Your search keyword '"Dna immunization"' showing total 17 results

1. A Vaccine Targeting Ovine Herpesvirus 2 Glycoprotein B Protects against Sheep-Associated Malignant Catarrhal Fever.

Author

Cunha, Cristina W., Baker, Katherine N., O'Toole, Donal, Cole, Emily, Shringi, Smriti, Dewals, Benjamin G., Vanderplasschen, Alain, and Li, Hong

Subjects

VACCINE effectiveness, ANIMAL diseases, GENETIC vectors, FEVER, VACCINE trials

Abstract

Malignant catarrhal fever (MCF) is a complex and often fatal disease of ungulates. Effective vaccines are needed to avoid MCF outbreaks and mitigate losses. This study aimed to evaluate a sheep-associated MCF (SA-MCF) vaccine candidate targeting ovine herpesvirus 2 (OvHV-2) glycoprotein B (gB). Rabbits were used as a laboratory animal model to test the safety, immunogenicity, and protective efficacy of a chimeric virus consisting of a recombinant, non-pathogenic strain of alcelaphine herpesvirus-1 encoding OvHV-2 ORF8 to express gB (AlHV-1∆ORF73/OvHV-2-ORF8). Viral-vectored immunizations were performed by using the AlHV-1∆ORF73/OvHV-2-ORF8 chimera alone or as a DNA prime (OvHV-2-ORF8)-virus boost regimen. The viral vector was inoculated by intravenous or intramuscular routes and the DNA was delivered by intradermal shots using a gene gun. The vaccine candidates were deemed safe as no clinical signs were observed following any of the immunizations. Anti-OvHV-2 gB antibodies with neutralizing activity were induced by all immunogens. At three weeks post-final immunization, all animals were challenged intranasally with a lethal dose of OvHV-2. MCF protection rates ranging from 66.7% to 71.4% were observed in vaccinated rabbits, while all mock-vaccinated animals developed the disease. The significant protective efficacy obtained with the vaccine platforms tested in this study encourages further trials in relevant livestock species, such as cattle and bison. [ABSTRACT FROM AUTHOR]

Published

2022

2. A Vaccine Targeting Ovine Herpesvirus 2 Glycoprotein B Protects against Sheep-Associated Malignant Catarrhal Fever

Author

Cristina W. Cunha, Katherine N. Baker, Donal O’Toole, Emily Cole, Smriti Shringi, Benjamin G. Dewals, Alain Vanderplasschen, and Hong Li

Subjects

malignant catarrhal fever, ovine herpesvirus-2, vaccine, viral-vector, DNA immunization, Medicine

Abstract

Malignant catarrhal fever (MCF) is a complex and often fatal disease of ungulates. Effective vaccines are needed to avoid MCF outbreaks and mitigate losses. This study aimed to evaluate a sheep-associated MCF (SA-MCF) vaccine candidate targeting ovine herpesvirus 2 (OvHV-2) glycoprotein B (gB). Rabbits were used as a laboratory animal model to test the safety, immunogenicity, and protective efficacy of a chimeric virus consisting of a recombinant, non-pathogenic strain of alcelaphine herpesvirus-1 encoding OvHV-2 ORF8 to express gB (AlHV-1∆ORF73/OvHV-2-ORF8). Viral-vectored immunizations were performed by using the AlHV-1∆ORF73/OvHV-2-ORF8 chimera alone or as a DNA prime (OvHV-2-ORF8)-virus boost regimen. The viral vector was inoculated by intravenous or intramuscular routes and the DNA was delivered by intradermal shots using a gene gun. The vaccine candidates were deemed safe as no clinical signs were observed following any of the immunizations. Anti-OvHV-2 gB antibodies with neutralizing activity were induced by all immunogens. At three weeks post-final immunization, all animals were challenged intranasally with a lethal dose of OvHV-2. MCF protection rates ranging from 66.7% to 71.4% were observed in vaccinated rabbits, while all mock-vaccinated animals developed the disease. The significant protective efficacy obtained with the vaccine platforms tested in this study encourages further trials in relevant livestock species, such as cattle and bison.

