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1. Interplay of diverse adjuvants and nanoparticle presentation of native-like HIV-1 envelope trimers

Author

Sliepen, K., Schermer, E., Bontjer, I., Burger, J.A., Lévai, R.F., Mundsperger, P., Brouwer, P.J.M., Tolazzi, M., Farsang, A., Katinger, D., Moore, J.P., Scarlatti, G., Shattock, R.J., Sattentau, Q.J., and Sanders, R.W.

Abstract

The immunogenicity of HIV-1 envelope (Env) trimers is generally poor. We used the clinically relevant ConM SOSIP trimer to compare the ability of different adjuvants (squalene emulsion, ISCOMATRIX, GLA-LSQ, and MPLA liposomes) to support neutralizing antibody (NAb) responses in rabbits. The trimers were administered as free proteins or on nanoparticles. The rank order for the adjuvants was ISCOMATRIX > SE > GLA-LSQ ~ MPLA liposomes > no adjuvant. Stronger NAb responses were elicited when the ConM SOSIP trimers were presented on ferritin nanoparticles. We also found that the GLA-LSQ adjuvant induced an unexpectedly strong antibody response to the ferritin core of the nanoparticles. This "off-target" effect may have compromised its ability to induce the more desired antitrimer antibodies. In summary, both adjuvants and nanoparticle display can improve the magnitude of the antibody response to SOSIP trimers but the best combination of trimer presentation and adjuvant can only be identified experimentally.

Published
2021

7. Protective effect of vaginal application of neutralizing and nonneutralizing inhibitory antibodies against vaginal SHIV challenge in macaques

Author

Moog, C, primary, Dereuddre-Bosquet, N, additional, Teillaud, J-L, additional, Biedma, M E, additional, Holl, V, additional, Van Ham, G, additional, Heyndrickx, L, additional, Van Dorsselaer, A, additional, Katinger, D, additional, Vcelar, B, additional, Zolla-Pazner, S, additional, Mangeot, I, additional, Kelly, C, additional, Shattock, R J, additional, and Le Grand, R, additional

Published
2014
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8. CN54gp140: product characteristics, peclinical and clinical use - recombinant glycoprotein for HIV immunization

Author

Katinger, D, primary, Jeffs, S, additional, Altmann, F, additional, Cope, A, additional, McKay, P, additional, Almond, N, additional, Sandström, E, additional, Hejdeman, B, additional, Biberfeld, G, additional, Nilsson, C, additional, Hallengärd, D, additional, Wahren, B, additional, Lehner, T, additional, Singh, M, additional, Lewis, DJ, additional, Lacey, C, additional, and Shattock, R, additional

Published
2012
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10. Profound structural conservation of chemically cross-linked HIV-1 envelope glycoprotein experimental vaccine antigens.

Author

Martin GM, Russell RA, Mundsperger P, Harris S, Jovanoska L, Trajano LF, Schiffner T, Fabian K, Tolazzi M, Scarlatti G, McFarlane L, Cheeseman H, Aldon Y, Schermer EE, Breemen M, Sliepen K, Katinger D, Kunert R, Sanders RW, Shattock R, Ward AB, and Sattentau QJ

Abstract

Chemical cross-linking is used to stabilize protein structures with additional benefits of pathogen and toxin inactivation for vaccine use, but its use has been restricted by the potential for local or global structural distortion. This is of particular importance when the protein in question requires a high degree of structural conservation for inducing a biological outcome such as the elicitation of antibodies to conformationally sensitive epitopes. The HIV-1 envelope glycoprotein (Env) trimer is metastable and shifts between different conformational states, complicating its use as a vaccine antigen. Here we have used the hetero-bifunctional zero-length reagent 1-Ethyl-3-(3-Dimethylaminopropyl)-Carbodiimide (EDC) to cross-link two soluble Env trimers, selected well-folded trimer species using antibody affinity, and transferred this process to good manufacturing practice (GMP) for experimental medicine use. Cross-linking enhanced trimer stability to biophysical and enzyme attack. Cryo-EM analysis revealed that cross-linking retained the overall structure with root-mean-square deviations (RMSDs) between unmodified and cross-linked Env trimers of 0.4-0.5 Å. Despite this negligible distortion of global trimer structure, we identified individual inter-subunit, intra-subunit, and intra-protomer cross-links. Antigenicity and immunogenicity of the trimers were selectively modified by cross-linking, with cross-linked ConS retaining bnAb binding more consistently than ConM. Thus, the EDC cross-linking process improves trimer stability whilst maintaining protein folding, and is readily transferred to GMP, consistent with the more general use of this approach in protein-based vaccine design., (© 2023. The Author(s).)

