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1. Cancer Vaccines: Recent Insights and Future Directions.

Author

Malacopol, Aretia-Teodora and Holst, Peter Johannes

Subjects
*HUMAN endogenous retroviruses, *CANCER vaccines, *IMMUNE checkpoint inhibitors, *TREATMENT effectiveness, *ANTIGEN presentation, *T cells, *B cells
Abstract

The field of cancer immunotherapy has seen incredible advancements in the past decades. mRNA-based cancer vaccines generating de novo T cell responses, particularly against tumor-specific antigens (TSAs), have demonstrated promising clinical outcomes and overcome diverse challenges. Despite the high potential of neoantigens to provide personalized immunotherapies through their tumor specificity and immunogenicity, challenges related to the scarcity of immunogenic neoepitopes have prompted continuous research towards finding new tumor-associated antigens (TAAs) and broader therapeutic frameworks, which may now learn from the genuine successes obtained with neoantigens. As an example, human endogenous retroviruses (HERVs) have emerged as potential alternatives to tumor neoantigens due to their high tumoral expression and ability to elicit both T cell reactivity and B cell responses associated with the efficacy of existing immunotherapies. This review aims to assess the status and limitations of TSA-directed mRNA cancer vaccines and the lessons that can be derived from these and checkpoint inhibitor studies to guide TAA vaccine development. We expect that shared B cell, CD4 and CD8 T cell antigen presentation will be key to stimulate continuous T cell expansion and efficacy for tumors that do not contain pre-existing tertiary lymphoid structures. When these structures are present in highly mutated tumors, the current checkpoint-based immunotherapies show efficacy even in immune privileged sites, and vaccines may hold the key to broaden efficacy to more tumor types and stages. [ABSTRACT FROM AUTHOR]

Published
2024
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2. The C-terminal peptide of CCL21 drastically augments CCL21 activity through the dendritic cell lymph node homing receptor CCR7 by interaction with the receptor N-terminus

Author

Jørgensen, Astrid Sissel, Brandum, Emma Probst, Mikkelsen, Jeppe Malthe, Orfin, Klaudia A., Boilesen, Ditte Rahbæk, Egerod, Kristoffer Lihme, Moussouras, Natasha A., Vilhardt, Frederik, Kalinski, Pawel, Basse, Per, Chen, Yen-Hsi, Yang, Zhang, Dwinell, Michael B., Volkman, Brian F., Veldkamp, Christopher T., Holst, Peter Johannes, Lahl, Katharina, Goth, Christoffer Knak, Rosenkilde, Mette Marie, and Hjortø, Gertrud Malene

Published
2021
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3. Preferential Expansion of HPV16 E1-Specific T Cells from Healthy Donors’ PBMCs after Ex Vivo Immunization with an E1E2E6E7 Fusion Antigen

Author

Daradoumis, Joana, primary, Müller, Mikkel Dons, additional, Neckermann, Patrick, additional, Asbach, Benedikt, additional, Schrödel, Silke, additional, Thirion, Christian, additional, Wagner, Ralf, additional, thor Straten, Per, additional, Holst, Peter Johannes, additional, and Boilesen, Ditte, additional

Published
2023
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5. Immunohistochemical characterization of integrin alfa 6 in uterus and cervix of the cynomolgus monkeys (Macaca fascicularis) with MfPV3 infection.

Author

Setyawaty, Dyah, Mariya, Silmi, Prabandari, Silvia A., Boilessen, Ditte Rahbaek, Holst, Peter Johannes, and Darusman, Huda Shalahudin

Subjects
KRA, CERVIX uteri, HUMAN papillomavirus, CERVICAL intraepithelial neoplasia, EPITHELIUM, EPITHELIAL cells
Abstract

Background: Cervical cancer is an abnormal growth of cervical tissue epithelial cells due to persistent human papilloma virus (HPV) infection. Cynomolgus monkeys (Macaca fascicularis) can be naturally and spontaneously infected with M. fascicularis Papillomavirus Type 3 (MfPV3), a virus that is phylogenetically closely related to human oncogenic HPV (HPV-16 and HPV-34), and therefore a potentially beneficial for modeling HPV disease. This study aims to evaluate the expression of the integrin alpha 6 (ITGa6) receptor in cynomolgus monkeys spontaneously infected with MfPV3, which this receptor also found in human infected with HPV. Methods: The study was done on archived Formalin-fixed Paraffin-Embedded (FFPE) samples of uterine and cervix tissue of cynomolgus monkeys. Immunohistochemistry was also performed to quantify the expression levels of ITGa6. Results: The results showed 80% of the samples positive Cervical Intraepithelial Neoplasia (CIN) and increased expression of ITGa6 significantly in Positive-MfPV3 group than negative-MfPV3 group. Conclusions: This indicated the potential of cynomolgus monkeys as a spontaneous oncogenesis model of PV infection type. [ABSTRACT FROM AUTHOR]

Published
2024
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7. An Endogenous Retrovirus Vaccine Encoding an Envelope with a Mutated Immunosuppressive Domain in Combination with Anti-PD1 Treatment Eradicates Established Tumours in Mice

Author

Daradoumis, Joana, primary, Ragonnaud, Emeline, additional, Skandorff, Isabella, additional, Nielsen, Karen Nørgaard, additional, Bermejo, Amaia Vergara, additional, Andersson, Anne-Marie, additional, Schroedel, Silke, additional, Thirion, Christian, additional, Neukirch, Lasse, additional, and Holst, Peter Johannes, additional

Published
2023
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8. Supplementary Data from Efficacy and Synergy with Cisplatin of an Adenovirus Vectored Therapeutic E1E2E6E7 Vaccine against HPV Genome–Positive C3 Cancers in Mice

