Your search keyword '"immunization route"' showing total 31 results

1. Immunogenicity and Protective Efficacy of Aerosolized Live-Attenuated Yellow Fever 17D Vaccine in Mice.

Author

Zhu, Feng, Sun, Meng-Xu, Zhao, Suo-Qun, Qin, Cheng-Feng, Wang, Jin-Hua, and Deng, Yong-Qiang

Subjects

YELLOW fever, IMMUNE response, PHYTOPLASMAS, IMMUNIZATION, BRONCHOALVEOLAR lavage

Abstract

Yellow fever (YF), caused by the yellow fever virus (YFV), continually spreads and causes epidemics worldwide, posing a great threat to human health. The live-attenuated YF 17D vaccine (YF-17D) has been licensed for preventing YFV infection and administrated via the intramuscular (i.m.) route. In this study, we sought to determine the immunogenicity and protective efficacy of aerosolized YF-17D via the intratracheal (i.t.) route in mice. YF-17D stocks in liquids were successfully aerosolized into particles of 6 μm. Further in vitro phenotype results showed the aerosolization process did not abolish the infectivity of YF-17D. Meanwhile, a single i.t. immunization with aerosolized YF-17D induced robust humoral and cellular immune responses in A129 mice, which is comparable to that received i.p. immunization. Notably, the aerosolized YF-17D also triggered specific secretory IgA (SIgA) production in bronchoalveolar lavage. Additionally, all immunized animals survived a lethal dose of YFV challenge in mice. In conclusion, our results support further development of aerosolized YF-17D in the future. [ABSTRACT FROM AUTHOR]

Published

2024

2. Effect of vaccination route (intradermal vs. intramuscular) against porcine reproductive and respiratory syndrome using a modified live vaccine on systemic and mucosal immune response and virus transmission in pigs

Author

Patricia Renson, Sophie Mahé, Mathieu Andraud, Mireille Le Dimna, Frédéric Paboeuf, Nicolas Rose, and Olivier Bourry

Subjects

PRRS virus, MLV, Immunization route, Transmission, Mucosal immune response, Vaccine efficacy, Veterinary medicine, SF600-1100

Abstract

Abstract Background Porcine reproductive and respiratory syndrome (PRRS) is a viral disease with worldwide distribution and an enormous economic impact. To control PRRS virus (PRRSV) infection, modified live vaccines (MLVs) are widely used in the field, mainly administered via an intramuscular (IM) route. Currently, some MLVs are authorized for intradermal (ID) administration, which has many practical and welfare advantages. The objectives of the study were to compare the immune responses (systemic in blood and mucosal in lungs) and vaccine efficacy in preventing challenge strain transmission after IM or needle-free ID immunization of piglets with an MLV against PRRSV-1 (MLV1). Methods Groups of sixteen 5-week-old specific pathogen-free piglets were vaccinated with Porcilis PRRS® (MSD) either by an IM (V+ IM) or ID route (V+ ID) using an IDAL®3G device or kept unvaccinated (V-). Four weeks after vaccination, in each group, 8 out of the 16 piglets were challenged intranasally with a PRRSV-1 field strain, and one day later, the inoculated pigs were mingled by direct contact with the remaining 8 sentinel noninoculated pigs to evaluate PRRSV transmission. Thus, after the challenge, each group (V+ IM, V+ ID or V-) included 8 inoculated and 8 contact piglets. During the postvaccination and postchallenge phases, PRRSV replication (RT–PCR), PRRSV-specific antibodies (ELISA IgG and IgA, virus neutralization tests) and cell-mediated immunity (ELISPOT Interferon gamma) were monitored in blood and bronchoalveolar lavages (BALs). Results Postvaccination, vaccine viremia was lower in V+ ID pigs than in V+ IM pigs, whereas the cell-mediated immune response was detected earlier in the V+ ID group at 2 weeks postvaccination. In the BAL fluid, a very low mucosal immune response (humoral and cellular) was detected. Postchallenge, the vaccine efficacy was similar in inoculated animals with partial control of PRRSV viremia in V+ ID and V+ IM animals. In vaccinated sentinel pigs, vaccination drastically reduced PRRSV transmission with similar estimated transmission rates and latency durations for the V+ IM and V+ ID groups. Conclusions Our results show that the tested MLV1 induced a faster cell-mediated immune response after ID immunization two weeks after vaccination but was equally efficacious after IM or ID immunization towards a challenge four weeks later. Considering the practical and welfare benefits of ID vaccination, these data further support the use of this route for PRRS MLVs.