Published
2023
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11. Dichotomy in Neutralizing Antibody Induction to Peptide-Conjugated Vaccine in Squalene Emulsion Contrast With Aluminum Hydroxide Formulation.

Author

Bonduelle O, Chaudesaigues C, Tolazzi M, Suleiman E, de Bernard S, Alves K, Nourikyan J, Bohec M, Baudrin LG, Katinger D, Debré P, Scarlatti G, Vieillard V, and Combadière B

Subjects
Adjuvants, Immunologic, Aluminum Hydroxide, Animals, Broadly Neutralizing Antibodies, Emulsions, Humans, Mice, Peptides, Rabbits, Squalene, Vaccines, Conjugate, Vaccines, Subunit, Antibodies, Neutralizing, HIV Infections
Abstract

W614A-3S peptide is a modified 3S motif of the HIV-gp41 (mutation W614A). We previously detected the presence of natural neutralizing antibodies directed against W614A-3S peptide (NAbs) in long-term non-progressor HIV + patients. Here, we compared the efficacy of W614A-3S peptide formulated in either squalene emulsion (SQE) or in aluminum hydroxide (Alum) in inducing broadly-NAbs (bNAbs). Rabbit and mouse models were used to screen the induction of bNAbs following 4 immunizations. SQE was more efficient than Alum formulation in inducing W614A-3S-specific bNAbs with up to 67%-93% of HIV strains neutralized. We then analyzed the quality of peptide-specific murine B cells by single-cell gene expression by quantitative reverse transcription-PCR and single-cell V(D)J sequencing. We found more frequent germinal center B cells in SQE than in Alum, albeit with a different gene expression profile. The V(D)J sequencing of W614A-3S-specific BCR showed significant differences in BCR sequences and validates the dichotomy between adjuvant formulations. All sixteen BCR sequences which were cloned were specific of peptide. Adjuvant formulations of W614A-3S-peptide-conjugated immunogen impact the quantity and quality of B cell immune responses at both the gene expression level and BCR sequence., Competing Interests: VV is a member of the scientific advisory board of Minka Therapeutics. ES and DK were employed by Polymun Scientific Immunbiologische Forschung GmbH. SB, KA, and JN were employed by Altrabio. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Bonduelle, Chaudesaigues, Tolazzi, Suleiman, de Bernard, Alves, Nourikyan, Bohec, Baudrin, Katinger, Debré, Scarlatti, Vieillard and Combadière.)

Published
2022
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13. Interplay of diverse adjuvants and nanoparticle presentation of native-like HIV-1 envelope trimers.

Author

Sliepen K, Schermer E, Bontjer I, Burger JA, Lévai RF, Mundsperger P, Brouwer PJM, Tolazzi M, Farsang A, Katinger D, Moore JP, Scarlatti G, Shattock RJ, Sattentau QJ, and Sanders RW

Abstract

The immunogenicity of HIV-1 envelope (Env) trimers is generally poor. We used the clinically relevant ConM SOSIP trimer to compare the ability of different adjuvants (squalene emulsion, ISCOMATRIX, GLA-LSQ, and MPLA liposomes) to support neutralizing antibody (NAb) responses in rabbits. The trimers were administered as free proteins or on nanoparticles. The rank order for the adjuvants was ISCOMATRIX > SE > GLA-LSQ ~ MPLA liposomes > no adjuvant. Stronger NAb responses were elicited when the ConM SOSIP trimers were presented on ferritin nanoparticles. We also found that the GLA-LSQ adjuvant induced an unexpectedly strong antibody response to the ferritin core of the nanoparticles. This "off-target" effect may have compromised its ability to induce the more desired antitrimer antibodies. In summary, both adjuvants and nanoparticle display can improve the magnitude of the antibody response to SOSIP trimers but the best combination of trimer presentation and adjuvant can only be identified experimentally., (© 2021. The Author(s).)