Author

Boilesen, Ditte Rahbæk, primary, Neckermann, Patrick, primary, Willert, Torsten, primary, Müller, Mikkel Dons, primary, Schrödel, Silke, primary, Pertl, Cordula, primary, Thirion, Christian, primary, Asbach, Benedikt, primary, Wagner, Ralf, primary, and Holst, Peter Johannes, primary

Published
2023
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10. The Insertion of an Evolutionary Lost Four-Amino-Acid Cytoplasmic Tail Peptide into a Syncytin-1 Vaccine Increases T- and B-Cell Responses in Mice

Author

Skandorff, Isabella, Gille, Jasmin, Ragonnaud, Emeline, Andersson, Anne Marie, Schrödel, Silke, Thirion, Christian, Wagner, Ralf, Holst, Peter Johannes, Skandorff, Isabella, Gille, Jasmin, Ragonnaud, Emeline, Andersson, Anne Marie, Schrödel, Silke, Thirion, Christian, Wagner, Ralf, and Holst, Peter Johannes

Abstract

Human endogenous retrovirus type W (HERV-W) is expressed in various cancers. We previously developed an adenovirus-vectored cancer vaccine targeting HERV-W by encoding an assembled HERV-W group-specific antigen sequence and the HERV-W envelope sequence Syncytin-1. Syncytin-1 is constitutively fusogenic and forms large multinucleated cell fusions when overexpressed. Consequently, immunising humans with a vaccine encoding Syncytin-1 can lead to the formation of extensive syncytia, which is undesirable and poses a potential safety issue. Here, we show experiments in cell lines that restoring an evolutionary lost cleavage site of the fusion inhibitory R-peptide of Syncytin-1 inhibit cell fusion. Interestingly, this modification of the HERV-W vaccine’s fusogenicity increased the expression of the vaccine antigens in vitro. It also enhanced Syncytin-1-specific antibody responses and CD8+-mediated T-cell responses compared to the wildtype vaccine in vaccinated mice, with a notable enhancement in responses to subdominant T-cell epitopes but equal responses to dominant epitopes and similar rates of survival following a tumour challenge. The impairment of cell–cell fusion and the enhanced immunogenicity profile of this HERV-W vaccine strengthens the prospects of obtaining a meaningful immune response against HERV-W in patients with HERV-W-overexpressing cancers.

Published
2023

11. Human Ad19a/64 HERV-W Vaccines Uncover Immunosuppression Domain-Dependent T-Cell Response Differences in Inbred Mice

Author

Skandorff, Isabella, Ragonnaud, Emeline, Gille, Jasmin, Andersson, Anne Marie, Schrödel, Silke, Duvnjak, Lara, Turner, Louise, Thirion, Christian, Wagner, Ralf, Holst, Peter Johannes, Skandorff, Isabella, Ragonnaud, Emeline, Gille, Jasmin, Andersson, Anne Marie, Schrödel, Silke, Duvnjak, Lara, Turner, Louise, Thirion, Christian, Wagner, Ralf, and Holst, Peter Johannes

Abstract

Expression of human endogenous retrovirus type W (HERV-W) has been linked to cancer, making HERV-W antigens potential targets for therapeutic cancer vaccines. In a previous study, we effectively treated established tumours in mice by using adenoviral-vectored vaccines targeting the murine endogenous retrovirus envelope and group-specific antigen (Gag) of melanoma-associated retrovirus (MelARV) in combination with anti-PD-1. To break the immunological tolerance to MelARV, we mutated the immunosuppressive domain (ISD) of the MelARV envelope. However, reports on the immunogenicity of the HERV-W envelope, Syncytin-1, and its ISD are conflicting. To identify the most effective HERV-W cancer vaccine candidate, we evaluated the immunogenicity of vaccines encoding either the wild-type or mutated HERV-W envelope ISD in vitro and in vivo. Here, we show that the wild-type HERV-W vaccine generated higher activation of murine antigen-presenting cells and higher specific T-cell responses than the ISD-mutated counterpart. We also found that the wild-type HERV-W vaccine was sufficient to increase the probability of survival in mice subjected to HERV-W envelope-expressing tumours compared to a control vaccine. These findings provide the foundation for developing a therapeutic cancer vaccine targeting HERV-W-positive cancers in humans.

Published
2023

12. Efficacy and Synergy with Cisplatin of an Adenovirus Vectored Therapeutic E1E2E6E7 Vaccine against HPV Genome-Positive C3 Cancers in Mice

Author

Boilesen, Ditte Rahbæk, Neckermann, Patrick, Willert, Torsten, Müller, Mikkel Dons, Schrödel, Silke, Pertl, Cordula, Thirion, Christian, Asbach, Benedikt, Wagner, Ralf, Holst, Peter Johannes, Boilesen, Ditte Rahbæk, Neckermann, Patrick, Willert, Torsten, Müller, Mikkel Dons, Schrödel, Silke, Pertl, Cordula, Thirion, Christian, Asbach, Benedikt, Wagner, Ralf, and Holst, Peter Johannes