Published

2022

3. M448R and MGF505-7R: Two African Swine Fever Virus Antigens Commonly Recognized by ASFV-Specific T-Cells and with Protective Potential

Author

Laia Bosch-Camós, Elisabet López, Javier Collado, María J. Navas, Miguel Blanco-Fuertes, Sonia Pina-Pedrero, Francesc Accensi, Maria Luisa Salas, Egbert Mundt, Veljko Nikolin, and Fernando Rodríguez

Subjects

African swine fever, antigen discovery, T-cells, DNA immunization, live attenuated virus, protection, Medicine

Abstract

African swine fever (ASF) is today′s number one threat for the global swine industry. Neither commercial vaccine nor treatment is available against ASF and, thus far, only live attenuated viruses (LAV) have provided robust protection against lethal ASF virus (ASFV) challenge infections. Identification of ASFV proteins inducing protective immune responses is one of the major challenges to develop safer and efficient subunit vaccines. Immunopeptidomic studies recently performed in our laboratory allowed identifying ASFV antigens recognized by ASFV-specific CD8+ T-cells. Here, we used data from the SLAI-peptide repertoire presented by a single set of ASFV-infected porcine alveolar macrophages to generate a complex DNA vaccine composed by 15 plasmids encoding the individual peptide-bearing ORFs. DNA vaccine priming improved the protection afforded by a suboptimal dose of the BA71ΔCD2 LAV given as booster vaccination, against Georgia2007/1 lethal challenge. Interestingly, M448R was the only protein promiscuously recognized by the induced ASFV-specific T-cells. Furthermore, priming pigs with DNA plasmids encoding M488R and MGF505-7R, a CD8+ T-cell antigen previously described, confirmed these two proteins as T-cell antigens with protective potential. These studies might be useful to pave the road for designing safe and more efficient vaccine formulations in the future.

Published

2021

4. The C-Terminal Domain of Nefmut Is Dispensable for the CD8+ T Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles

Author

Chiara Chiozzini, Francesco Manfredi, Flavia Ferrantelli, Patrizia Leone, Andrea Giovannelli, Eleonora Olivetta, and Maurizio Federico

Subjects

extracellular vesicles, HIV-1 Nef, DNA immunization, CD8+ T cell immunity, HPV vaccines, SARS-CoV-2 vaccines, Medicine

Abstract

Intramuscular injection of DNA vectors expressing the extracellular vesicle (EV)-anchoring protein Nefmut fused at its C-terminus to viral and tumor antigens elicit a potent, effective, and anti-tolerogenic CD8+ T cell immunity against the heterologous antigen. The immune response is induced through the production of EVs incorporating Nefmut-derivatives released by muscle cells. In the perspective of a possible translation into the clinic of the Nefmut-based vaccine platform, we aimed at increasing its safety profile by identifying the minimal part of Nefmut retaining the EV-anchoring protein property. We found that a C-terminal deletion of 29-amino acids did not affect the ability of Nefmut to associate with EVs. The EV-anchoring function was also preserved when antigens from both HPV16 (i.e., E6 and E7) and SARS-CoV-2 (i.e., S1 and S2) were fused to its C-terminus. Most important, the Nefmut C-terminal deletion did not affect levels, quality, and diffusion at distal sites of the antigen-specific CD8+ T immunity. We concluded that the C-terminal Nefmut truncation does not influence stability, EV-anchoring, and CD8+ T cell immunogenicity of the fused antigen. Hence, the C-terminal deleted Nefmut may represent a safer alternative to the full-length isoform for vaccines in humans.

Published

2021

5. N-Terminal Fatty Acids of NEFMUT Are Required for the CD8+ T-Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles

Author

Chiara Chiozzini, Francesco Manfredi, Claudia Arenaccio, Flavia Ferrantelli, Patrizia Leone, and Maurizio Federico

Subjects

CD8+ T-cell immunity, exosomes, extracellular vesicles, HIV-1 Nef, DNA immunization, Medicine

Abstract

We recently described a cytotoxic CD8+ T lymphocyte (CTL) vaccine platform based on the intramuscular (i.m.) injection of DNA eukaryotic vectors expressing antigens of interest fused at the C-terminus of HIV-1 Nefmut, i.e., a functionally defective mutant that is incorporated at quite high levels into exosomes/extracellular vesicles (EVs). This system has been proven to elicit strong CTL immunity against a plethora of both viral and tumor antigens, as well as inhibit both transplantable and orthotopic tumors in mice. However, a number of open issues remain regarding the underlying mechanism. Here we provide evidence that hindering the uploading into EVs of Nefmut-derived products by removing the Nefmut N-terminal fatty acids leads to a dramatic reduction of the downstream antigen-specific CD8+ T-cell activation after i.m. injection of DNA vectors in mice. This result formally demonstrates that the generation of engineered EVs is part of the mechanism underlying the in vivo induced CD8+ T-cell immunogenicity. Gaining new insights on the EV-based vaccine platform can be relevant in view of its possible translation into the clinic to counteract both chronic and acute infections as well as tumors.