Published
2021
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14. Regulatory approval and a first-in-human phase I clinical trial of a monoclonal antibody produced in transgenic tobacco plants.

Author

Ma JK, Drossard J, Lewis D, Altmann F, Boyle J, Christou P, Cole T, Dale P, van Dolleweerd CJ, Isitt V, Katinger D, Lobedan M, Mertens H, Paul MJ, Rademacher T, Sack M, Hundleby PA, Stiegler G, Stoger E, Twyman RM, Vcelar B, and Fischer R

Subjects
Animals, Broadly Neutralizing Antibodies, Female, Glycomics, HIV Antibodies, Humans, Molecular Sequence Data, Phenotype, Plants, Genetically Modified, Protein Stability, Proteomics, Rabbits, Transformation, Genetic, Antibodies, Monoclonal biosynthesis, Antibodies, Monoclonal therapeutic use, Drug Approval, Social Control, Formal, Nicotiana genetics
Abstract

Although plant biotechnology has been widely investigated for the production of clinical-grade monoclonal antibodies, no antibody products derived from transgenic plants have yet been approved by pharmaceutical regulators for clinical testing. In the Pharma-Planta project, the HIV-neutralizing human monoclonal antibody 2G12 was expressed in transgenic tobacco (Nicotiana tabacum). The scientific, technical and regulatory demands of good manufacturing practice (GMP) were addressed by comprehensive molecular characterization of the transgene locus, confirmation of genetic and phenotypic stability over several generations of transgenic plants, and by establishing standard operating procedures for the creation of a master seed bank, plant cultivation, harvest, initial processing, downstream processing and purification. The project developed specifications for the plant-derived antibody (P2G12) as an active pharmaceutical ingredient (API) based on (i) the guidelines for the manufacture of monoclonal antibodies in cell culture systems; (ii) the draft European Medicines Agency Points to Consider document on quality requirements for APIs produced in transgenic plants; and (iii) de novo guidelines developed with European national regulators. From the resulting process, a GMP manufacturing authorization was issued by the competent authority in Germany for transgenic plant-derived monoclonal antibodies for use in a phase I clinical evaluation. Following preclinical evaluation and ethical approval, a clinical trial application was accepted by the UK national pharmaceutical regulator. A first-in-human, double-blind, placebo-controlled, randomized, dose-escalation phase I safety study of a single vaginal administration of P2G12 was carried out in healthy female subjects. The successful completion of the clinical trial marks a significant milestone in the commercial development of plant-derived pharmaceutical proteins., (© 2015 Society for Experimental Biology, Association of Applied Biologists and John Wiley & Sons Ltd.)

Published
2015
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15. Ch14.18 antibody produced in CHO cells in relapsed or refractory Stage 4 neuroblastoma patients: a SIOPEN Phase 1 study.

Author

Ladenstein R, Weixler S, Baykan B, Bleeke M, Kunert R, Katinger D, Pribill I, Glander P, Bauer S, Pistoia V, Michon J, Garaventa A, and Lode HN

Subjects
Adolescent, Anemia chemically induced, Animals, Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal pharmacokinetics, Area Under Curve, CHO Cells, Child, Child, Preschool, Cricetinae, Cricetulus, Dose-Response Relationship, Drug, Drug Resistance, Neoplasm, Female, Fever chemically induced, Humans, Male, Metabolic Clearance Rate, Mice, Mice, Inbred BALB C, Mice, Inbred Strains, Neoplasm Recurrence, Local, Neoplasm Staging, Neuroblastoma metabolism, Neuroblastoma pathology, Tissue Distribution, Treatment Outcome, Antibodies, Monoclonal therapeutic use, Neuroblastoma drug therapy
Abstract

