, 1997, Vaccine 15(5), 533–540) and also as a recombinant vaccine vector expressing antigens to protect against viral disease in humans. However, in the 1950s MPIV1 was reported to have been isolated from humans, suggesting that zoonotic transmission might have occurred. It is therefore important to examine the ability of MPIV1 to replicate in nonhuman primates, i.e., surrogate hosts for humans. In the present study the level of replication of MPIV1 and HPIV1 was compared in African green monkeys and chimpanzees. Surprisingly, MPIV1 replicated as efficiently as HPIV1 in the upper and lower respiratory tract of African green monkeys at doses of 104 and 106 and replicated only slightly less efficiently at both sites in chimpanzees. African green monkeys immunized with MPIV1 were highly resistant to subsequent challenge with HPIV1 even though MPIV1 did not induce a detectable HPIV1-neutralizing antibody response. The high level of replication of MPIV1 observed in the upper and lower respiratory tract of these primates suggests that MPIV1 likely would require significant attenuation before it could be given to humans as a vaccine against HPIV1 or as a vaccine vector. Its ability to efficiently replicate in nonhuman primates suggests that MPIV1 lacks a significant host range restriction in primates and could theoretically cause zoonotic disease in humans.

Published

2002

15. Evaluation of the Replication and Immunogenicity of Recombinant Human Parainfluenza Virus Type 3 Vectors Expressing up to Three Foreign Glycoproteins

Author

Claes Örvell, Sonja R. Surman, Brian R. Murphy, Jeffrey M. Riggs, Mario H. Skiadopoulos, and Peter L. Collins

Subjects

Genetic Vectors, Gene Expression, Hemagglutinins, Viral, Hemagglutinin (influenza), Antibodies, Viral, Virus Replication, Insert (molecular biology), Virus, Cell Line, law.invention, Measles virus, Neutralization Tests, law, Cricetinae, Virology, Animals, Gene, HN Protein, biology, Viral Vaccines, Hemagglutination Tests, biology.organism_classification, Fusion protein, Parainfluenza Virus 3, Human, Viral replication, Drug Design, Recombinant DNA, biology.protein, Reassortant Viruses

Abstract

The level of replication and immunogenicity of recombinant parainfluenza virus type 3 (rHPIV3) bearing one, two, or three gene insertions expressing foreign protective antigens was examined. cDNA-derived recombinant HPIV3s bearing genes encoding the open reading frames (ORFs) of the hemagglutinin-neuraminidase (HN) of HPIV1, the HN of HPIV2, or the hemagglutinin (HA) of measles virus replicated efficiently in vitro, including the largest recombinant, which had three gene unit insertions and which was almost 23 kb in length, 50% longer than unmodified HPIV3. Several viruses were recovered from cDNAs whose genome length was not a multiple of six nucleotides and these contained nucleotide insertions that corrected the length to be a multiple of 6, confirming that the “rule of six” applies to HPIV3. Using a hemagglutination inhibition assay, we determined that the HPIV1 HN expressed by recombinant HPIV3 was incorporated into HPIV3 virions, whereas using this assay incorporation of the HPIV2 HN could not be detected. HPIV3 virions bearing HPIV1 HN were not neutralized by HPIV1 antiserum but were readily neutralized by antibodies to the HPIV3 HN or fusion protein (F). Viruses with inserts were restricted for replication in the respiratory tract of hamsters, and the level of restriction was a function of the total number of genes inserted, the nature of the insert, and the position of the inserted gene in the gene order. A single insert of HPIV2 HN or measles virus HA reduced the in vivo replication of rHPIV3 up to 25-fold, whereas the HPIV1 HN insert decreased replication almost 1000-fold. This indicates that the HPIV1 HN insert has an attenuating effect in addition to that of the extra gene insert itself, presumably because it is incorporated into the virus particle. Viruses containing two inserts were generally more attenuated than those with a single insert, and viruses with three inserts were over-attenuated for replication in hamsters. Inserts between the N and P genes were slightly more attenuating than those between the P and the M genes. A recombinant HPIV3 bearing both the HPIV1 and the HPIV2 HN genes (r1HN 2HN) was attenuated, immunogenic, and protected immunized hamsters from challenge with HPIV1, HPIV2, and HPIV3. Thus, it is possible to use a single HPIV vector expressing two foreign gene inserts to protect infants and young children from the severe lower respiratory tract disease caused by the three major human PIV pathogens.