Abstract

Human papillomavirus (HPV) infections are the main cause of cervical and oropharyngeal cancers. As prophylactic vaccines have no curative effect, an efficient therapy would be highly desired. Most therapeutic vaccine candidates target only a small subset of HPV regulatory proteins, namely, E6 and E7, and are therefore restricted in the breadth of their immune response. However, research has suggested E1 and E2 as promising targets to fight HPV+ cancer. Here, we report the design of adenoviral vectors efficiently expressing HPV16 E1 and E2 in addition to transformation-deficient E6 and E7. Vaccination elicited vigorous CD4+ and CD8+ T-cell responses against all encoded HPV16 proteins in outbred mice and against E1 and E7 in C57BL/6 mice. Therapeutic vaccination of C3 tumor-bearing mice led to significantly reduced tumor growth and enhanced survival for both small and established tumors. Tumor biopsies revealed increased numbers of tumor-infiltrating CD8+ T cells in treated mice. Cisplatin enhanced the effect of therapeutic vaccination, accompanied by enhanced infiltration of dendritic cells into the tumor. CD8+ T cells were identified as effector cells in T-cell depletion assays, seemingly under regulation by FoxP3+CD4+ regulatory T cells. Finally, therapeutic vaccination with Ad-Ii-E1E2E6E7 exhibited significantly enhanced survival compared with vaccination with two peptides each harboring a known E6/E7 epitope. We hypothesize that this difference could be due to the induction of additional T-cell responses against E1. These results support the use of this novel vaccine candidate targeting an extended set of antigens (Ad-Ii-E1E2E6E7), in combination with cisplatin, as an advanced strategy to combat HPV+ cancers.

Published
2023

13. Preferential Expansion of HPV16 E1-Specific T Cells from Healthy Donors’ PBMCs after Ex Vivo Immunization with an E1E2E6E7 Fusion Antigen

Author

Daradoumis, Joana, Müller, Mikkel Dons, Neckermann, Patrick, Asbach, Benedikt, Schrödel, Silke, Thirion, Christian, Wagner, Ralf, thor Straten, Per, Holst, Peter Johannes, Boilesen, Ditte, Daradoumis, Joana, Müller, Mikkel Dons, Neckermann, Patrick, Asbach, Benedikt, Schrödel, Silke, Thirion, Christian, Wagner, Ralf, thor Straten, Per, Holst, Peter Johannes, and Boilesen, Ditte

Abstract

Persistent human papillomavirus (HPV) infection is responsible for practically all cervical and a high proportion of anogenital and oropharyngeal cancers. Therapeutic HPV vaccines in clinical development show great promise in improving outcomes for patients who mount an anti-HPV T-cell response; however, far from all patients elicit a sufficient immunological response. This demonstrates a translational gap between animal models and human patients. Here, we investigated the potential of a new assay consisting of co-culturing vaccine-transduced dendritic cells (DCs) with syngeneic, healthy, human peripheral blood mononuclear cells (PBMCs) to mimic a human in vivo immunization. This new promising human ex vivo PBMC assay was evaluated using an innovative therapeutic adenovirus (Adv)-based HPV vaccine encoding the E1, E2, E6, and E7 HPV16 genes. This new method allowed us to show that vaccine-transduced DCs yielded functional effector T cells and unveiled information on immunohierarchy, showing E1-specific T-cell immunodominance over time. We suggest that this assay can be a valuable translational tool to complement the known animal models, not only for HPV therapeutic vaccines, and supports the use of E1 as an immunotherapeutic target. Nevertheless, the findings reported here need to be validated in a larger number of donors and preferably in patient samples.

Published
2023

15. Efficacy and Synergy with Cisplatin of an Adenovirus Vectored Therapeutic E1E2E6E7 Vaccine against HPV Genome–Positive C3 Cancers in Mice

Author

Boilesen, Ditte Rahbæk, primary, Neckermann, Patrick, additional, Willert, Torsten, additional, Müller, Mikkel Dons, additional, Schrödel, Silke, additional, Pertl, Cordula, additional, Thirion, Christian, additional, Asbach, Benedikt, additional, Wagner, Ralf, additional, and Holst, Peter Johannes, additional

Published
2022
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18. A systematic review of expression and immunogenicity of human endogenous retroviral proteins in cancer and discussion of therapeutic approaches

Author

Müller, Mikkel Dons, Holst, Peter Johannes, Nielsen, Karen Nørgaard, Müller, Mikkel Dons, Holst, Peter Johannes, and Nielsen, Karen Nørgaard

Abstract

Human endogenous retroviruses (HERVs) are remnants of ancient retroviral infections that have become fixed in the human genome. While HERV genes are typically silenced in healthy somatic cells, there are numerous reports of HERV transcription and translation across a wide spectrum of cancers, while T and B cell responses against HERV proteins have been detected in cancer patients. This review systematically categorizes the published evidence on the expression of and adaptive immune response against specific HERVs in distinct cancer types. A systematic literature search was performed using Medical Search Headings (MeSH) in the PubMed/Medline database. Papers were included if they described the translational activity of HERVs. We present multiple tables that pair the protein expression of specific HERVs and cancer types with information on the quality of the evidence. We find that HERV-K is the most investigated HERV. HERV-W (syncytin-1) is the second-most investigated, while other HERVs have received less attention. From a therapeutic perspective, HERV-K and HERV-E are the only HERVs with experimental demonstration of effective targeted therapies, but unspecific approaches using antiviral and demethylating agents in combination with chemo- and immunotherapies have also been investigated.