Purpose: This study aimed to assess the safety, pharmacokinetic and activity profiles of the human-mouse chimeric monoclonal anti-disialoganglioside GD2 antibody ch14.18 produced in Chinese hamster ovary (CHO) cells (ch14.18/CHO)., Methods: Sixteen children with recurrent/refractory neuroblastoma (median age 7.6 y) were enrolled in this Phase 1 dose-finding study. Patients received ch14.18/CHO courses of 10, 20 or 30 mg/m (2)/day as an eight-hour infusion over five consecutive days. Three courses at the same dose level were allowed unless disease progressed. Clearance and biodistribution of radiolabelled ch14.18/CHO in Balb/c and A/J mice were analyzed., Results: A total of 41 ch14.18/CHO courses were given (10 × 3 courses, 5 × 2 courses, 1 × 1 course). Side effects were similar in expectedness, frequency and magnitude to those reported for ch14.18/SP2/0. The dose level of 20 mg/m(2)/day was confirmed. Toxicity was reversible and no treatment-related deaths occurred. In children, the peak plasma concentration was 16.51 µg/ml ± 5.9 µg/ml and the half-life was 76.91 h ± 52.5 h. A partial response following ch14.18/CHO was observed in 2/7 patients with residual disease. In mice, the half-lives were 22.7 h ± 1.9h for ch14.18/CHO and 25.0 h ± 1.9 h for ch14.18/SP2/0. The biodistribution of (125)I-ch14.18/CHO in mice with neuroblastoma was identical to (125)I-ch14.18/SP2/0, indicating GD 2 targeting activity in vivo. Ch14.18 produced in CHO cells showed an unchanged toxicity profile and pharmacokinetics in neuroblastoma patients compared with ch14.18 produced in SP2/0 cells, and evidence of clinical activity was observed. In mice, analysis of pharmacokinetics and biodistribution showed comparable results between ch14.18/CHO and ch14.18/SP2/0. Based on these results, ch14.18/CHO was accepted for prospective clinical evaluation.

Published
2013
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16. Live attenuated influenza viruses produced in a suspension process with avian AGE1.CR.pIX cells.

Author

Lohr V, Genzel Y, Jordan I, Katinger D, Mahr S, Sandig V, and Reichl U

Subjects
Adaptation, Physiological, Animals, Bioreactors, Cell Culture Techniques, Cell Line, Culture Media chemistry, Ducks, Humans, Influenza A Virus, H1N1 Subtype immunology, Influenza A Virus, H1N1 Subtype physiology, Influenza, Human prevention & control, Temperature, Vaccines, Attenuated biosynthesis, Vaccines, Attenuated immunology, Virus Cultivation, Virus Replication, Influenza A Virus, H1N1 Subtype growth & development
Abstract

Background: Current influenza vaccines are trivalent or quadrivalent inactivated split or subunit vaccines administered intramuscularly, or live attenuated influenza vaccines (LAIV) adapted to replicate at temperatures below body temperature and administered intranasally. Both vaccines are considered safe and efficient, but due to differences in specific properties may complement each other to ensure reliable vaccine coverage. By now, licensed LAIV are produced in embryonated chicken eggs. In the near future influenza vaccines for human use will also be available from adherent MDCK or Vero cell cultures, but a scalable suspension process may facilitate production and supply with vaccines., Results: We evaluated the production of cold-adapted human influenza virus strains in the duck suspension cell line AGE1.CR.pIX using a chemically-defined medium. One cold-adapted A (H1N1) and one cold-adapted B virus strain was tested, as well as the reference strain A/PR/8/34 (H1N1). It is shown that a medium exchange is not required for infection and that maximum virus titers are obtained for 1 × 10⁻⁶ trypsin units per cell. 1 L bioreactor cultivations showed that 4 × 10⁶ cells/mL can be infected without a cell density effect achieving titers of 1 × 10⁸ virions/mL after 24 h., Conclusions: Overall, this study demonstrates that AGE1.CR.pIX cells support replication of LAIV strains in a chemically-defined medium using a simple process without medium exchanges. Moreover, the process is fast with peak titers obtained 24 h post infection and easily scalable to industrial volumes as neither microcarriers nor medium replacements are required.

Published
2012
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17. Sustained release of proteins from a modified vaginal ring device.