Published

2020

6. Genetically Modified Mouse Mesenchymal Stem Cells Expressing Non-Structural Proteins of Hepatitis C Virus Induce Effective Immune Response

Author

Olga V. Masalova, Ekaterina I. Lesnova, Regina R. Klimova, Ekaterina D. Momotyuk, Vyacheslav V. Kozlov, Alla M. Ivanova, Olga V. Payushina, Nina N. Butorina, Natalia F. Zakirova, Alexander N. Narovlyansky, Alexander V. Pronin, Alexander V. Ivanov, and Alla A. Kushch

Subjects

hepatitis c virus (hcv), mesenchymal stem cells (msc), modified msc, dna immunization, nonstructural hcv proteins, immune response, hcv vaccine, myeloid derived suppressor cells (mdscs), Medicine

Abstract

Hepatitis C virus (HCV) is one of the major causes of chronic liver disease and leads to cirrhosis and hepatocarcinoma. Despite extensive research, there is still no vaccine against HCV. In order to induce an immune response in DBA/2J mice against HCV, we obtained modified mouse mesenchymal stem cells (mMSCs) simultaneously expressing five nonstructural HCV proteins (NS3-NS5B). The innate immune response to mMSCs was higher than to DNA immunization, with plasmid encoding the same proteins, and to naïve unmodified MSCs. mMSCs triggered strong phagocytic activity, enhanced lymphocyte proliferation, and production of type I and II interferons. The adaptive immune response to mMSCs was also more pronounced than in the case of DNA immunization, as exemplified by a fourfold stronger stimulation of lymphocyte proliferation in response to HCV, a 2.6-fold higher rate of biosynthesis, and a 30-fold higher rate of secretion of IFN-γ, as well as by a 40-fold stronger production of IgG2a antibodies to viral proteins. The immunostimulatory effect of mMSCs was associated with pronounced IL-6 secretion and reduction in the population of myeloid derived suppressor cells (MDSCs). Thus, this is the first example that suggests the feasibility of using mMSCs for the development of an effective anti-HCV vaccine.

Published

2020

7. DNA Immunization for HIV Vaccine Development

Author

Yuxin Chen, Shixia Wang, and Shan Lu

Subjects

HIV-1, AIDS, vaccine, DNA immunization, Medicine

Abstract

DNA vaccination has been studied in the last 20 years for HIV vaccine research. Significant experience has been accumulated in vector design, antigen optimization, delivery approaches and the use of DNA immunization as part of a prime-boost HIV vaccination strategy. Key historical data and future outlook are presented. With better understanding on the potential of DNA immunization and recent progress in HIV vaccine research, it is anticipated that DNA immunization will play a more significant role in the future of HIV vaccine development.

Published

2014

8. Genetically Modified Mouse Mesenchymal Stem Cells Expressing Non-Structural Proteins of Hepatitis C Virus Induce Effective Immune Response

Author

Klimova Rr, N. F. Zakirova, A. V. Pronin, Alla A. Kushch, Olga V Payushina, O. V. Masalova, Alexander V. Ivanov, Vyacheslav V Kozlov, Ekaterina D Momotyuk, Nina N Butorina, E. I. Lesnova, A M Ivanova, and A.N. Narovlyansky

Subjects

0301 basic medicine, Genetically modified mouse, DNA immunization, viruses, mesenchymal stem cells (MSC), Immunology, Population, lcsh:Medicine, Lymphocyte proliferation, HCV vaccine, Article, immune response, 03 medical and health sciences, 0302 clinical medicine, Immune system, Drug Discovery, Pharmacology (medical), education, Pharmacology, education.field_of_study, Innate immune system, biology, lcsh:R, nonstructural HCV proteins, virus diseases, biochemical phenomena, metabolism, and nutrition, Acquired immune system, digestive system diseases, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Myeloid-derived Suppressor Cell, myeloid derived suppressor cells (MDSCs), Antibody, hepatitis C virus (HCV), modified MSC