Published
2022

20. GPR183 Is Dispensable for B1 Cell Accumulation and Function, but Affects B2 Cell Abundance, in the Omentum and Peritoneal Cavity

Author

Barington, Line, primary, Christensen, Liv von Voss, additional, Pedersen, Kristian Kåber, additional, Niss Arfelt, Kristine, additional, Roumain, Martin, additional, Jensen, Kristian Høj Reveles, additional, Kjær, Viktoria Madeline Skovgaard, additional, Daugvilaite, Viktorija, additional, Kearney, John F., additional, Christensen, Jan Pravsgaard, additional, Hjortø, Gertrud Malene, additional, Muccioli, Giulio G., additional, Holst, Peter Johannes, additional, and Rosenkilde, Mette Marie, additional

Published
2022
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23. Design and Immunological Validation of Macaca fascicularis Papillomavirus Type 3 Based Vaccine Candidates in Outbred Mice: Basis for Future Testing of a Therapeutic Papillomavirus Vaccine in NHPs

Author

Neckermann, Patrick, primary, Boilesen, Ditte Rahbaek, additional, Willert, Torsten, additional, Pertl, Cordula, additional, Schrödel, Silke, additional, Thirion, Christian, additional, Asbach, Benedikt, additional, Holst, Peter Johannes, additional, and Wagner, Ralf, additional

Published
2021
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25. Novel antigenic targets of HPV therapeutic vaccines

Author

Boilesen, Ditte Rahbæk, Nielsen, Karen Nørgaard, Holst, Peter Johannes, Boilesen, Ditte Rahbæk, Nielsen, Karen Nørgaard, and Holst, Peter Johannes

Abstract

Human papillomavirus (HPV) infection is the cause of the majority of cervical cancers and head and neck cancers worldwide. Although prophylactic vaccines and cervical cancer screening programs have shown efficacy in preventing HPV-associated cervical cancer, cervical cancer is still a major cause of morbidity and mortality, especially in third world countries. Furthermore, head and neck cancer cases caused by HPV infection and associated mortality are increasing. The need for better therapy is clear, and therapeutic vaccination generating cytotoxic T cells against HPV proteins is a promising strategy. This review covers the current scene of HPV therapeutic vaccines in clinical development and discusses relevant considerations for the design of future HPV therapeutic vaccines and clinical trials, such as HPV protein expression patterns, immunogenicity, and exhaustion in relation to the different stages and types of HPV-associated lesions and cancers. Ultimately, while the majority of the HPV therapeutic vaccines currently in clinical testing target the two HPV oncoproteins E6 and E7, we suggest that there is a need to include more HPV antigens in future HPV therapeutic vaccines to increase efficacy and find that especially E1 and E2 could be promising novel targets.

Published
2021

26. Design and immunological validation of Macaca fascicularis Papillomavirus Type 3 based vaccine candidates in outbred mice:Basis for future testing of a therapeutic papillomavirus vaccine in NHPs

Author

Neckermann, Patrick, Boilesen, Ditte Rahbaek, Willert, Torsten, Pertl, Cordula, Schrödel, Silke, Thirion, Christian, Asbach, Benedikt, Holst, Peter Johannes, Wagner, Ralf, Neckermann, Patrick, Boilesen, Ditte Rahbaek, Willert, Torsten, Pertl, Cordula, Schrödel, Silke, Thirion, Christian, Asbach, Benedikt, Holst, Peter Johannes, and Wagner, Ralf

Abstract

Persistent human papillomavirus (HPV) infections are causative for cervical neoplasia and carcinomas. Despite the availability of prophylactic vaccines, morbidity and mortality induced by HPV are still too high. Thus, an efficient therapy, such as a therapeutic vaccine, is urgently required. Herein, we describe the development and validation of Macaca fascicularis papillomavirus type 3 (MfPV3) antigens delivered via nucleic-acid and adenoviral vectors in outbred mouse models. Ten artificially fused polypeptides comprising early viral regulatory proteins were designed and optionally linked to the T cell adjuvant MHC-II-associated invariant chain. Transfected HEK293 cells and A549 cells transduced with recombinant adenoviruses expressing the same panel of artificial antigens proved proper and comparable expression, respectively. Immunization of outbred CD1 and OF1 mice led to CD8+ and CD4+ T cell responses against MfPV3 antigens after DNA- and adenoviral vector delivery. Moreover, in vivo cytotoxicity of vaccine-induced CD8+ T cells was demonstrated in BALB/c mice by quantifying specific killing of transferred peptide-pulsed syngeneic target cells. The use of the invariant chain as T cell adjuvant enhanced the T cell responses regarding cytotoxicity and in vitro analysis suggested an accelerated turnover of the antigens as causative. Notably, the fusion-polypeptide elicited the same level of T-cell responses as administration of the antigens individually, suggesting no loss of immunogenicity by fusing multiple proteins in one vaccine construct. These data support further development of the vaccine candidates in a follow up efficacy study in persistently infected Macaca fascicularis monkeys to assess their potential to eliminate pre-malignant papillomavirus infections, eventually instructing the design of an analogous therapeutic HPV vaccine.

Published
2021

28. MHC class II invariant chain-adjuvanted viral vectored vaccines enhances T cell responses in humans

Author

Esposito, Ilaria, Cicconi, Paola, D'Alise, Anna Morena, Brown, Anthony, Esposito, Marialuisa, Swadling, Leo, Holst, Peter Johannes, Bassi, Maria Rosaria, Stornaiuolo, Mariano, Mori, Federica, Vassilev, Ventzislav, Li, Wenqin, Donnison, Timothy, Gentile, Chiara, Turner, Bethany, von Delft, Annette, Del Sorbo, Mariarosaria, Barra, Federica, Contino, Alessandra Maria, Abbate, Adele, Novellino, Ettore, Thomsen, Allan Randrup, Christensen, Jan Pravsgaard, Lahm, Armin, Grazioli, Fabiana, Ammendola, Virginia, Siani, Loredana, Colloca, Stefano, Klenerman, Paul, Nicosia, Alfredo, Dorrell, Lucy, Folgori, Antonella, Capone, Stefania, Barnes, Eleanor, Esposito, Ilaria, Cicconi, Paola, D'Alise, Anna Morena, Brown, Anthony, Esposito, Marialuisa, Swadling, Leo, Holst, Peter Johannes, Bassi, Maria Rosaria, Stornaiuolo, Mariano, Mori, Federica, Vassilev, Ventzislav, Li, Wenqin, Donnison, Timothy, Gentile, Chiara, Turner, Bethany, von Delft, Annette, Del Sorbo, Mariarosaria, Barra, Federica, Contino, Alessandra Maria, Abbate, Adele, Novellino, Ettore, Thomsen, Allan Randrup, Christensen, Jan Pravsgaard, Lahm, Armin, Grazioli, Fabiana, Ammendola, Virginia, Siani, Loredana, Colloca, Stefano, Klenerman, Paul, Nicosia, Alfredo, Dorrell, Lucy, Folgori, Antonella, Capone, Stefania, and Barnes, Eleanor

