Your search keyword '"José Herrera Rodriguez"' showing total 5 results

1. Adjuvantation of Pulmonary-Administered Influenza Vaccine with GPI-0100 Primarily Stimulates Antibody Production and Memory B Cell Proliferation

Author

Harshad P. Patil, José Herrera Rodriguez, Jacqueline de Vries-Idema, Tjarko Meijerhof, Henderik W. Frijlink, Wouter L. J. Hinrichs, and Anke Huckriede

Subjects

influenza, pulmonary immunization, adjuvant, immune mechanisms, Medicine

Abstract

Adjuvants are key components in vaccines, they help in reducing the required antigen dose but also modulate the phenotype of the induced immune response. We previously showed that GPI-0100, a saponin-derived adjuvant, enhances antigen-specific mucosal and systemic antibody responses to influenza subunit and whole inactivated influenza virus (WIV) vaccine administered via the pulmonary route. However, the impact of the GPI-0100 dose on immune stimulation and the immune mechanisms stimulated by GPI-0100 along with antigen are poorly understood. Therefore, in this study we immunized C57BL/6 mice via the pulmonary route with vaccine consisting of WIV combined with increasing amounts of GPI-0100, formulated as a dry powder. Adjuvantation of WIV enhanced influenza-specific mucosal and systemic immune responses, with intermediate doses of 5 and 7.5 μg GPI-0100 being most effective. The predominant antibody subtype induced by GPI-0100-adjuvanted vaccine was IgG1. Compared to non-adjuvanted vaccine, GPI-0100-adjuvanted WIV vaccine gave rise to higher numbers of antigen-specific IgA- but not IgG-producing B cells in the lungs along with better mucosal and systemic memory B cell responses. The GPI-0100 dose was negatively correlated with the number of influenza-specific IFNγ- and IL17-producing T cells and positively correlated with the number of IL4-producing T cells observed after immunization and challenge. Overall, our results show that adjuvantation of pulmonary-delivered WIV with GPI-0100 mostly affects B cell responses and effectively induces B cell memory.

Published

2017

2. Inactivated or damaged? Comparing the effect of inactivation methods on influenza virions to optimize vaccine production

Author

Marijke Holtrop, Anke Huckriede, Aurora Signorazzi, José Herrera-Rodriguez, Jacqueline de Vries-Idema, and Transplantation Immunology Groningen

Subjects

Hemagglutination, viruses, BPL, β-propiolactone, Hemagglutinin Glycoproteins, Influenza Virus, Inactivation, 0302 clinical medicine, 030212 general & internal medicine, Receptor, Infectivity, biology, Chemistry, NA, neuraminidase, 3. Good health, Titer, HAU, hemagglutination units, Infectious Diseases, β-propiolactone, Formaldehyde, Vaccine, Influenza, Inactivation, Influenza A virus, Influenza Vaccines, FA, formaldehyde, Molecular Medicine, TLR, Toll-like receptor, WIV, whole inactivated virus, 030231 tropical medicine, Hemagglutinin (influenza), Virus, Article, TCID50, tissue culture infectious dose (50% thereof), WHO, World Health Organization, Incubation period, Cell Line, 03 medical and health sciences, Formaldehyde, Animals, Humans, General Veterinary, General Immunology and Microbiology, Public Health, Environmental and Occupational Health, Virion, β-propiolactone, Virology, Influenza, Vaccines, Inactivated, Cell culture, biology.protein, RBCs, red blood cells, RNA, ribonucleic acid, Virus Inactivation, ssRNA, single strand RNA, Vaccine, HA, hemagglutinin