Abstract

Hepatitis C virus (HCV) is one of the major causes of chronic liver disease and leads to cirrhosis and hepatocarcinoma. Despite extensive research, there is still no vaccine against HCV. In order to induce an immune response in DBA/2J mice against HCV, we obtained modified mouse mesenchymal stem cells (mMSCs) simultaneously expressing five nonstructural HCV proteins (NS3-NS5B). The innate immune response to mMSCs was higher than to DNA immunization, with plasmid encoding the same proteins, and to na&iuml, ve unmodified MSCs. mMSCs triggered strong phagocytic activity, enhanced lymphocyte proliferation, and production of type I and II interferons. The adaptive immune response to mMSCs was also more pronounced than in the case of DNA immunization, as exemplified by a fourfold stronger stimulation of lymphocyte proliferation in response to HCV, a 2.6-fold higher rate of biosynthesis, and a 30-fold higher rate of secretion of IFN-&gamma, as well as by a 40-fold stronger production of IgG2a antibodies to viral proteins. The immunostimulatory effect of mMSCs was associated with pronounced IL-6 secretion and reduction in the population of myeloid derived suppressor cells (MDSCs). Thus, this is the first example that suggests the feasibility of using mMSCs for the development of an effective anti-HCV vaccine.

Published

2019

9. M448R and MGF505-7R: Two African Swine Fever Virus Antigens Commonly Recognized by ASFV-Specific T-Cells and with Protective Potential

Author

Javier Collado, Egbert Mundt, Elisabet López, Laia Bosch-Camós, Veljko Nikolin, María L. Salas, Miguel Blanco-Fuertes, Sonia Pina-Pedrero, Francesc Accensi, Fernando Rodriguez, Maria Jesus Navas, Generalitat de Catalunya, Ministerio de Ciencia e Innovación (España), Red de Investigación en Sanidad Animal (España), Producció Animal, and Sanitat Animal

Subjects

0301 basic medicine, DNA immunization, 030106 microbiology, Immunology, Priming (immunology), Immunopeptidomics, Biology, African swine fever virus, Article, Virus, DNA vaccination, 03 medical and health sciences, Plasmid, Immune system, Antigen, Drug Discovery, Pharmacology (medical), Antigen discovery, live attenuated virus, Pharmacology, Protection, Attenuated vaccine, Live attenuated virus, T-cells, immunopeptidomics, protection, biology.organism_classification, Virology, antigen discovery, 030104 developmental biology, Infectious Diseases, Medicine, African swine fever

Abstract

African swine fever (ASF) is today s number one threat for the global swine industry. Neither commercial vaccine nor treatment is available against ASF and, thus far, only live attenuated viruses (LAV) have provided robust protection against lethal ASF virus (ASFV) challenge infections. Identification of ASFV proteins inducing protective immune responses is one of the major challenges to develop safer and efficient subunit vaccines. Immunopeptidomic studies recently performed in our laboratory allowed identifying ASFV antigens recognized by ASFV-specific CD8 T-cells. Here, we used data from the SLAI-peptide repertoire presented by a single set of ASFV-infected porcine alveolar macrophages to generate a complex DNA vaccine composed by 15 plasmids encoding the individual peptide-bearing ORFs. DNA vaccine priming improved the protection afforded by a suboptimal dose of the BA71∆CD2 LAV given as booster vaccination, against Georgia2007/1 lethal challenge. Interestingly, M448R was the only protein promiscuously recognized by the induced ASFV-specific T-cells. Furthermore, priming pigs with DNA plasmids encoding M488R and MGF505-7R, a CD8 T-cell antigen previously described, confirmed these two proteins as T-cell antigens with protective potential. These studies might be useful to pave the road for designing safe and more efficient vaccine formulations in the future., Generalitat de Catalunya (Spain), grant number 2015 DI 037. Studies were co-financed by Boehringer Ingelheim Veterinary Research Center (BIVRC) GmbH & Co. KG, the Ministerio de Ciencia e Innovación of Spain (grant numbers AGL2016-78169-C2-1-R and PID2019-107616RB-I00) and Red de Investigación en Sanidad Animal (RISA)

Published

2021

10. The C-Terminal Domain of Nefmut Is Dispensable for the CD8+ T Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles

Author

Patrizia Leone, Maurizio Federico, Eleonora Olivetta, Francesco Manfredi, Chiara Chiozzini, Flavia Ferrantelli, and Andrea Giovannelli