Published

2002

16. [Untitled]

Author

Mario H. Skiadopoulos, Jason T. Newman, Peter L. Collins, Brian R. Murphy, Sonja R. Surman, Chris T. Hansen, and Jeffrey M. Riggs

Subjects

biology, Sequence analysis, Virulence, General Medicine, biology.organism_classification, Virology, Sendai virus, Virus, Reverse genetics, Plasmid, Complementary DNA, Genetics, Consensus sequence, Molecular Biology

Abstract

A complete consensus sequence was determined for the genomic RNA of human parainfluenza virus type 1 (HPIV1) strain Washington/20993/1964 (HPIV1 WASH/64), a clinical isolate that previously was shown to be virulent in adults. The sequence exhibited a high degree of relatedness to both Sendai virus, a PIV1 virus recovered from mice, and human PIV3 (HPIV3) with regard to cis-acting regulatory regions and protein-coding sequences. This consensus sequence was used to generate a full-length antigenomic cDNA and to recover a recombinant wild-type HPIV1 (rHPIV1). Interestingly, the rHPIV1 could be rescued from full-length antigenomic rHPIV1 cDNA using HPIV3 support plasmids, HPIV1 support plasmids, or a mixture thereof. The replication of rHPIV1 in vitro and in the respiratory tract of hamsters was similar to that of its biologically derived parent virus. The similar biological properties of rHPIV1 and HPIV1 WASH/64 in vitro and in vivo, together with the previous demonstration of the virulence of this specific isolate in humans, authenticates the rHPIV1 sequence as that of a wild-type virus. This rHPIV1 can now be used to study the biological properties of HPIV1 and as a substrate to introduce attenuating mutations for the generation of live-attenuated HPIV1 vaccine candidates.

Published

2002

17. A Chimeric Human-Bovine Parainfluenza Virus Type 3 Expressing Measles Virus Hemagglutinin Is Attenuated for Replication but Is Still Immunogenic in Rhesus Monkeys

Author

Brian R. Murphy, Peter L. Collins, Jeffrey M. Riggs, Sonja R. Surman, and Mario H. Skiadopoulos

Subjects

viruses, Measles Vaccine, Respiratory System, Immunology, Hemagglutinins, Viral, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Recombinant virus, Microbiology, Measles, Respirovirus, Virus, Measles virus, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Neutralizing antibody, Vaccines, Synthetic, biology, Chimera, Viral culture, biology.organism_classification, medicine.disease, Macaca mulatta, Parainfluenza Virus 3, Human, Insect Science, Respiratory Syncytial Virus Vaccines, biology.protein, Cattle, Immunization, Measles vaccine

Abstract

The chimeric recombinant virus rHPIV3-N B , a version of human parainfluenza virus type 3 (HPIV3) that is attenuated due to the presence of the bovine PIV3 nucleocapsid (N) protein open reading frame (ORF) in place of the HPIV3 ORF, was modified to encode the measles virus hemagglutinin (HA) inserted as an additional, supernumerary gene between the HPIV3 P and M genes. This recombinant, designated rHPIV3-N B HA, replicated like its attenuated rHPIV3-N B parent virus in vitro and in the upper and lower respiratory tracts of rhesus monkeys, indicating that the insertion of the measles virus HA did not further attenuate rHPIV3-N B in vitro or in vivo. Monkeys immunized with rHPIV3-N B HA developed a vigorous immune response to both measles virus and HPIV3, with serum antibody titers to both measles virus (neutralizing antibody) and HPIV3 (hemagglutination inhibiting antibody) of over 1:500. An attenuated HPIV3 expressing a major protective antigen of measles virus provides a method for immunization against measles by the intranasal route, a route that has been shown with HPIV3 and respiratory syncytial virus vaccines to be relatively refractory to the neutralizing and immunosuppressive effects of maternally derived virus-specific serum antibodies. It should now be possible to induce a protective immune response against measles virus in 6-month-old infants, an age group that in developing areas of the world is not responsive to the current measles virus vaccine.

Published

2001

18. Human Parainfluenza Virus Type 3 (PIV3) Expressing the Hemagglutinin Protein of Measles Virus Provides a Potential Method for Immunization against Measles Virus and PIV3 in Early Infancy

Author

Jeffrey M. Riggs, Mario H. Skiadopoulos, Peter L. Collins, Brian R. Murphy, Josephine M. McAuliffe, Anna P. Durbin, and Sonja R. Surman

Subjects

viruses, Measles Vaccine, Molecular Sequence Data, Immunology, Hemagglutinins, Viral, Antibodies, Viral, Virus Replication, Microbiology, Measles, Virus, law.invention, Measles virus, law, Cricetinae, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Cells, Cultured, Vaccines, Synthetic, Base Sequence, Mesocricetus, biology, Vaccination, Temperature, Infant, biology.organism_classification, medicine.disease, Parainfluenza Virus 3, Human, Human Parainfluenza Virus, Titer, Insect Science, Recombinant DNA, biology.protein, Antibody