Author

Morrow RJ, Woolfson AD, Donnelly L, Curran R, Andrews G, Katinger D, and Malcolm RK

Subjects
Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal chemistry, Excipients chemistry, Proteins analysis, Proteins chemistry, Silanes chemistry, Silicone Elastomers chemistry, Solubility, Technology, Pharmaceutical, Time Factors, Water analysis, Contraceptive Devices, Female, Delayed-Action Preparations, Proteins administration & dosage
Abstract

A new vaginal ring technology, the insert vaginal ring (InVR), is presented. The InVR overcomes the current shortfall of conventional vaginal rings (VRs) that are generally ineffectual for the delivery of hydrophilic and/or macromolecular actives, including peptides, proteins and antibodies, due to their poor permeation characteristics in the hydrophobic polymeric elastomers from which VRs are usually fabricated. Release of the model protein BSA from a variety of insert matrices for the InVR is demonstrated, including modified silicone rods, directly compressed tablets and lyophilised gels, which collectively provided controlled release profiles from several hours to beyond 4 weeks. Furthermore, the InVR was shown to deliver over 1 mg of the monoclonal antibody 2F5 from a single device, offering a potential means of protecting women against the transmission of HIV., (Crown Copyright © 2010. Published by Elsevier B.V. All rights reserved.)

Published
2011
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18. Live cold-adapted influenza A vaccine produced in Vero cell line.

Author

Romanova J, Katinger D, Ferko B, Vcelar B, Sereinig S, Kuznetsov O, Stukova M, Erofeeva M, Kiselev O, Katinger H, and Egorov A

Subjects
Adult, Animals, Chlorocebus aethiops, Ferrets, Humans, Influenza A virus genetics, Influenza A virus pathogenicity, Influenza, Human prevention & control, Mice, Mice, Inbred BALB C, Vaccination, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated adverse effects, Vaccines, Attenuated immunology, Vero Cells virology, Virus Replication, Adaptation, Physiological, Cold Temperature, Influenza A virus physiology, Influenza Vaccines administration & dosage, Influenza Vaccines adverse effects, Influenza Vaccines immunology
Abstract

The African green monkey kidney (Vero) cell line was used as a substrate for the development of a live cold-adapted (ca) reassortant influenza vaccine. For that purpose, a new master strain was generated by an adaptation of the wild type (wt) A/Singapore/1/57 virus to growth at 25 degrees C in a Vero cell line. The resulting cold-adapted (ca) muster strain A/Singapore/1/57ca showed temperature sensitive (ts) phenotype and was attenuated in animal models and protective in the challenge experiments in ferrets. Two vaccine candidates of influenza A(H1N1) and A(H3N2) subtypes (6/2 reassortants) inheriting six genes coding internal proteins from the new master strain and the surface antigens hemagglutinin (HA) and neuraminidase (NA) from the epidemic viruses were obtained by a standard method of genetic reassortment. All steps of the vaccine preparation were done exclusively in Vero cells, including the isolation of the epidemic viruses. Both vaccine strains were used for immunization of young adult volunteers in a limited clinical trial and appeared to be safe, well tolerated and immunogenic after intranasal administration.

Published
2004
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19. Effect of a single mutation in neuraminidase on the properties of Influenza B virus isolates.

Author

Katinger D, Romanova J, Ferko B, Fekete H, and Egorov A

Subjects
Amino Acid Substitution, Animals, Cell Division, Cell Line, Chlorocebus aethiops, Dogs, Influenza B virus genetics, Influenza B virus isolation & purification, Neuraminidase metabolism, Vero Cells, Viral Plaque Assay, Influenza B virus enzymology, Mutation, Neuraminidase genetics
Abstract

Two strains of Influenza B virus were isolated in Vero cells. Subclones with improved efficiency of plaque formation were selected. The activity of the neuraminidase (NA) of the two subclones compared to their respective isolates dropped 20- and 100-fold, respectively. Both subclones had a common mutation in segment 6 leading to a change from Asp to Asn at position 457 in the NA. This mutation destroyed a salt bridge of the contact surface between the monomers, thereby causing the loss in enzymatic activity. The decreased NA activity caused improved plaque formation but had no significant impact on the replication in liquid culture.

Published
2004
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20. Receptor-binding properties of modern human influenza viruses primarily isolated in Vero and MDCK cells and chicken embryonated eggs.