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, DNA immunization, viruses, T cell, Immunology, lcsh:Medicine, Heterologous, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Drug Discovery, CD8+ T cell immunity, medicine, Cytotoxic T cell, Pharmacology (medical), Pharmacology, Chemistry, Immunogenicity, lcsh:R, virus diseases, Extracellular vesicle, HPV vaccines, SARS-CoV-2 vaccines, Cell biology, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, HIV-1 Nef, 030220 oncology & carcinogenesis, extracellular vesicles, CD8

Abstract

Intramuscular injection of DNA vectors expressing the extracellular vesicle (EV)-anchoring protein Nefmut fused at its C-terminus to viral and tumor antigens elicit a potent, effective, and anti-tolerogenic CD8+ T cell immunity against the heterologous antigen. The immune response is induced through the production of EVs incorporating Nefmut-derivatives released by muscle cells. In the perspective of a possible translation into the clinic of the Nefmut-based vaccine platform, we aimed at increasing its safety profile by identifying the minimal part of Nefmut retaining the EV-anchoring protein property. We found that a C-terminal deletion of 29-amino acids did not affect the ability of Nefmut to associate with EVs. The EV-anchoring function was also preserved when antigens from both HPV16 (i.e., E6 and E7) and SARS-CoV-2 (i.e., S1 and S2) were fused to its C-terminus. Most important, the Nefmut C-terminal deletion did not affect levels, quality, and diffusion at distal sites of the antigen-specific CD8+ T immunity. We concluded that the C-terminal Nefmut truncation does not influence stability, EV-anchoring, and CD8+ T cell immunogenicity of the fused antigen. Hence, the C-terminal deleted Nefmut may represent a safer alternative to the full-length isoform for vaccines in humans.

Published

2021

11. N-Terminal Fatty Acids of NEFMUT Are Required for the CD8+ T-Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles

Author

Maurizio Federico, Chiara Chiozzini, Claudia Arenaccio, Francesco Manfredi, Flavia Ferrantelli, Patrizia Leone, Chiozzini, C., Manfredi, F., Arenaccio, C., Ferrantelli, F., Leone, P., and Federico, M.

Subjects

0301 basic medicine, DNA immunization, Immunology, lcsh:Medicine, exosomes, +, Article, T-cell immunity, 03 medical and health sciences, 0302 clinical medicine, Antigen, In vivo, Drug Discovery, Cytotoxic T cell, Pharmacology (medical), Pharmacology, CD8+ T-cell immunity, Chemistry, Immunogenicity, lcsh:R, CD8, T lymphocyte, Microvesicles, Cell biology, Exosome, CTL, 030104 developmental biology, Infectious Diseases, HIV-1 Nef, Extracellular vesicle, extracellular vesicles, 030215 immunology

Abstract

We recently described a cytotoxic CD8+ T lymphocyte (CTL) vaccine platform based on the intramuscular (i.m.) injection of DNA eukaryotic vectors expressing antigens of interest fused at the C-terminus of HIV-1 Nefmut, i.e., a functionally defective mutant that is incorporated at quite high levels into exosomes/extracellular vesicles (EVs). This system has been proven to elicit strong CTL immunity against a plethora of both viral and tumor antigens, as well as inhibit both transplantable and orthotopic tumors in mice. However, a number of open issues remain regarding the underlying mechanism. Here we provide evidence that hindering the uploading into EVs of Nefmut-derived products by removing the Nefmut N-terminal fatty acids leads to a dramatic reduction of the downstream antigen-specific CD8+ T-cell activation after i.m. injection of DNA vectors in mice. This result formally demonstrates that the generation of engineered EVs is part of the mechanism underlying the in vivo induced CD8+ T-cell immunogenicity. Gaining new insights on the EV-based vaccine platform can be relevant in view of its possible translation into the clinic to counteract both chronic and acute infections as well as tumors.

Published

2020

12. M448R and MGF505-7R: Two African Swine Fever Virus Antigens Commonly Recognized by ASFV-Specific T-Cells and with Protective Potential.