Abstract

Recombinant human parainfluenza virus type 3 (PIV3) was used as a vector to express the major protective antigen of measles virus, the hemagglutinin (HA) glycoprotein, in order to create a bivalent PIV3-measles virus that can be administered intranasally. The measles virus HA open reading frame (ORF) was inserted as an additional transcriptional unit into the N-P, P-M, or HA-neuraminidase (HN)-L gene junction of wild-type PIV3 or into the N-P or P-M gene junction of an attenuated derivative of PIV3, termed r cp 45L. The recombinant PIV3 (rPIV3) viruses bearing the HA inserts replicated more slowly in vitro than their parental viruses but reached comparable peak titers of ≥10 7.5 50% tissue culture infective doses per ml. Each of the wild-type or cold-passaged 45L ( cp 45L) PIV3(HA) chimeric viruses replicated 5- to 10-fold less well than its respective parent virus in the upper respiratory tract of hamsters. Thus, insertion of the ∼2-kb ORF itself conferred attenuation, and this attenuation was additive to that conferred by the cp 45L mutations. The attenuated cp 45L PIV3(HA) recombinants induced a high level of resistance to replication of PIV3 challenge virus in hamsters and induced very high levels of measles virus neutralizing antibodies (>1:8,000) that are well in excess of those known to be protective in humans. rPIV3s expressing the HA gene in the N-P or P-M junction induced about 400-fold more measles virus-neutralizing antibody than did the rPIV3 with the HA gene in the HN-L junction, indicating that the N-P or P-M junction appears to be the preferred insertion site. Previous studies indicated that the PIV3 cp 45 virus, a more attenuated version of r cp 45L, replicates efficiently in the respiratory tract of monkeys and is immunogenic and protective even when administered in the presence of very high titers of passively transferred PIV3 antibodies (A. P. Durbin, C. J. Cho, W. R. Elkins, L. S. Wyatt, B. Moss, and B. R. Murphy, J. Infect. Dis. 179:1345–1351, 1999). This suggests that this intranasally administered PIV3(HA) chimeric virus can be used to immunize infants with maternally acquired measles virus antibodies in whom the current parenterally administered live measles virus vaccine is ineffective.

Published

2000

19. Replacement of the Ectodomains of the Hemagglutinin-Neuraminidase and Fusion Glycoproteins of Recombinant Parainfluenza Virus Type 3 (PIV3) with Their Counterparts from PIV2 Yields Attenuated PIV2 Vaccine Candidates

Author

Fatemeh Davoodi, Tao Tao, Mario H. Skiadopoulos, Brian R. Murphy, Jeffrey M. Riggs, and Peter L. Collins

Subjects

Pan troglodytes, Molecular Sequence Data, Respiratory System, Immunology, Biology, Vaccines, Attenuated, Virus Replication, Microbiology, Cell Line, law.invention, Parainfluenza virus type 2, law, Cricetinae, Virology, Chlorocebus aethiops, Vaccines and Antiviral Agents, Animals, Amino Acid Sequence, HN Protein, Vero Cells, Recombination, Genetic, Vaccines, Synthetic, Base Sequence, Mesocricetus, Viral Vaccine, Vaccination, Viral Vaccines, Parainfluenza Virus 2, Human, Parainfluenza Virus 3, Human, Protein Structure, Tertiary, Transmembrane domain, Viral replication, Ectodomain, Insect Science, Mutagenesis, Site-Directed, Recombinant DNA, Viral Fusion Proteins, Hemagglutinin-neuraminidase

Abstract

We sought to develop a live attenuated parainfluenza virus type 2 (PIV2) vaccine strain for use in infants and young children, using reverse genetic techniques that previously were used to rapidly produce a live attenuated PIV1 vaccine candidate. The PIV1 vaccine candidate, designated rPIV3-1cp45, was generated by substituting the full-length HN and F proteins of PIV1 for those of PIV3 in the attenuated cp 45 PIV3 vaccine candidate (T. Tao et al., J. Virol. 72:2955–2961, 1998; M. H. Skiadopoulos et al., Vaccine 18:503–510, 1999). However, using the same strategy, we failed to recover recombinant chimeric PIV3-PIV2 isolate carrying the full-length PIV2 glycoproteins in a wild-type PIV3 backbone. Viable PIV3-PIV2 chimeras were recovered when chimeric HN and F open reading frames (ORFs) rather than complete PIV2 F and HN ORFs were used to construct the full-length cDNA. The recovered viruses, designated rPIV3-2CT, in which the PIV2 ectodomain and transmembrane domain were fused to the PIV3 cytoplasmic domain, and rPIV3-2TM, in which the PIV2 ectodomain was fused to the PIV3 transmembrane and cytoplasmic tail domain, possessed similar in vitro and in vivo phenotypes. Thus, it appeared that only the cytoplasmic tail of the HN or F glycoprotein of PIV3 was required for successful recovery of PIV3-PIV2 chimeras. Although rPIV3-2CT and rPIV3-2TM replicated efficiently in vitro, they were moderately to highly attenuated for replication in the respiratory tracts of hamsters, African green monkeys (AGMs), and chimpanzees. This unexpected finding indicated that chimerization of the HN and F proteins of PIV2 and PIV3 itself specified an attenuation phenotype in vivo. Despite this attenuation, these viruses were highly immunogenic and protective against challenge with wild-type PIV2 in hamsters and AGMs, and they represent promising candidates for clinical evaluation as a vaccine against PIV2. These chimeric viruses were further attenuated by the addition of 12 mutations of PIV3cp45 which lie outside of the HN and F genes. The attenuating effects of these mutations were additive with that of the chimerization, and thus inclusion of all or some of the cp 45 mutations provides a means to further attenuate the PIV3-PIV2 chimeric vaccine candidates if necessary.