Abstract

Strategies to enhance the induction of high magnitude T cell responses through vaccination are urgently needed. Major histocompatibility complex (MHC) class II-associated invariant chain (Ii) plays a critical role in antigen presentation, forming MHC class II peptide complexes for the generation of CD4+ T cell responses. Preclinical studies evaluating the fusion of Ii to antigens encoded in vector delivery systems have shown that this strategy may enhance T cell immune responses to the encoded antigen. We now assess this strategy in humans, using chimpanzee adenovirus 3 and modified vaccinia Ankara vectors encoding human Ii fused to the nonstructural (NS) antigens of hepatitis C virus (HCV) in a heterologous prime/boost regimen. Vaccination was well tolerated and enhanced the peak magnitude, breadth, and proliferative capacity of anti-HCV T cell responses compared to non-Ii vaccines in humans. Very high frequencies of HCV-specific T cells were elicited in humans. Polyfunctional HCV-specific CD8+ and CD4+ responses were induced with up to 30% of CD3+CD8+ cells targeting single HCV epitopes; these were mostly effector memory cells with a high proportion expressing T cell activation and cytolytic markers. No volunteers developed anti-Ii T cell or antibody responses. Using a mouse model and in vitro experiments, we show that Ii fused to NS increases HCV immune responses through enhanced ubiquitination and proteasomal degradation. This strategy could be used to develop more potent HCV vaccines that may contribute to the HCV elimination targets and paves the way for developing class II Ii vaccines against cancer and other infections.

Published
2020

29. The potential of adenoviral vaccine vectors with altered antigen presentation capabilities

Author

Neukirch, Lasse, Fougeroux, Cyrielle, Andersson, Anne Marie Carola, Holst, Peter Johannes, Neukirch, Lasse, Fougeroux, Cyrielle, Andersson, Anne Marie Carola, and Holst, Peter Johannes

Abstract

Introduction: Despite their appeal as vaccine vectors, adenoviral vectors are yet unable to induce protective immune responses against some weakly immunogenic antigens. Additionally, the maximum doses of adenovirus-based vaccines are limited by vector-induced toxicity, causing vector elimination and diminished immune responses against the target antigen. In order to increase immune responses to the transgene, while maintaining a moderate vector dose, new technologies for improved transgene presentation have been developed for adenoviral vaccine vectors. Areas covered: This review provides an overview of different genetic-fusion adjuvants that aim to improve antigen presentation in the context of adenoviral vector-based vaccines. The influence on both T cell and B cell responses are discussed, with a main focus on two technologies: MHC class II-associated invariant chain and virus-like-vaccines. Expert opinion: Different strategies have been tested to improve adenovirus-based vaccinations with varying degrees of success. The reviewed genetic adjuvants were designed to increase antigen processing and MHC presentation, or promote humoral immune responses with an improved conformational antigen display. While none of the introduced technologies is universally applicable, this review shall give an overview to identify potential improvements for future vaccination approaches.

Published
2020

35. In vivo testing of novel vaccine prototypes against Actinobacillus pleuropneumoniae

Author

Antenucci, Fabio, Fougeroux, Cyrielle, Deeney, Alannah, Ørskov, Cathrine, Rycroft, Andrew, Holst, Peter Johannes, Bojesen, Anders Miki, Antenucci, Fabio, Fougeroux, Cyrielle, Deeney, Alannah, Ørskov, Cathrine, Rycroft, Andrew, Holst, Peter Johannes, and Bojesen, Anders Miki

Abstract

Actinobacillus pleuropneumoniae (A. pleuropneumoniae) is a Gram-negative bacterium that represents the main cause of porcine pleuropneumonia in pigs, causing significant economic losses to the livestock industry worldwide. A. pleuropneumoniae, as the majority of Gram-negative bacteria, excrete vesicles from its outer membrane (OM), accordingly defined as outer membrane vesicles (OMVs). Thanks to their antigenic similarity to the OM, OMVs have emerged as a promising tool in vaccinology. In this study we describe the in vivo testing of several vaccine prototypes for the prevention of infection by all known A. pleuropneumoniae serotypes. Previously identified vaccine candidates, the recombinant proteins ApfA and VacJ, administered individually or in various combinations with the OMVs, were employed as vaccination strategies. Our data show that the addition of the OMVs in the vaccine formulations significantly increased the specific IgG titer against both ApfA and VacJ in the immunized animals, confirming the previously postulated potential of the OMVs as adjuvant. Unfortunately, the antibody response raised did not translate into an effective protection against A. pleuropneumoniae infection, as none of the immunized groups following challenge showed a significantly lower degree of lesions than the controls. Interestingly, quite the opposite was true, as the animals with the highest IgG titers were also the ones bearing the most extensive lesions in their lungs. These results shed new light on A. pleuropneumoniae pathogenicity, suggesting that antibody-mediated cytotoxicity from the host immune response may play a central role in the development of the lesions typically associated with A. pleuropneumoniae infections.