Abstract

Highlights • β-propiolactone (BPL) and formaldehyde (FA) were used to inactivate several influenza virus strains. • BPL abolished the infectivity, FA was unable to completely inactivate the virus. • All methods damaged the binding and fusion capacity; BPL caused greater loss than FA. • FA treatments caused the highest reduction in TLR-7 stimulation. • All the observed effects were strain-dependent., The vast majority of commercially available inactivated influenza vaccines are produced from egg-grown or cell-grown live influenza virus. The first step in the production process is virus inactivation with β-propiolactone (BPL) or formaldehyde (FA). Recommendations for production of inactivated vaccines merely define the maximal concentration for both reagents, leaving the optimization of the process to the manufacturers. We assessed the effect of inactivation with BPL and FA on 5 different influenza virus strains. The properties of the viral formulation, such as successful inactivation, preservation of hemagglutinin (HA) binding ability, fusion capacity and the potential to stimulate a Toll-like receptor 7 (TLR7) reporter cell line were then assessed and compared to the properties of the untreated virus. Inactivation with BPL resulted in undetectable infectivity levels, while FA-treated virus retained very low infectious titers. Hemagglutination and fusion ability were highly affected by those treatments that conferred higher inactivation, with BPL-treated virus binding and fusing at a lower degree compared to FA-inactivated samples. On the other hand, BPL-inactivated virus induced higher levels of activation of TLR7 than FA-inactivated virus. The alterations caused by BPL or FA treatments were virus strain dependent. This data shows that the inactivation procedures should be tailored on the virus strain, and that many other elements beside the concentration of the inactivating agent, such as incubation time and temperature, buffer and virus concentration, have to be defined to achieve a functional product.

Published

2019

3. A novel peptide-based vaccine candidate with protective efficacy against influenza A in a mouse model

Author

Maja A. Sommerfelt, Birger Sørensen, Tjarko Meijerhof, José Herrera-Rodriguez, Anke Huckriede, Mats Ökvist, Arnt-Ove Hovden, Hubert G. M. Niesters, Grete Stjernholm, Microbes in Health and Disease (MHD), and Translational Immunology Groningen (TRIGR)

Subjects

0301 basic medicine, Influenza vaccine, Epitopes, T-Lymphocyte, Hemagglutinin (influenza), Mice, Transgenic, Human leukocyte antigen, Cell mediated immunity, IMMUNITY, Biology, Epitope, Mice, Random Allocation, 03 medical and health sciences, Immune system, T-CELL EPITOPES, Immunity, Virology, HLA-A2 Antigen, Influenza, Human, Animals, Humans, Immunity, Cellular, Influenza, Immunity, Humoral, Mice, Inbred C57BL, Disease Models, Animal, Humoral immunity, Universal vaccine, 030104 developmental biology, Influenza A virus, Influenza Vaccines, SAFETY, biology.protein, VIRUS, Female, Immunization, TRIAL, Antibody, Peptides, RESPONSES

Abstract

Current influenza vaccines mainly induce antibody responses to the variable hemagglutinin proteins of the virus strains included in the vaccine. Instead, a broadly protective influenza vaccine should aim at inducing antibody and/or cell -mediated immunity against conserved viral proteins. Vacc-FLU is a peptide based vaccine combining conserved B and T cell epitopes. Peptide selection was done using a proprietary peptide design platform technology focusing on responses to human leukocyte antigen (HLA)-restricted epitopes. Immunization of wild -type mice and mice transgenic for HLA-A2.1 with the peptide mix successfully induced both humoral and cell mediated immune responses. Partial protection from severe weight loss upon challenge was observed in both mouse strains but was stronger and observed at lower vaccine doses in transgenic mice. Our results show that the Vacc-FLU peptide mix is capable of inducing IFNy-producing T cells and antibody-producing B cells which can protect from severe disease symptoms upon infection.