Published

2000

20. Biased VH Gene Usage in Early Lineage Human B Cells: Evidence for Preferential Ig Gene Rearrangement in the Absence of Selection

Author

Sambasiva P. Rao, Jeffrey M. Riggs, David F. Friedman, Michael S. Scully, Tucker W. LeBien, and Leslie E. Silberstein

Subjects

Immunology, Immunology and Allergy

Abstract

Certain VH genes are predominantly expressed in mature B cells. We hypothesized that several, mutually nonexclusive VH-dependent mechanisms operating at distinct stages during B cell development may be responsible for overrepresentation of these VH genes. In the present study, we have assessed whether one of the mechanisms involves preferential rearrangement at the pro-B cell stage. The frequency of individual VH4 and VH3 genes in rearrangement libraries from FACS-purified human CD34+/CD19+ pro-B and CD34−/CD19+ pre-B cells was assessed. The in-frame and out-of-frame rearrangements from both cell populations were analyzed using a high resolution PAGE system. The frequencies of individual VH gene segments among out-of-frame rearrangements from pro-B cells were determined, because these frequencies should reflect only processes before the translation of the μ-heavy chain and should not be biased by selection mechanisms. Our results demonstrate that, at the pro-B cell stage, the V4–34, V4–39, and V4–59 gene segments are the most frequently rearranged VH4 family genes, and the V3–23 and V3–30 gene segments are the most frequently rearranged VH3 family genes. This finding suggests that the predominant expression of these VH genes in peripheral mature B cells is determined to a significant degree by their preferential rearrangement during V-DJ recombination.

Published

1999

21. Pharmacological inhibition of type I interferon signaling protects mice against lethal sepsis

Author

Sofie Vandevyver, Ling-Ling An, Jeffrey M. Riggs, Lien Dejager, Marlies Ballegeer, Claude Libert, Roland Kolbeck, and Elien Van Wonterghem

Subjects

Male, Chemokine, Neutrophils, Peritonitis, Bacteremia, Kaplan-Meier Estimate, Receptor, Interferon alpha-beta, medicine.disease_cause, Sepsis, Mice, Interferon, Gene expression, medicine, Immunology and Allergy, Animals, Humans, Secretion, Receptor, Cecum, Mice, Knockout, Analysis of Variance, biology, Pseudomonas aeruginosa, Antibodies, Monoclonal, medicine.disease, Endotoxemia, Mice, Inbred C57BL, Infectious Diseases, Immunology, Interferon Type I, biology.protein, Female, medicine.drug, Signal Transduction

Abstract

Current research on new therapeutic strategies for sepsis uses different animal models, such as the lipopolysaccharide-induced endotoxemia model and the cecal ligation and puncture (CLP) peritonitis model. By using genetic and pharmacologic inhibition of the type I interferon (IFN) receptor (IFNAR1), we show that type I IFN signaling plays a detrimental role in these sepsis models. Mortality after CLP was reduced even when type I IFN responses were blocked after the onset of sepsis. Our findings reveal that type I IFNs play an important detrimental role during sepsis by negatively regulating neutrophil recruitment. Reduced neutrophil influx likely occurs via the induction of the CXC motif chemokine 1. Moreover, human white blood cells exposed to heat-killed Pseudomonas aeruginosa secrete IFN-β and stimulate type I IFN signaling. We provide data that support pharmacologic inhibition of type I IFN signaling as a novel therapeutic treatment in severe sepsis.