Author

Mochalova L, Gambaryan A, Romanova J, Tuzikov A, Chinarev A, Katinger D, Katinger H, Egorov A, and Bovin N

Subjects
Agglutination Tests, Amino Sugars metabolism, Animals, Carbohydrate Sequence, Cell Line, Chick Embryo, Chlorocebus aethiops, Hemagglutinins, Viral chemistry, Hemagglutinins, Viral genetics, Humans, Influenza A virus growth & development, Lactose metabolism, Models, Molecular, Molecular Sequence Data, Vero Cells, Virus Cultivation, Influenza A virus metabolism, Lactose analogs & derivatives, Receptors, Virus metabolism
Abstract

To study the receptor specificity of modern human influenza H1N1 and H3N2 viruses, the analogs of natural receptors, namely sialyloligosaccharides conjugated with high molecular weight (about 1500 kDa) polyacrylamide as biotinylated and label-free probes, have been used. Viruses isolated from clinical specimens were grown in African green monkey kidney (Vero) or Madin-Darby canine kidney (MDCK) cells and chicken embryonated eggs. All Vero-derived viruses had hemagglutinin (HA) sequences indistinguishable from original viruses present in clinical samples, but HAs of three of seven tested MDCK-derived isolates had one or two amino acid substitutions. Despite these host-dependent mutations and differences in the structure of HA molecules of individual strains, all studied Vero- and MDCK-isolated viruses bound to Neu5Ac alpha2-6Galbeta1-4GlcNAc (6'SLN) essentially stronger than to Neu5Acalpha2-6Galbeta1-4Glc (6'SL). Such receptor-binding specificity has been typical for earlier isolated H1N1 human influenza viruses, but there is a new property of H3N2 viruses that has been circulating in the human population during recent years. Propagation of human viruses in chicken embryonated eggs resulted in a selection of variants with amino acid substitutions near the HA receptor-binding site, namely Gln226Arg or Asp225Gly for H1N1 viruses and Leu194Ile and Arg220Ser for H3N2 viruses. These HA mutations disturb the observed strict 6'SLN specificity of recent human influenza viruses.

Published
2003
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21. Distinct host range of influenza H3N2 virus isolates in Vero and MDCK cells is determined by cell specific glycosylation pattern.

Author

Romanova J, Katinger D, Ferko B, Voglauer R, Mochalova L, Bovin N, Lim W, Katinger H, and Egorov A

Subjects
Animals, Cell Line, Chlorocebus aethiops, Dogs, Electrophoresis, Polyacrylamide Gel, Genetic Variation, Humans, Influenza A virus classification, Influenza A virus genetics, Influenza A virus isolation & purification, Kidney, Molecular Sequence Data, Urothelium, Vero Cells, Virus Replication, Influenza A Virus, H3N2 Subtype, Influenza A virus pathogenicity
Abstract

Influenza A viruses were isolated in Vero, MDCK cells and chicken embryos. In contrast to MDCK-derived variants all H3N2 isolates obtained in Vero cells neither agglutinated chicken erythrocytes nor grew in chicken eggs. These host range differences of H3N2 Vero and MDCK isolates were noticed even in the absence of amino acid substitutions in the HA1 molecule. Evaluation of HA glycosylation pattern by treatment with endoglycosidases H and F revealed that Vero-variants contained more oligosaccharides of the high mannose type than did the corresponding MDCK-isolates. Removal of some mannose residues from the non-reducing termini of the carbohydrates by exomannosidase treatment resulted in the ability of Vero-isolates to agglutinate chicken erythrocytes. Glycosylation pattern and properties of H3N2 viruses grown in Vero cells were close to those of viruses grown in human kidney epithelial cells, whereas the H1N1 variants isolated from Vero, MDCK cells or eggs did not differ in agglutination properties, carbohydrate composition or ability to infect eggs.

Published
2003
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22. Hyperattenuated recombinant influenza A virus nonstructural-protein-encoding vectors induce human immunodeficiency virus type 1 Nef-specific systemic and mucosal immune responses in mice.