Published

2024

3. 鲤疱疹病毒二型（CyHV-II)疫苗研究进展.

Author

吴琳娇, 孙丽芳, 朱春华, 张红, 董盼盼, 陈磊清, and 吴允昆

Abstract

Copyright of Journal of Agricultural Science & Technology (1008-0864) is the property of Journal of Agricultural Science & Technology and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

4. Effect of vaccination route (intradermal vs. intramuscular) against porcine reproductive and respiratory syndrome using a modified live vaccine on systemic and mucosal immune response and virus transmission in pigs.

Author

Renson, Patricia, Mahé, Sophie, Andraud, Mathieu, Le Dimna, Mireille, Paboeuf, Frédéric, Rose, Nicolas, and Bourry, Olivier

Subjects

*PORCINE reproductive & respiratory syndrome, *SWINE breeding, *IMMUNE response, *VACCINE effectiveness, *SWINE, *VACCINATION, *CELLULAR immunity

Abstract

Background: Porcine reproductive and respiratory syndrome (PRRS) is a viral disease with worldwide distribution and an enormous economic impact. To control PRRS virus (PRRSV) infection, modified live vaccines (MLVs) are widely used in the field, mainly administered via an intramuscular (IM) route. Currently, some MLVs are authorized for intradermal (ID) administration, which has many practical and welfare advantages. The objectives of the study were to compare the immune responses (systemic in blood and mucosal in lungs) and vaccine efficacy in preventing challenge strain transmission after IM or needle-free ID immunization of piglets with an MLV against PRRSV-1 (MLV1). Methods: Groups of sixteen 5-week-old specific pathogen-free piglets were vaccinated with Porcilis PRRS® (MSD) either by an IM (V+ IM) or ID route (V+ ID) using an IDAL®3G device or kept unvaccinated (V-). Four weeks after vaccination, in each group, 8 out of the 16 piglets were challenged intranasally with a PRRSV-1 field strain, and one day later, the inoculated pigs were mingled by direct contact with the remaining 8 sentinel noninoculated pigs to evaluate PRRSV transmission. Thus, after the challenge, each group (V+ IM, V+ ID or V-) included 8 inoculated and 8 contact piglets. During the postvaccination and postchallenge phases, PRRSV replication (RT–PCR), PRRSV-specific antibodies (ELISA IgG and IgA, virus neutralization tests) and cell-mediated immunity (ELISPOT Interferon gamma) were monitored in blood and bronchoalveolar lavages (BALs). Results: Postvaccination, vaccine viremia was lower in V+ ID pigs than in V+ IM pigs, whereas the cell-mediated immune response was detected earlier in the V+ ID group at 2 weeks postvaccination. In the BAL fluid, a very low mucosal immune response (humoral and cellular) was detected. Postchallenge, the vaccine efficacy was similar in inoculated animals with partial control of PRRSV viremia in V+ ID and V+ IM animals. In vaccinated sentinel pigs, vaccination drastically reduced PRRSV transmission with similar estimated transmission rates and latency durations for the V+ IM and V+ ID groups. Conclusions: Our results show that the tested MLV1 induced a faster cell-mediated immune response after ID immunization two weeks after vaccination but was equally efficacious after IM or ID immunization towards a challenge four weeks later. Considering the practical and welfare benefits of ID vaccination, these data further support the use of this route for PRRS MLVs. [ABSTRACT FROM AUTHOR]

Published

2024

5. Immunogenicity and Protective Efficacy of Aerosolized Live-Attenuated Yellow Fever 17D Vaccine in Mice

Author

Feng Zhu, Meng-Xu Sun, Suo-Qun Zhao, Cheng-Feng Qin, Jin-Hua Wang, and Yong-Qiang Deng