Published

2013

22. AB0146 Self-Reactive IGE Exacerbates Interferon Responses Associated with Autoimmunity

Author

Jeffrey M. Riggs, Kerry A. Casey, Ronald Herbst, Linda Xu, Michael A Smith, Jill Henault, Jodi L. Karnell, Roland Kolbeck, Rachel Ettinger, Lena Shirinian, Miguel A. Sanjuan, M. Petri, Marcus R. Clark, Deepak B. Khatry, Tomas Mustelin, Lorraine Clarke, and Vladimir M. Liarski

Subjects

0301 basic medicine, Immunology, Inflammation, medicine.disease_cause, Immunoglobulin E, General Biochemistry, Genetics and Molecular Biology, Autoimmunity, Immune tolerance, 03 medical and health sciences, chemistry.chemical_compound, Immune system, Rheumatology, Interferon, medicine, Immunology and Allergy, biology, business.industry, Autoantibody, 030104 developmental biology, chemistry, biology.protein, medicine.symptom, business, Histamine, medicine.drug

Abstract

Background The discovery of Immunoglobulin E (IgE) nearly 40 years ago was a breakthrough in the field of allergy research. IgE directed against parasitic worms and allergens binds mast cells and basophils, triggering an inflammatory response that is characterized by the release of histamine and Th2 cytokines. Here we report that double-stranded DNA (dsDNA)-specific IgE autoantibodies complexed to DNA activate plasmacytoid dendritic cells (pDC), an immune cell type linked to viral defense, leading to the secretion of substantial amounts of IFN-a. Although typical IgE mediated responses are not a hallmark of systemic lupus erythematosus (SLE), IFN-a producing pDCs are a key driver for loss of immune tolerance to host DNA in SLE. We, therefore, investigated this apparent paradox and found that even the small concentrations of circulating dsDNA-specific IgE found in SLE patients greatly potentiated pDC secretion of IFN-a by triggering phagocytosis via the Fc-epsilon receptor I (FceRI) and TLR9-mediated DNA sensing in the phagolysosome. Consequently, this potent pDC signaling mechanism reduces the threshold of pDC activation, which has the potential to expand anti-DNA responses and greatly exacerbate self-inflicted damage. These findings expand the known pathogenic mechanisms of IgE mediated inflammation beyond those found in allergies and demonstrate that, in addition to recognizing exogenous allergens, IgE can also bind to autoantigens and drive an aberrant and self-destructive anti-viral response. This previously unrecognized link between IgE and the interferon pathway provides additional insights into the pathological mechanisms underlying autoimmunity and may be useful in the rational design of therapies for the treatment of diseases such as SLE. Disclosure of Interest M. Sanjuan Employee of: Medimmune, J. Henault Employee of: Medimmune, J. Riggs Employee of: Medimmune, J. Karnell Employee of: Medimmune, V. Liarski: None declared, L. Shirinian Employee of: Medimmune, L. Xu Employee of: Medimmune, K. Casey Employee of: Medimmune, M. Smith Employee of: Medimmune, D. Khatry Employee of: Medimmune, L. Clarke Employee of: Medimmune, R. Herbst Employee of: Medimmune, R. Ettinger Employee of: Medimmune, M. Petri: None declared, M. Clark: None declared, T. Mustelin Employee of: Medimmune, R. Kolbeck Employee of: Medimmune

Published

2016

23. Noncanonical autophagy is required for type I interferon secretion in response to DNA-immune complexes

Author

Jane Tian, Douglas R. Green, Jennifer Martinez, Miguel A. Sanjuan, Payal Mehta, Jill Henault, Jeffrey M. Riggs, Akiko Iwasaki, Eicke Latz, Lorraine Clarke, Melanie M. Brinkmann, Anthony J. Coyle, Roland Kolbeck, Miwa Sasai, and Respiratory, Inflammation and Autoimmunity Research Department, MedImmune, Gaithersburg, MD 20878, USA.

Subjects

Immunology, Inflammation, Antigen-Antibody Complex, Biology, Mice, Immune system, Phagocytosis, Interferon, Phagosomes, medicine, Autophagy, Immunology and Allergy, Animals, Humans, Secretion, Mice, Knockout, TLR9, Membrane Transport Proteins, DNA, Cell biology, Protein Transport, Infectious Diseases, Type I interferon secretion, Immunoglobulin G, Toll-Like Receptor 9, Transcription preinitiation complex, Interferon Type I, medicine.symptom, Microtubule-Associated Proteins, medicine.drug

Abstract

SummaryToll-like receptor-9 (TLR9) is largely responsible for discriminating self from pathogenic DNA. However, association of host DNA with autoantibodies activates TLR9, inducing the pathogenic secretion of type I interferons (IFNs) from plasmacytoid dendritic cells (pDCs). Here, we found that in response to DNA-containing immune complexes (DNA-IC), but not to soluble ligands, IFN-α production depended upon the convergence of the phagocytic and autophagic pathways, a process called microtubule-associated protein 1A/1B-light chain 3 (LC3)-associated phagocytosis (LAP). LAP was required for TLR9 trafficking into a specialized interferon signaling compartment by a mechanism that involved autophagy-related proteins, but not the conventional autophagic preinitiation complex, or adaptor protein-3 (AP-3). Our findings unveil a new role for nonconventional autophagy in inflammation and provide one mechanism by which anti-DNA autoantibodies, such as those found in several autoimmune disorders, bypass the controls that normally restrict the apportionment of pathogenic DNA and TLR9 to the interferon signaling compartment.