Author

Ferko B, Stasakova J, Sereinig S, Romanova J, Katinger D, Niebler B, Katinger H, and Egorov A

Subjects
AIDS Vaccines, Animals, Genetic Vectors, HIV Infections immunology, HIV Infections prevention & control, Immunity, Mucosal, Influenza A virus genetics, Influenza A virus immunology, Mice, Reassortant Viruses genetics, Reassortant Viruses immunology, nef Gene Products, Human Immunodeficiency Virus, Gene Products, nef immunology, HIV-1 immunology, Viral Nonstructural Proteins genetics, Viral Nonstructural Proteins immunology
Abstract

We have generated recombinant influenza A viruses belonging to the H1N1 and H3N2 virus subtypes containing an insertion of the 137 C-terminal amino acid residues of the human immunodeficiency virus type 1 (HIV-1) Nef protein into the influenza A virus nonstructural-protein (NS1) reading frame. These viral vectors were found to be genetically stable and capable of growing efficiently in embryonated chicken eggs and tissue culture cells but did not replicate in the murine respiratory tract. Despite the hyperattenuated phenotype of influenza/NS-Nef viruses, a Nef and influenza virus (nucleoprotein)-specific CD8(+)-T-cell response was detected in spleens and the lymph nodes draining the respiratory tract after a single intranasal immunization of mice. Compared to the primary response, a marked enhancement of the CD8(+)-T-cell response was detected in the systemic and mucosal compartments, including mouse urogenital tracts, if mice were primed with the H1N1 subtype vector and subsequently boosted with the H3N2 subtype vector. In addition, Nef-specific serum IgG was detected in mice which were immunized twice with the recombinant H1N1 and then boosted with the recombinant H3N2 subtype virus. These findings may contribute to the development of alternative immunization strategies utilizing hyperattenuated live recombinant influenza virus vectors to prevent or control infectious diseases, e.g., HIV-1 infection.

Published
2001
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23. Chimeric influenza virus replicating predominantly in the murine upper respiratory tract induces local immune responses against human immunodeficiency virus type 1 in the genital tract.

Author

Ferko B, Katinger D, Grassauer A, Egorov A, Romanova J, Niebler B, Katinger H, and Muster T

Subjects
AIDS Vaccines immunology, Administration, Intranasal, Animals, Antibodies, Monoclonal metabolism, Chimera, Enzyme-Linked Immunosorbent Assay, Female, Genetic Vectors, HIV Antibodies immunology, HIV Envelope Protein gp41 genetics, HIV Envelope Protein gp41 immunology, HIV-1 genetics, Humans, Immunity, Mucosal, Influenza A virus genetics, Influenza A virus physiology, Intestinal Mucosa immunology, Intestinal Mucosa virology, Lung virology, Mice, Mice, Inbred BALB C, Mucous Membrane immunology, Mucous Membrane virology, Nasal Mucosa virology, Peptide Fragments immunology, Reassortant Viruses genetics, Vagina metabolism, Vagina virology, Virus Replication, HIV Antibodies biosynthesis, HIV-1 immunology, Influenza A virus immunology, Lung immunology, Nasal Mucosa immunology, Reassortant Viruses immunology, Vagina immunology
Abstract

Previously, a mucosal model of immunization against human immunodeficiency virus type 1 (HIV-1) was established by using influenza virus as a vector for the neutralizing gp41 epitope ELDKWA. Whether replication of this chimeric influenza virus in the upper respiratory tract of mice is sufficient for inducing mucosal immune responses in the genital tract was investigated. An immunization strategy was established that permits the virus to replicate in the murine upper respiratory tracts but not in the lungs. Intranasal application of the chimeric virus induced HIV-1-specific antibodies in sera and genital tract. In addition, chimeric virus-specific antibody-secreting cells were detected in lymphocyte populations obtained from lungs, spleens, and urogenital tracts. These results indicate that replication of the chimeric influenza/ELDKWA virus in the upper respiratory tract is sufficient to induce systemic immune responses as well as local immune responses in the genital tract.

Published
1998
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24. Transfectant influenza A viruses with long deletions in the NS1 protein grow efficiently in Vero cells.