Subjects

yellow fever virus, aerosol, immunization route, immunogenicity, protective efficacy, Medicine

Abstract

Yellow fever (YF), caused by the yellow fever virus (YFV), continually spreads and causes epidemics worldwide, posing a great threat to human health. The live-attenuated YF 17D vaccine (YF-17D) has been licensed for preventing YFV infection and administrated via the intramuscular (i.m.) route. In this study, we sought to determine the immunogenicity and protective efficacy of aerosolized YF-17D via the intratracheal (i.t.) route in mice. YF-17D stocks in liquids were successfully aerosolized into particles of 6 μm. Further in vitro phenotype results showed the aerosolization process did not abolish the infectivity of YF-17D. Meanwhile, a single i.t. immunization with aerosolized YF-17D induced robust humoral and cellular immune responses in A129 mice, which is comparable to that received i.p. immunization. Notably, the aerosolized YF-17D also triggered specific secretory IgA (SIgA) production in bronchoalveolar lavage. Additionally, all immunized animals survived a lethal dose of YFV challenge in mice. In conclusion, our results support further development of aerosolized YF-17D in the future.

Published

2024

6. Perception and willingness toward various immunization routes for COVID-19 vaccines: a cross-sectional survey in China

Author

Haohang Wang, Mingting Cui, Shunran Li, Fan Wu, Shiqiang Jiang, Hongbiao Chen, Jianhui Yuan, and Caijun Sun

Subjects

COVID-19 vaccine, immunization route, booster, needle fear, vaccine hesitancy, Public aspects of medicine, RA1-1270

Abstract

BackgroundTo date, most vaccines, including the COVID-19 vaccine, are mainly administered by intramuscular injection, which might lead to vaccine hesitancy in some populations due to needle fear. Alternatively, needle-free immunization technology is extensively developed to improve the efficacy and acceptance of vaccination. However, there is no study to report the perception and willingness toward various immunization routes of the COVID-19 vaccine in the general population.MethodsA cross-sectional survey was conducted nationwide using an online questionnaire. Bivariate analyses were undertaken to assess variable associations among the participants who reported a hesitancy to receive the COVID-19 booster vaccination. Multivariable logistic regression with a backward step-wise approach was used to analyze the predicted factors associated with the willingness to receive the COVID-19 booster vaccination.ResultsA total of 3,244 valid respondents were included in this survey, and 63.2% of participants thought they had a good understanding of intramuscular injection, but only 20.7, 9.2, 9.4, and 6.0% of participants had a self-perceived good understanding of inhalation vaccine, nasal spray vaccine, oral vaccine, and microneedle patch vaccine. Correspondingly, there was high acceptance for intramuscular injection (76.5%), followed by oral inhalation (64.4%) and nasal spray (43.0%). Those participants who were only willing to receive an intramuscular vaccine had less vaccine knowledge (OR = 0.78; 95% CI: 0.65–0.94) than those who were willing to receive a needle-free vaccine (OR = 1.97; 95% CI: 1.52–2.57). Some factors were found to be associated with vaccine hesitancy toward booster COVID-19 vaccination.ConclusionNeedle-free vaccination is a promising technology for the next generation of vaccines, but we found that intramuscular injection was still the most acceptable immunization route in this survey. One major reason might be that most people lack knowledge about needle-free vaccination. We should strengthen the publicity of needle-free vaccination technology, and thus improve the acceptance and coverage of vaccination in different populations.

Published

2023

7. Subunit vaccines for Acinetobacter baumannii.

Author

Ning Yang, Xiao Jin, Chenghua Zhu, Fenglin Gao, Zheqi Weng, Xingran Du, and Ganzhu Feng

Subjects

ACINETOBACTER baumannii, VACCINES, INTRAMUSCULAR injections, SUBCUTANEOUS injections, VACCINE effectiveness