Author

Bosch-Camós, Laia, López, Elisabet, Collado, Javier, Navas, María J., Blanco-Fuertes, Miguel, Pina-Pedrero, Sonia, Accensi, Francesc, Salas, Maria Luisa, Mundt, Egbert, Nikolin, Veljko, Rodríguez, Fernando, and Paillot, Romain

Subjects

AFRICAN swine fever virus, AFRICAN swine fever, T cells, ANTIGENS, DNA vaccines

Abstract

African swine fever (ASF) is today′s number one threat for the global swine industry. Neither commercial vaccine nor treatment is available against ASF and, thus far, only live attenuated viruses (LAV) have provided robust protection against lethal ASF virus (ASFV) challenge infections. Identification of ASFV proteins inducing protective immune responses is one of the major challenges to develop safer and efficient subunit vaccines. Immunopeptidomic studies recently performed in our laboratory allowed identifying ASFV antigens recognized by ASFV-specific CD8+ T-cells. Here, we used data from the SLAI-peptide repertoire presented by a single set of ASFV-infected porcine alveolar macrophages to generate a complex DNA vaccine composed by 15 plasmids encoding the individual peptide-bearing ORFs. DNA vaccine priming improved the protection afforded by a suboptimal dose of the BA71ΔCD2 LAV given as booster vaccination, against Georgia2007/1 lethal challenge. Interestingly, M448R was the only protein promiscuously recognized by the induced ASFV-specific T-cells. Furthermore, priming pigs with DNA plasmids encoding M488R and MGF505-7R, a CD8+ T-cell antigen previously described, confirmed these two proteins as T-cell antigens with protective potential. These studies might be useful to pave the road for designing safe and more efficient vaccine formulations in the future. [ABSTRACT FROM AUTHOR]

Published

2021

13. The C-Terminal Domain of Nef mut Is Dispensable for the CD8 + T Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles.

Author

Chiozzini, Chiara, Manfredi, Francesco, Ferrantelli, Flavia, Leone, Patrizia, Giovannelli, Andrea, Olivetta, Eleonora, Federico, Maurizio, and Tripp, Ralph A.

Subjects

EXTRACELLULAR vesicles, T cells, VIRAL antigens, TUMOR antigens, INTRAMUSCULAR injections

Abstract

Intramuscular injection of DNA vectors expressing the extracellular vesicle (EV)-anchoring protein Nefmut fused at its C-terminus to viral and tumor antigens elicit a potent, effective, and anti-tolerogenic CD8+ T cell immunity against the heterologous antigen. The immune response is induced through the production of EVs incorporating Nefmut-derivatives released by muscle cells. In the perspective of a possible translation into the clinic of the Nefmut-based vaccine platform, we aimed at increasing its safety profile by identifying the minimal part of Nefmut retaining the EV-anchoring protein property. We found that a C-terminal deletion of 29-amino acids did not affect the ability of Nefmut to associate with EVs. The EV-anchoring function was also preserved when antigens from both HPV16 (i.e., E6 and E7) and SARS-CoV-2 (i.e., S1 and S2) were fused to its C-terminus. Most important, the Nefmut C-terminal deletion did not affect levels, quality, and diffusion at distal sites of the antigen-specific CD8+ T immunity. We concluded that the C-terminal Nefmut truncation does not influence stability, EV-anchoring, and CD8+ T cell immunogenicity of the fused antigen. Hence, the C-terminal deleted Nefmut may represent a safer alternative to the full-length isoform for vaccines in humans. [ABSTRACT FROM AUTHOR]

Published

2021

14. N-Terminal Fatty Acids of NEFMUT Are Required for the CD8+ T-Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles.

Author

Chiozzini, Chiara, Manfredi, Francesco, Arenaccio, Claudia, Ferrantelli, Flavia, Leone, Patrizia, and Federico, Maurizio

Subjects

EXTRACELLULAR vesicles, FATTY acids, CYTOTOXIC T cells, TUMOR antigens, VIRAL antigens

Abstract

We recently described a cytotoxic CD8+ T lymphocyte (CTL) vaccine platform based on the intramuscular (i.m.) injection of DNA eukaryotic vectors expressing antigens of interest fused at the C-terminus of HIV-1 Nefmut, i.e., a functionally defective mutant that is incorporated at quite high levels into exosomes/extracellular vesicles (EVs). This system has been proven to elicit strong CTL immunity against a plethora of both viral and tumor antigens, as well as inhibit both transplantable and orthotopic tumors in mice. However, a number of open issues remain regarding the underlying mechanism. Here we provide evidence that hindering the uploading into EVs of Nefmut-derived products by removing the Nefmut N-terminal fatty acids leads to a dramatic reduction of the downstream antigen-specific CD8+ T-cell activation after i.m. injection of DNA vectors in mice. This result formally demonstrates that the generation of engineered EVs is part of the mechanism underlying the in vivo induced CD8+ T-cell immunogenicity. Gaining new insights on the EV-based vaccine platform can be relevant in view of its possible translation into the clinic to counteract both chronic and acute infections as well as tumors. [ABSTRACT FROM AUTHOR]

Published

2020

15. Genetically Modified Mouse Mesenchymal Stem Cells Expressing Non-Structural Proteins of Hepatitis C Virus Induce Effective Immune Response.