Published
2018

37. Mucosal vaccination with heterologous viral vectored vaccine targeting subdominant SIV accessory antigens strongly inhibits early viral replication

Author

Xu, Huanbin, Andersson, Anne-Marie Carola, Ragonnaud, Emeline, Boilesen, Ditte, Tolver, Anders, Jensen, Benjamin Anderschou Holbech, Blanchard, James L, Nicosia, Alfredo, Folgori, Antonella, Colloca, Stefano, Cortese, Riccardo, Thomsen, Allan Randrup, Christensen, Jan Pravsgaard, Veazey, Ronald S., Holst, Peter Johannes, Xu, Huanbin, Andersson, Anne-Marie Carola, Ragonnaud, Emeline, Boilesen, Ditte, Tolver, Anders, Jensen, Benjamin Anderschou Holbech, Blanchard, James L, Nicosia, Alfredo, Folgori, Antonella, Colloca, Stefano, Cortese, Riccardo, Thomsen, Allan Randrup, Christensen, Jan Pravsgaard, Veazey, Ronald S., and Holst, Peter Johannes

Abstract

Conventional HIV T cell vaccine strategies have not been successful in containing acute peak viremia, nor in providing long-term control. We immunized rhesus macaques intramuscularly and rectally using a heterologous adenovirus vectored SIV vaccine regimen encoding normally weakly immunogenic tat, vif, rev and vpr antigens fused to the MHC class II associated invariant chain. Immunizations induced broad T cell responses in all vaccinees. Following up to 10 repeated low-dose intrarectal challenges, vaccinees suppressed early viral replication (P=0.01) and prevented the peak viremia in 5/6 animals. Despite consistently undetectable viremia in 2 out of 6 vaccinees, all animals showed evidence of infection induced immune responses indicating that infection had taken place. Vaccinees, with and without detectable viremia better preserved their rectal CD4+ T cell population and had reduced immune hyperactivation as measured by naïve T cell depletion, Ki-67 and PD-1 expression on T cells. These results indicate that vaccination towards SIV accessory antigens vaccine can provide a level of acute control of SIV replication with a suggestion of beneficial immunological consequences in infected animals of unknown long-term significance. In conclusion, our studies demonstrate that a vaccine encoding subdominant antigens not normally associated with virus control can exert a significant impact on acute peak viremia.

Published
2017

38. Identification and characterization of serovar-independent immunogens in Actinobacillus pleuropneumoniae

Author

Antenucci, Fabio, Fougeroux, Cyrielle, Bosse, Janine T., Magnowska, Zofia, Roesch, Camille, Langford, Paul, Holst, Peter Johannes, Bojesen, Anders Miki, Antenucci, Fabio, Fougeroux, Cyrielle, Bosse, Janine T., Magnowska, Zofia, Roesch, Camille, Langford, Paul, Holst, Peter Johannes, and Bojesen, Anders Miki

Abstract

Despite numerous actions to prevent disease, Actinobacillus pleuropneumoniae (A. pleuropneumoniae) remains a major cause of porcine pleuropneumonia, resulting in economic losses to the swine industry worldwide. In this paper, we describe the utilization of a reverse vaccinology approach for the selection and in vitro testing of serovar-independent A. pleuropneumoniae immunogens. Potential immunogens were identified in the complete genomes of three A. pleuropneumoniae strains belonging to different serovars using the following parameters: predicted outer-membrane subcellular localization; ≤ 1 trans-membrane helices; presence of a signal peptide in the protein sequence; presence in all known A. pleuropneumoniae genomes; homology with other well characterized factors with relevant data regarding immunogenicity/protective potential. Using this approach, we selected the proteins ApfA and VacJ to be expressed and further characterized, both in silico and in vitro. Additionally, we analysed outer membrane vesicles (OMVs) of A. pleuropneumoniae MIDG2331 as potential immunogens, and compared deletions in degS and nlpI for increasing yields of OMVs compared to the parental strain. Our results indicated that ApfA and VacJ are highly conserved proteins, naturally expressed during infection by all A. pleuropneumoniae serovars tested. Furthermore, OMVs, ApfA and VacJ were shown to possess a high immunogenic potential in vitro. These findings favour the immunogen selection protocol used, and suggest that OMVs, along with ApfA and VacJ, could represent effective immunogens for the prevention of A. pleuropneumoniae infections in a serovar-independent manner. This hypothesis is nonetheless predictive in nature, and in vivo testing in a relevant animal model will be necessary to verify its validity.

Published
2017

39. Breadth of T cell responses after immunization with adenovirus vectors encoding ancestral antigens or polyvalent papillomavirus antigens

Author

Ragonnaud, Emeline, Pedersen, Anders Gorm, Holst, Peter Johannes, Ragonnaud, Emeline, Pedersen, Anders Gorm, and Holst, Peter Johannes

Abstract

Oncogenic human papillomaviruses (HPVs) are in most cases eliminated by intervention of T cells. As many other pathogens, these oncogenic HPVs belong to an ancient and diverse virus family. Therefore, we found it relevant to investigate the potential and limitations of inducing a broad response - either by inducing cross-reactive T cells or by administering a polyvalent vaccine. To test these strategies, we designed 3 ancestral and 2 circulating sequences based on the two domains of the E1 and E2 proteins of papillomaviruses (PVs) that exhibit the highest degree of conservation in comparison to the other PV proteins. The PV sequences were fused to a T cell adjuvant, the murine invariant chain and encoded in a recombinant adenoviral vector which was administered to naïve outbred mice. By measuring T cell responses induced by these different vaccines and towards peptide pools representing 3 circulating strains and a putative ancestor of oncogenic HPVs, we showed that the ancestral vaccine antigen has to be approximately 90% identical to the circulating PVs before a marked drop of ~90% mean CD8+ T cell responses ensues. Interestingly, the combination of two or three type-specific PV vaccines did not induce a significant decrease of the CD8+ T cell response to the individual targeted PV types. Polyvalent HPV vaccine based on the E1 and E2 proteins seem to be capable of triggering responses towards more than one type of PV while the cross-reactivity of ancestral vaccine seems insufficient in consideration of the sequence diversity between HPV types.