Abstract

Acinetobacter baumannii is a gram-negative bacterium and a crucial opportunistic pathogen in hospitals. A. baumannii infection has become a challenging problem in clinical practice due to the increasing number of multidrug-resistant strains and their prevalence worldwide. Vaccines are effective tools to prevent and control A. baumannii infection. Many researchers are studying subunit vaccines against A. baumannii. Subunit vaccines have the advantages of high purity, safety, and stability, ease of production, and highly targeted induced immune responses. To date, no A. baumannii subunit vaccine candidate has entered clinical trials. This may be related to the easy degradation of subunit vaccines in vivo and weak immunogenicity. Using adjuvants or delivery vehicles to prepare subunit vaccines can slow down degradation and improve immunogenicity. The common immunization routes include intramuscular injection, subcutaneous injection, intraperitoneal injection and mucosal vaccination. The appropriate immunization method can also enhance the immune effect of subunit vaccines. Therefore, selecting an appropriate adjuvant and immunization method is essential for subunit vaccine research. This review summarizes the past exploration of A. baumannii subunit vaccines, hoping to guide current and future research on these vaccines. [ABSTRACT FROM AUTHOR]

Published

2023

8. A new candidate vaccine for human brucellosis based on influenza viral vectors: a preliminary investigation for the development of an immunization schedule in a guinea pig model

Author

Dina Bugybayeva, Zhailaubay Kydyrbayev, Nadezhda Zinina, Nurika Assanzhanova, Bolat Yespembetov, Yerken Kozhamkulov, Kunsulu Zakarya, Sholpan Ryskeldinova, and Kaissar Tabynov

Subjects

Human brucellosis, Influenza viral vectors, Vaccine candidate, Protection, Guinea pigs, Immunization route, Infectious and parasitic diseases, RC109-216, Public aspects of medicine, RA1-1270

Abstract

Abstract Background A new candidate vector vaccine against human brucellosis based on recombinant influenza viral vectors (rIVV) subtypes H5N1 expressing Brucella outer membrane protein (Omp) 16, L7/L12, Omp19 or Cu–Zn SOD proteins has been developed. This paper presents the results of the study of protection of the vaccine using on guinea pigs, including various options of administering, dose and frequency. Provided data of the novel vaccine candidate will contribute to its further movement into the preclinical stage study. Methods General states of guinea pigs was assessed based on behavior and dynamics of a guinea pig weight-gain test. The effectiveness of the new anti-brucellosis vector vaccine was determined by studying its protective effect after conjunctival, intranasal and sublingual administration in doses 105 EID50, 106 EID50 and 107 EID50 during prime and boost vaccinations of animals, followed by challenge with a virulent strain of B. melitensis 16 M infection. For sake of comparison, the commercial B. melitensis Rev.1 vaccine was used as a control. The protective properties of vaccines were assessed by quantitation of Brucella colonization in organs and tissues of infected animals and compared to the control groups. Results It was observed a gradual increase in body weight of guinea pigs after prime and booster immunization with the vaccine using conjunctival, intranasal and sublingual routes of administration, as well as after using various doses of vaccine. The most optimal way of using the vaccine has been established: double intranasal immunization of guinea pigs at a dose of 106 EID50, which provides 80% protection of guinea pigs from B. melitensis 16 M infection (P

Published

2021

9. Simultaneous Intramuscular And Intranasal Administration Of Chitosan Nanoparticles–Adjuvanted Chlamydia Vaccine Elicits Elevated Protective Responses In The Lung

Author

Li Y, Wang C, Sun Z, Xiao J, Yan X, Chen Y, Yu J, and Wu Y

Subjects

Chlamydia psittaci, vaccine, chitosan nanoparticles, immunization route, respiratory infection, Medicine (General), R5-920