Author

Egorov A, Brandt S, Sereinig S, Romanova J, Ferko B, Katinger D, Grassauer A, Alexandrova G, Katinger H, and Muster T

Subjects
Animals, Cell Line, Chick Embryo, Chlorocebus aethiops, Dogs, Humans, Influenza A virus genetics, Influenza A virus metabolism, Influenza A virus physiology, Mice, Mice, Inbred BALB C, Nucleocapsid biosynthesis, Peptide Biosynthesis, Sequence Deletion, Transfection, Vero Cells, Viral Matrix Proteins biosynthesis, Viral Nonstructural Proteins genetics, Virus Replication, Influenza A virus growth & development, Viral Nonstructural Proteins physiology
Abstract

We established a reverse genetics system for the nonstructural (NS) gene segment of influenza A virus. This system is based on the use of the temperature-sensitive (ts) reassortant virus 25A-1. The 25A-1 virus contains the NS gene from influenza A/Leningrad/134/57 virus and the remaining gene segments from A/Puerto Rico (PR)/8/34 virus. This particular gene constellation was found to be responsible for the ts phenotype. For reverse genetics of the NS gene, a plasmid-derived NS gene from influenza A/PR/8/34 virus was ribonucleoprotein transfected into cells that were previously infected with the 25A-1 virus. Two subsequent passages of the transfection supernatant at 40 degreesC selected viruses containing the transfected NS gene derived from A/PR/8/34 virus. The high efficiency of the selection process permitted the rescue of transfectant viruses with large deletions of the C-terminal part of the NS1 protein. Viable transfectant viruses containing the N-terminal 124, 80, or 38 amino acids of the NS1 protein were obtained. Whereas all deletion mutants grew to high titers in Vero cells, growth on Madin-Darby canine kidney (MDCK) cells and replication in mice decreased with increasing length of the deletions. In Vero cells expression levels of viral proteins of the deletion mutants were similar to those of the wild type. In contrast, in MDCK cells the level of the M1 protein was significantly reduced for the deletion mutants.

Published
1998
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25. Interaction between a Fab fragment against gp41 of human immunodeficiency virus 1 and its peptide epitope: characterization using a peptide epitope library and molecular modeling.

Author

Stigler RD, Rüker F, Katinger D, Elliott G, Höhne W, Henklein P, Ho JX, Keeling K, Carter DC, and Nugel E

Subjects
Amino Acid Sequence, Antibodies, Monoclonal immunology, Binding Sites, Cloning, Molecular, Computer Graphics, Epitopes chemistry, Epitopes metabolism, HIV Envelope Protein gp41 chemistry, HIV Envelope Protein gp41 metabolism, HIV-1 chemistry, Humans, Hydrogen Bonding, Immunodominant Epitopes, Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments metabolism, Models, Molecular, Molecular Sequence Data, Peptides chemistry, Peptides metabolism, Protein Conformation, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins isolation & purification, Recombinant Fusion Proteins metabolism, HIV Envelope Protein gp41 immunology, HIV-1 immunology, Immunoglobulin Fab Fragments immunology
Abstract

The molecular interaction of the Fab fragment of the human monoclonal antibody 3D6, directed against the transmembrane protein gp41 of human immunodeficiency virus (HIV) 1, with its peptide epitope is characterized by a panel of overlapping peptides, a peptide epitope library and molecular modeling techniques. The sequence CSGKLICTTAVPW, corresponding to amino acids 605-617 of gp41, was identified as the best binding peptide (KD = 1 x 10(-8) mol/l). This peptide served as a starting point to prepare a cellulose-bound peptide epitope library in which each residue of the epitope is substituted by all L- and D-amino acids, resulting in 494 epitope peptide variants which were subsequently analyzed for binding 3D6. The library was synthesized to identify residues critical for binding and to obtain information about the molecular environment of the epitope peptide bound to 3D6. Both cysteine residues, as well as isoleucine 6, threonine 8 and proline 12, of the epitope were highly sensitive to substitution. Using the data obtained from the epitope characterization, as well as a low-resolution electron density map of a 3D6 Fab-peptide complex, a 3-D model of the Fab-peptide complex was generated by molecular modeling. The modeling experiments predict binding of the peptide, which is cyclized via the two cysteine residues, to a pocket formed dominantly by the hypervariable loops complementarity determining regions CDR3L, CDR2H and CDR3H.

Published
1995
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