Published

2012

24. The two major human metapneumovirus genetic lineages are highly related antigenically, and the fusion (F) protein is a major contributor to this antigenic relatedness

Author

Josephine M. McAuliffe, Stéphane Biacchesi, Brian R. Murphy, William R. Elkins, Ursula J. Buchholz, Mario H. Skiadopoulos, Peter L. Collins, Marisa St. Claire, Jeffrey M. Riggs, Sonja R. Surman, and Emerito Amaro-Carambot

Subjects

Pan troglodytes, viruses, Immunology, Molecular Sequence Data, Respiratory System, Heterologous, Cross Reactions, Antibodies, Viral, Virus Replication, Microbiology, Neutralization, Virus, Epitope, Cell Line, Human metapneumovirus, Neutralization Tests, Virology, Cricetinae, Antigenic variation, Animals, Humans, Metapneumovirus, Paramyxoviridae Infections, biology, Base Sequence, virus diseases, biology.organism_classification, Antigenic Variation, respiratory tract diseases, Parainfluenza Virus 1, Human, Disease Models, Animal, Insect Science, biology.protein, Pathogenesis and Immunity, Antibody, Viral Fusion Proteins

Abstract

The growth properties and antigenic relatedness of the CAN98-75 (CAN75) and the CAN97-83 (CAN83) human metapneumovirus (HMPV) strains, which represent the two distinct HMPV genetic lineages and exhibit 5 and 63% amino acid divergence in the fusion (F) and attachment (G) proteins, respectively, were investigated in vitro and in rodents and nonhuman primates. Both strains replicated to high titers (≥6.0 log 10 ) in the upper respiratory tract of hamsters and to moderate titers (≥3.6 log 10 ) in the lower respiratory tract. The two lineages exhibited 48% antigenic relatedness based on reciprocal cross-neutralization assay with postinfection hamster sera, and infection with each strain provided a high level of resistance to reinfection with the homologous or heterologous strain. Hamsters immunized with a recombinant human parainfluenza virus type 1 expressing the fusion F protein of the CAN83 strain developed a serum antibody response that efficiently neutralized virus from both lineages and were protected from challenge with either HMPV strain. This result indicates that the HMPV F protein is a major antigenic determinant that mediates extensive cross-lineage neutralization and protection. Both HMPV strains replicated to low titers in the upper and lower respiratory tracts of rhesus macaques but induced high levels of HMPV-neutralizing antibodies in serum effective against both lineages. The level of HMPV replication in chimpanzees was moderately higher, and infected animals developed mild colds. HMPV replicated the most efficiently in the respiratory tracts of African green monkeys, and the infected animals developed a high level of HMPV serum-neutralizing antibodies (1:500 to 1:1,000) effective against both lineages. Reciprocal cross-neutralization assays in which postinfection sera from all three primate species were used indicated that CAN75 and CAN83 are 64 to 99% related antigenically. HMPV-infected chimpanzees and African green monkeys were highly protected from challenge with the heterologous HMPV strain. Taken together, the results from hamsters and nonhuman primates support the conclusion that the two HMPV genetic lineages are highly related antigenically and are not distinct antigenic subtypes or subgroups as defined by reciprocal cross-neutralization in vitro.

Published

2004

25. Codon Substitution Mutations at Two Positions in the L Polymerase Protein of Human Parainfluenza Virus Type 1 Yield Viruses with a Spectrum of Attenuation In Vivo and Increased Phenotypic Stability In Vitro

Author

Brian R. Murphy, Sonja R. Surman, Peter L. Collins, Jason T. Newman, Mario H. Skiadopoulos, Josephine M. McAuliffe, and Jeffrey M. Riggs

Subjects

Silent mutation, Immunology, Mutant, Respiratory System, DNA-Directed DNA Polymerase, medicine.disease_cause, Vaccines, Attenuated, Virus Replication, Microbiology, Respirovirus Infections, Cell Line, Viral Proteins, Serial passage, Virology, Cricetinae, Vaccines and Antiviral Agents, medicine, Missense mutation, Animals, Humans, Codon, Parainfluenza Vaccines, Polymerase, Genetics, Mutation, biology, Temperature, Molecular biology, Parainfluenza Virus 1, Human, Phenotype, Amino Acid Substitution, Insect Science, Codon usage bias, biology.protein, Synonymous substitution