Published
2017

41. Mucosal Vaccination with Heterologous Viral Vectored Vaccine Targeting Subdominant SIV Accessory Antigens Strongly Inhibits Early Viral Replication

Author

Xu, Huanbin, primary, Andersson, Anne-Marie, additional, Ragonnaud, Emeline, additional, Boilesen, Ditte, additional, Tolver, Anders, additional, Jensen, Benjamin Anderschou Holbech, additional, Blanchard, James L., additional, Nicosia, Alfredo, additional, Folgori, Antonella, additional, Colloca, Stefano, additional, Cortese, Riccardo, additional, Thomsen, Allan Randrup, additional, Christensen, Jan Pravsgaard, additional, Veazey, Ronald S., additional, and Holst, Peter Johannes, additional

Published
2017
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42. Increased T cell breadth and antibody response elicited in prime-boost regimen by viral vector encoded homologous SIV Gag/Env in outbred CD1 mice

Author

Andersson, Anne Marie Carola, Holst, Peter Johannes, Andersson, Anne Marie Carola, and Holst, Peter Johannes

Abstract

Background: A major obstacle for the development of HIV vaccines is the virus' worldwide sequence diversity. Nevertheless, the presence of T cell epitopes within conserved regions of the virus' structural Gag protein and conserved structures in the envelope (env) sequence raises the possibility that cross-reactive responses may be induced by vaccination. In this study, the aim was to investigate the importance of antigenic match on immunodominance and breadth of obtainable T cell responses. Methods: Outbred CD1 mice were immunized with either heterologous (SIVmac239 and HIV-1 clade B consensus) or homologous (SIVmac239) gag sequences using adenovirus (Ad5) and MVA vectors. Env (SIVmac239) was co-encoded in the vectors to study the induction of antibodies, which is a primary target of current HIV vaccine designs. All three vaccines were designed as virus-encoded virus-like particle vaccines. Antibody responses were analysed by ELISA, avidity ELISA, and neutralization assay. T cell responses were determined by intracellular cytokine staining of splenocytes. Results: The homologous Env/Gag prime-boost regimen induced higher Env binding antibodies, and induced stronger and broader Gag specific CD8+ T cell responses than the homologous Env/heterologous Gag prime-boost regimen. Homologous Env/heterologous Gag immunization resulted in selective boosting of Env specific CD8+ T cell responses and consequently a paradoxical decreased recognition of variant sequences including conserved elements of p24 Gag. Conclusions: These results contrast with related studies using Env or Gag as the sole antigen and suggest that prime-boost immunizations based on homologous SIVmac239 Gag inserts is an efficient component of genetic VLP vaccines-both for induction of potent antibody responses and cross-reactive CD8+ T cell responses.

Published
2016

43. Early life vaccination:Generation of adult-quality memory CD8+ T cells in infant mice using non-replicating adenoviral vectors

Author

Nazerai, Loulieta, Bassi, Maria Rosaria, Uddbäck, Ida Elin Maria, Holst, Peter Johannes, Christensen, Jan Pravsgaard, Thomsen, Allan Randrup, Nazerai, Loulieta, Bassi, Maria Rosaria, Uddbäck, Ida Elin Maria, Holst, Peter Johannes, Christensen, Jan Pravsgaard, and Thomsen, Allan Randrup

Abstract

Intracellular pathogens represent a serious threat during early life. Importantly, even though the immune system of newborns may be characterized as developmentally immature, with a propensity to develop Th2 immunity, significant CD8+ T-cell responses may still be elicited in the context of optimal priming. Replication deficient adenoviral vectors have been demonstrated to induce potent CD8+ T-cell response in mice, primates and humans. The aim of the present study was therefore to assess whether replication-deficient adenovectors could overcome the risk of overwhelming antigen stimulation during the first period of life and provide a pertinent alternative in infant vaccinology. To address this, infant mice were vaccinated with three different adenoviral vectors and the CD8+ T-cell response after early life vaccination was explored. We assessed the frequency, polyfunctionality and in vivo cytotoxicity of the elicited memory CD8+ T cells, as well as the potential of these cells to respond to secondary infections and confer protection. We further tested the impact of maternal immunity against our replication-deficient adenoviral vector during early life vaccination. Overall, our results indicate that memory CD8+ T cells induced by adenoviral vectors in infant mice are of good quality and match those elicited in the adult host.