Author

Masalova, Olga V., Lesnova, Ekaterina I., Klimova, Regina R., Momotyuk, Ekaterina D., Kozlov, Vyacheslav V., Ivanova, Alla M., Payushina, Olga V., Butorina, Nina N., Zakirova, Natalia F., Narovlyansky, Alexander N., Pronin, Alexander V., Ivanov, Alexander V., and Kushch, Alla A.

Subjects

MESENCHYMAL stem cells, HEPATITIS C virus, PROTEIN C, IMMUNE response, INTERFERON gamma

Abstract

Hepatitis C virus (HCV) is one of the major causes of chronic liver disease and leads to cirrhosis and hepatocarcinoma. Despite extensive research, there is still no vaccine against HCV. In order to induce an immune response in DBA/2J mice against HCV, we obtained modified mouse mesenchymal stem cells (mMSCs) simultaneously expressing five nonstructural HCV proteins (NS3-NS5B). The innate immune response to mMSCs was higher than to DNA immunization, with plasmid encoding the same proteins, and to naïve unmodified MSCs. mMSCs triggered strong phagocytic activity, enhanced lymphocyte proliferation, and production of type I and II interferons. The adaptive immune response to mMSCs was also more pronounced than in the case of DNA immunization, as exemplified by a fourfold stronger stimulation of lymphocyte proliferation in response to HCV, a 2.6-fold higher rate of biosynthesis, and a 30-fold higher rate of secretion of IFN-γ, as well as by a 40-fold stronger production of IgG2a antibodies to viral proteins. The immunostimulatory effect of mMSCs was associated with pronounced IL-6 secretion and reduction in the population of myeloid derived suppressor cells (MDSCs). Thus, this is the first example that suggests the feasibility of using mMSCs for the development of an effective anti-HCV vaccine. [ABSTRACT FROM AUTHOR]

Published

2020

16. N-Terminal Fatty Acids of NEF MUT Are Required for the CD8 + T-Cell Immunogenicity of In Vivo Engineered Extracellular Vesicles.

Author

Chiozzini C, Manfredi F, Arenaccio C, Ferrantelli F, Leone P, and Federico M

Abstract

We recently described a cytotoxic CD8 + T lymphocyte (CTL) vaccine platform based on the intramuscular (i.m.) injection of DNA eukaryotic vectors expressing antigens of interest fused at the C-terminus of HIV-1 Nef mut , i.e., a functionally defective mutant that is incorporated at quite high levels into exosomes/extracellular vesicles (EVs). This system has been proven to elicit strong CTL immunity against a plethora of both viral and tumor antigens, as well as inhibit both transplantable and orthotopic tumors in mice. However, a number of open issues remain regarding the underlying mechanism. Here we provide evidence that hindering the uploading into EVs of Nef mut -derived products by removing the Nef mut N-terminal fatty acids leads to a dramatic reduction of the downstream antigen-specific CD8 + T-cell activation after i.m. injection of DNA vectors in mice. This result formally demonstrates that the generation of engineered EVs is part of the mechanism underlying the in vivo induced CD8 + T-cell immunogenicity. Gaining new insights on the EV-based vaccine platform can be relevant in view of its possible translation into the clinic to counteract both chronic and acute infections as well as tumors.

Published

2020

17. DNA Immunization for HIV Vaccine Development.

Author

Chen Y, Wang S, and Lu S

Abstract

DNA vaccination has been studied in the last 20 years for HIV vaccine research. Significant experience has been accumulated in vector design, antigen optimization, delivery approaches and the use of DNA immunization as part of a prime-boost HIV vaccination strategy. Key historical data and future outlook are presented. With better understanding on the potential of DNA immunization and recent progress in HIV vaccine research, it is anticipated that DNA immunization will play a more significant role in the future of HIV vaccine development.

Published

2014