Abstract

The Y942H and L992F temperature-sensitive ( ts ) and attenuating amino acid substitution mutations, previously identified in the L polymerase of the HPIV3 cp 45 vaccine candidate, were introduced into homologous positions of the L polymerase of recombinant human parainfluenza virus type 1 (rHPIV1). In rHPIV1, the Y942H mutation specified the ts phenotype in vitro and the attenuation ( att ) phenotype in hamsters, whereas the L992F mutation specified neither phenotype. Each of these codon mutations was generated by a single nucleotide substitution and therefore had the potential to readily revert to a codon specifying the wild-type amino acid residue. We introduced alternative amino acid assignments at codon 942 or 992 as a strategy to increase genetic stability and to generate mutants that exhibit a range of attenuation. Twenty-three recombinants with codon substitutions at position 942 or 992 of the L protein were viable. One highly ts and att mutant, the Y942A virus, which had a difference of three nucleotides from the codon encoding a wild-type tyrosine, also possessed a high level of genetic and phenotypic stability upon serial passage in vitro at restrictive temperatures compared to that of the parent Y942H virus, which possessed a single nucleotide substitution. We obtained mutants with substitutions at position 992 that, in contrast to the L992F virus, possessed the ts and att phenotypes. These findings identify the use of alternative codon substitution mutations as a method that can be used to generate candidate vaccine viruses with increased genetic stability and/or a modified level of attenuation.

Published

2004

26. Generation of recombinant human parainfluenza virus type 1 vaccine candidates by importation of temperature-sensitive and attenuating mutations from heterologous paramyxoviruses

Author

Jason T. Newman, Sonja R. Surman, Mario H. Skiadopoulos, Jeffrey M. Riggs, Teresa A. Mulaikal, Josephine M. McAuliffe, Peter L. Collins, and Brian R. Murphy

Subjects

Paramyxoviridae, Immunology, Mutant, Molecular Sequence Data, Heterologous, Biology, Recombinant virus, medicine.disease_cause, Antibodies, Viral, Vaccines, Attenuated, Microbiology, Respirovirus Infections, Virus, Viral Proteins, Virology, Cricetinae, Vaccines and Antiviral Agents, medicine, Animals, Humans, Point Mutation, Mononegavirales, Parainfluenza Vaccines, Mutation, Vaccines, Synthetic, Base Sequence, Mesocricetus, Point mutation, Temperature, biology.organism_classification, Parainfluenza Virus 1, Human, Parainfluenza Virus 3, Human, Respiratory Syncytial Viruses, Insect Science

Abstract

Human parainfluenza virus type 1 (HPIV1) is a significant cause of respiratory tract disease in infants and young children for which a vaccine is needed. In the present study, we sought to attenuate HPIV1 by the importation of one or more known attenuating point mutations from heterologous paramyxoviruses into homologous sites in HPIV1. The introduced mutations were derived from three attenuated paramyxoviruses: (i) HPIV3 cp 45, a live-attenuated HPIV3 vaccine candidate containing multiple attenuating mutations; (ii) the respiratory syncytial virus cpts 530 with an attenuating mutation in the L polymerase protein; and (iii) a murine PIV1 (MPIV1) attenuated by a mutation in the accessory C protein. Recombinant HPIV1 (rHPIV1) mutants bearing a single imported mutation in C, any of three different mutations in L, or a pair of mutations in F exhibited a 100-fold or greater reduction in replication in the upper or lower respiratory tract of hamsters. Both temperature-sensitive ( ts ) (mutations in the L and F proteins) and non- ts (the mutation in the C protein) attenuating mutations were identified. rHPIV1 mutants containing a combination of mutations in L were generated that were more attenuated than viruses bearing the individual mutations, showing that the systematic accretion of mutations can yield progressive increases in attenuation. Hamsters immunized with rHPIV1 mutants bearing one or two mutations developed neutralizing antibodies and were resistant to challenge with wild-type HPIV1. Thus, importation of attenuating mutations from heterologous viruses is an effective means for rapidly identifying mutations that attenuate HPIV1 and for generating live-attenuated HPIV1 vaccine candidates.