Published
2016

45. Targeting of non-dominant antigens as a vaccine strategy to broaden T-cell responses during chronic viral infection

Author

Holst, Peter Johannes, Jensen, Benjamin Anderschou Holbech, Ragonnaud, Emeline, Thomsen, Allan Randrup, Christensen, Jan Pravsgaard, Holst, Peter Johannes, Jensen, Benjamin Anderschou Holbech, Ragonnaud, Emeline, Thomsen, Allan Randrup, and Christensen, Jan Pravsgaard

Abstract

In this study, we compared adenoviral vaccine vectors with the capacity to induce equally potent immune responses against non-dominant and immunodominant epitopes of murine lymphocytic choriomeningitis virus (LCMV). Our results demonstrate that vaccination targeting non-dominant epitopes facilitates potent virus-induced T-cell responses against immunodominant epitopes during subsequent challenge with highly invasive virus. In contrast, when an immunodominant epitope was included in the vaccine, the T-cell response associated with viral challenge remained focussed on that epitope. Early after challenge with live virus, the CD8+ T cells specific for vaccine-encoded epitopes, displayed a phenotype typically associated with prolonged/persistent antigenic stimulation marked by high levels of KLRG-1, as compared to T cells reacting to epitopes not included in the vaccine. Notably, this association was lost over time in T cells specific for the dominant T cell epitopes, and these cells were fully capable of expanding in response to a new viral challenge. Overall, our data suggests a potential for broadening of the antiviral CD8+ T-cell response by selecting non-dominant antigens to be targeted by vaccination. In addition, our findings suggest that prior adenoviral vaccination is not likely to negatively impact the long-term and protective immune response induced and maintained by a vaccine-attenuated chronic viral infection.

Published
2015

48. IFNγ and perforin cooperate to control infection and prevent fatal pathology during persistent gammaherpesvirus infection in mice

Author

Bartholdy, Christina, Høgh-Petersen, Mette, Storm, Pernille, Holst, Peter Johannes, Orskov, Cathrine, Christensen, Jan Pravsgaard, Thomsen, Allan Randrup, Bartholdy, Christina, Høgh-Petersen, Mette, Storm, Pernille, Holst, Peter Johannes, Orskov, Cathrine, Christensen, Jan Pravsgaard, and Thomsen, Allan Randrup

Abstract

Infection with murine gammaherpes virus 68 has become an accepted model for studying the virus/host interactions with regard to gammaherpes virus infections. Previous studies using gene deficient mice have revealed that neither IFNγ nor perforin are essential in controlling the course of infection or the virus load during chronic infection in C57BL/6 mice. However, transient multiorgan fibrosis and splenic atrophy is observed in mice lacking IFNγ or the IFNγ receptor. To study the interplay between perforin and IFNγ in controlling the virus-induced pathology and the viral load during chronic gamma herpes virus infection, we infected IFNγ/perforin double deficient C57BL/6 mice and followed the outcome of infection. While absence of perforin prevented the splenic atrophy in IFNγ deficient mice, fibrosis did not disappear. Moreover, double deficient mice developed extreme splenomegaly, were unable to control the viral load and displayed chronic immune activation. Thus IFNγ and perforin act in concert to minimize pathology and control the viral load in mice chronically infected with MHV68. Furthermore, while certain aspect of the virus-induced pathology in IFNγ deficient mice may be alleviated in double deficient mice, other aspects are exaggerated, and the normal architecture of the spleen is completely destroyed. Thus, IFNγ and perforin work in concert to minimize pathology and control the viral load. In the absence of both effector molecules, the balancing race between the virus and the host is tipped in favour of the virus causing chronic immune activation and fatal disease. This article is protected by copyright. All rights reserved.

Published
2014

49. Qualitative and quantitative analysis of adenovirus type 5 vector-induced memory CD8 T cells:not as bad as their reputation

Author

Steffensen, Maria Abildgaard, Holst, Peter Johannes, Steengaard, Sanne Skovvang, Jensen, Benjamin Anderschou Holbech, Bartholdy, Christina, Buus, Anette Stryhn, Christensen, Jan Pravsgaard, Thomsen, Allan Randrup, Steffensen, Maria Abildgaard, Holst, Peter Johannes, Steengaard, Sanne Skovvang, Jensen, Benjamin Anderschou Holbech, Bartholdy, Christina, Buus, Anette Stryhn, Christensen, Jan Pravsgaard, and Thomsen, Allan Randrup

Published
2013

50. Qualitative and quantitative analysis of Ad5 vector induced memory CD8 T cells:not as bad as their reputation

Author

Steffensen, Maria Abildgaard, Holst, Peter Johannes, Steengaard, Sanne Skovvang, Jensen, Benjamin Anderschou Holbech, Bartholdy, Christina, Stryhn, Anette, Christensen, Jan Pravsgaard, Thomsen, Allan Randrup, Steffensen, Maria Abildgaard, Holst, Peter Johannes, Steengaard, Sanne Skovvang, Jensen, Benjamin Anderschou Holbech, Bartholdy, Christina, Stryhn, Anette, Christensen, Jan Pravsgaard, and Thomsen, Allan Randrup

Abstract

It has been reported that adenovirus (Ad) primed CD8 T cells may display a distinct and partially exhausted phenotype. Given the practical implications of this claim, we decided to analyze in detail the quality of Ad-primed CD8 T cells directly comparing these cells to CD8 T cells induced through infection with lymphocytic choriomeningitis virus. We found that localized immunization with intermediate doses of Ad vector induce a moderate number of functional CD8 T cells, which qualitatively match those found in LCMV-infected mice. Numbers of these cells may be efficiently increased by additional adenoviral boosting and, importantly, the generated secondary memory cells cannot be qualitatively differentiated from those induced by primary infection with replicating virus. Quantitatively, DNA priming prior to Ad-vaccination will lead to even higher numbers of memory cells. In this case, the vaccination leads to the generation of a population of memory cells characterized by relatively low CD27 expression and high CD127 and KLRG1 expression. These memory CD8 T cells are capable of proliferating in response to viral challenge, and protect against infection with live virus. Furthermore, viral challenge is followed by sustained expansion of the memory CD8 T-cell population, and the generated memory cells do not appear to have been driven towards exhaustive differentiation. Based on these findings, we suggest that adenovirus based prime-boost regimens (including Ad5 and Ad5-like vectors) represent an effective means to induce a substantially expanded, long-lived population of high-quality transgene-specific memory CD8 T cells.

Published
2013

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