Published

2018

4. Adjuvantation of Pulmonary-Administered Influenza Vaccine with GPI-0100 Primarily Stimulates Antibody Production and Memory B Cell Proliferation

Author

José Herrera Rodriguez, Jacqueline de Vries-Idema, Harshad P. Patil, Anke Huckriede, Henderik W. Frijlink, Wouter L. J. Hinrichs, Tjarko Meijerhof, Pharmaceutical Technology and Biopharmacy, Biopharmaceuticals, Discovery, Design and Delivery (BDDD), Nanotechnology and Biophysics in Medicine (NANOBIOMED), Microbes in Health and Disease (MHD), and Translational Immunology Groningen (TRIGR)

Subjects

0301 basic medicine, Influenza vaccine, medicine.medical_treatment, Immunology, lcsh:Medicine, Biology, RESPIRATORY-TRACT, Article, 03 medical and health sciences, DELIVERY, 0302 clinical medicine, Immune system, Antigen, adjuvant, Drug Discovery, INFECTION, medicine, Journal Article, Pharmacology (medical), Memory B cell, pulmonary immunization, B cell, Pharmacology, influenza, immune mechanisms, IMMUNE-RESPONSES, lcsh:R, PERSISTENCE, Virology, PATHOLOGY, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, DIFFERENTIATION, Immunization, biology.protein, INNATE IMMUNITY, VIRUS, Antibody, CHALLENGE, Adjuvant, 030215 immunology

Abstract

Adjuvants are key components in vaccines, they help in reducing the required antigen dose but also modulate the phenotype of the induced immune response. We previously showed that GPI-0100, a saponin-derived adjuvant, enhances antigen-specific mucosal and systemic antibody responses to influenza subunit and whole inactivated influenza virus (WIV) vaccine administered via the pulmonary route. However, the impact of the GPI-0100 dose on immune stimulation and the immune mechanisms stimulated by GPI-0100 along with antigen are poorly understood. Therefore, in this study we immunized C57BL/6 mice via the pulmonary route with vaccine consisting of WIV combined with increasing amounts of GPI-0100, formulated as a dry powder. Adjuvantation of WIV enhanced influenza-specific mucosal and systemic immune responses, with intermediate doses of 5 and 7.5 μg GPI-0100 being most effective. The predominant antibody subtype induced by GPI-0100-adjuvanted vaccine was IgG1. Compared to non-adjuvanted vaccine, GPI-0100-adjuvanted WIV vaccine gave rise to higher numbers of antigen-specific IgA- but not IgG-producing B cells in the lungs along with better mucosal and systemic memory B cell responses. The GPI-0100 dose was negatively correlated with the number of influenza-specific IFNγ- and IL17-producing T cells and positively correlated with the number of IL4-producing T cells observed after immunization and challenge. Overall, our results show that adjuvantation of pulmonary-delivered WIV with GPI-0100 mostly affects B cell responses and effectively induces B cell memory.

Published

2017

5. Dengue tropism for macrophages and dendritic cells: the host cell effect

Author

Mayra Diosa-Toro, Jacky Flipse, Silvio Urcuqui-Inchima, Izabela A. Rodenhuis-Zybert, Jolanda M. Smit, Silvia Torres Pedraza, José Herrera-Rodriguez, Heidi van der Ende-Metselaar, Anke Huckriede, Microbes in Health and Disease (MHD), and Translational Immunology Groningen (TRIGR)

Subjects

0301 basic medicine, TISSUES, viruses, 030106 microbiology, CLEC5A, VIRUS-INFECTION, Dengue virus, Biology, Virus Replication, medicine.disease_cause, Virus, DISEASE, Microbiology, Dengue fever, Dengue, 03 medical and health sciences, Immune system, Virology, medicine, Humans, PARTICLES, Antibody-dependent enhancement, Cells, Cultured, Tropism, ANTIBODY-DEPENDENT ENHANCEMENT, Infectivity, Macrophages, Dendritic Cells, Dengue Virus, medicine.disease, 030104 developmental biology, ENTRY, Tissue tropism, TARGET-CELLS

Abstract

Dengue virus infects immune cells, including monocytes, macrophages and dendritic cells (DC). We compared virus infectivity in macrophages and DC, and found that the virus origin determined the cell tropism of progeny virus. The highest efficiency of re-infection was seen for macrophage-derived dengue virus. Furthermore, in the presence of enhancing antibodies, macrophage-derived virus gave greater enhancement of infection compared with immature DC derived virus. Taken together, our results highlight the importance of macrophages in dengue infection.

Published

2016