Published

2004

27. The Genome Length of Human Parainfluenza Virus Type 2 Follows the Rule of Six, and Recombinant Viruses Recovered from Non-Polyhexameric-Length Antigenomic cDNAs Contain a Biased Distribution of Correcting Mutations

Author

Sonja R. Surman, Mario H. Skiadopoulos, Brian R. Murphy, Jeffrey M. Riggs, Leatrice Vogel, and Peter L. Collins

Subjects

Paramyxoviridae, Immunology, Molecular Sequence Data, Replication, Context (language use), Genome, Viral, Biology, Microbiology, Genome, law.invention, Intergenic region, law, Virology, Complementary DNA, Chlorocebus aethiops, Animals, Amino Acid Sequence, Gene, Vero Cells, Genetics, Recombination, Genetic, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, biology.organism_classification, Parainfluenza Virus 2, Human, Viral replication, Insect Science, Mutation, Recombinant DNA

Abstract

Members of the Paramyxovirinae subfamily of the Paramyxoviridae family of viruses have the unusual requirement that the nucleotide length of the viral genome must be an even multiple of six in order for efficient RNA replication, and hence virus replication, to occur. Human parainfluenza virus type 2 (HPIV2) is the only member of the genus that has been reported to have a genome length that is not an even multiple of six, and it has also been recovered from a full-length antigenomic-sense cDNA that did not conform to the “rule of six.” To reexamine the issue of nucleotide length in natural isolates of HPIV2, a complete consensus genomic sequence was determined for three HPIV2 strains: Greer, Vanderbilt/1994 (V94), and Vanderbilt/1998. Each of these strains was found to have a genome length of 15,654 nucleotides (nt), thus conforming in each case to the rule of six. To directly examine the requirement that the genomic length of HPIV2 be an even multiple of six, we constructed six full-length antigenomic HPIV2/V94 cDNAs that deviated from a polyhexameric length by 0 to 5 nt. Recombinant HPIV2s were readily recovered from all of the cDNAs, including those that did not conform to the rule of six. One recombinant HPIV2 isolate was completely sequenced for each of the nonpolyhexameric antigenomic cDNAs. These were found to contain small nucleotide insertions or deletions that conferred polyhexameric length to the recovered genome. Interestingly, almost all of the length corrections occurred within the hemagglutinin-neuraminidase and large polymerase genes or the intervening intergenic region and thus were proximal to the insert that caused the deviation from the rule of six. These results demonstrate, in the context of complete infectious virus, that HPIV2 has a strong and seemingly absolute requirement for a polyhexameric genome.

Published

2003

28. Sequence analysis of the Washington/1964 strain of human parainfluenza virus type 1 (HPIV1) and recovery and characterization of wild-type recombinant HPIV1 produced by reverse genetics

Author

Jason T, Newman, Sonja R, Surman, Jeffrey M, Riggs, Chris T, Hansen, Peter L, Collins, Brian R, Murphy, and Mario H, Skiadopoulos

Subjects

Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, Molecular Sequence Data, Paramyxoviridae, Humans, Genome, Viral, Sequence Alignment, Sequence Analysis, Cell Line, Parainfluenza Virus 1, Human, Plasmids

Abstract

A complete consensus sequence was determined for the genomic RNA of human parainfluenza virus type 1 (HPIV1) strain Washington/20993/1964 (HPIV1 WASH/64), a clinical isolate that previously was shown to be virulent in adults. The sequence exhibited a high degree of relatedness to both Sendai virus, a PIV1 virus recovered from mice, and human PIV3 (HPIV3) with regard to cis-acting regulatory regions and protein-coding sequences. This consensus sequence was used to generate a full-length antigenomic cDNA and to recover a recombinant wild-type HPIV1 (rHPIV1). Interestingly, the rHPIV1 could be rescued from full-length antigenomic rHPIV1 cDNA using HPIV3 support plasmids, HPIV1 support plasmids, or a mixture thereof. The replication of rHPIV1 in vitro and in the respiratory tract of hamsters was similar to that of its biologically derived parent virus. The similar biological properties of rHPIV1 and HPIV1 WASH/64 in vitro and in vivo, together with the previous demonstration of the virulence of this specific isolate in humans, authenticates the rHPIV1 sequence as that of a wild-type virus. This rHPIV1 can now be used to study the biological properties of HPIV1 and as a substrate to introduce attenuating mutations for the generation of live-attenuated HPIV1 vaccine candidates.

Published

2002

29. 81 Mechanism of action of Sifnalimumab, a human IFN-α neutralizing monoclonal antibody

Author

Claudia R. Morris, Meina Liang, Inna Vainshtein, Jeffrey M. Riggs, Anthony J. Coyle, Vaheh Oganesyan, L. Roskos, W DallAcqua, Ricardo Cibotti, and Peter A. Kiener

Subjects

Mechanism of action, medicine.drug_class, Chemistry, Immunology, medicine, Immunology and Allergy, Hematology, medicine.symptom, Monoclonal antibody, Molecular Biology, Biochemistry, Molecular biology

Published

2008