Abstract

Yumeng Li,1 Chuan Wang,1 Zhenjie Sun,1 Jian Xiao,1 Xiaoliang Yan,1 Yuqing Chen,1 Jian Yu,2 Yimou Wu1 1Hunan Provincial Key Laboratory for Special Pathogens Prevention and Control, Institution of Pathogenic Biology, Hengyang Medical College, University of South China, Hengyang 421001, People’s Republic of China; 2Department of Experimental Zoology, Hengyang Medical College, University of South China, Hengyang 421001, People’s Republic of ChinaCorrespondence: Yimou WuHunan Provincial Key Laboratory for Special Pathogens Prevention and Control, Institution of Pathogenic Biology, Hengyang Medical College, University of South China, 28 West Changsheng Road, Hengyang, Hunan 421001, People’s Republic of ChinaTel +86 734-13707340050Fax +86-734-8282907Email yimouwu@sina.comBackground: Chlamydia psittaci is a zoonotic bacteria closely associated with psittacosis/ornithosis. Vaccination has been recognized as the best way to inhibit the spread of C. psittaci due to the majority ignored of infections. The optimal Chlamydia vaccine was obstructed by the defect of single immunization route and the lack of availability of nontoxic and valid adjuvants.Methods: In this study, we developed a novel immunization strategy, simultaneous (SIM) intramuscular (IM) and intranasal (IN) administration of a C. psittaci antigens (Ags) adjuvanted with chitosan nanoparticles (CNPs). And SIM-CNPs-Ags were used to determine the different types of immune response and the protective role in vivo.Results: CNPs-Ags with zeta-potential values of 13.12 mV and of 276.1 nm showed excellent stability and optimal size for crossing the mucosal barrier with high 71.7% encapsulation efficiency. SIM-CPN-Ags mediated stronger humoral and mucosal responses by producing meaningfully high levels of IgG and secretory IgA (sIgA) antibodies. The SIM route also led to Ags-specific T-cell responses and increased IFN-γ, IL-2, TNF-α and IL-17A in the splenocyte supernatants. Following respiratory infection with C. psittaci, we found that SIM immunization remarkably reduced bacterial load and the degree of inflammation in the infected lungs and made for a lower level of IFN-γ, TNF-α and IL-6. Furthermore, SIM vaccination with CNPs-Ags had obviously inhibited C. psittaci disseminating to various organs in vivo.Conclusion: SIM immunization with CNPs-adjuvanted C. psittaci Ags may present a novel strategy for the development of a vaccine against the C. psittaci infection.Keywords: Chlamydia psittaci, vaccine, chitosan nanoparticles, immunization route, respiratory infection

Published

2019

10. A new candidate vaccine for human brucellosis based on influenza viral vectors: a preliminary investigation for the development of an immunization schedule in a guinea pig model.

Author

Bugybayeva, Dina, Kydyrbayev, Zhailaubay, Zinina, Nadezhda, Assanzhanova, Nurika, Yespembetov, Bolat, Kozhamkulov, Yerken, Zakarya, Kunsulu, Ryskeldinova, Sholpan, and Tabynov, Kaissar

Subjects

*GENETIC vectors, *GUINEA pigs, *BRUCELLOSIS, *INFLUENZA, *IMMUNIZATION

Abstract

Background: A new candidate vector vaccine against human brucellosis based on recombinant influenza viral vectors (rIVV) subtypes H5N1 expressing Brucella outer membrane protein (Omp) 16, L7/L12, Omp19 or Cu–Zn SOD proteins has been developed. This paper presents the results of the study of protection of the vaccine using on guinea pigs, including various options of administering, dose and frequency. Provided data of the novel vaccine candidate will contribute to its further movement into the preclinical stage study. Methods: General states of guinea pigs was assessed based on behavior and dynamics of a guinea pig weight-gain test. The effectiveness of the new anti-brucellosis vector vaccine was determined by studying its protective effect after conjunctival, intranasal and sublingual administration in doses 105 EID50, 106 EID50 and 107 EID50 during prime and boost vaccinations of animals, followed by challenge with a virulent strain of B. melitensis 16 M infection. For sake of comparison, the commercial B. melitensis Rev.1 vaccine was used as a control. The protective properties of vaccines were assessed by quantitation of Brucella colonization in organs and tissues of infected animals and compared to the control groups. Results: It was observed a gradual increase in body weight of guinea pigs after prime and booster immunization with the vaccine using conjunctival, intranasal and sublingual routes of administration, as well as after using various doses of vaccine. The most optimal way of using the vaccine has been established: double intranasal immunization of guinea pigs at a dose of 106 EID50, which provides 80% protection of guinea pigs from B. melitensis 16 M infection (P < 0.05), which is comparable to the results of the effectiveness of the commercial B. melitensis Rev.1 vaccine. Conclusions: We developed effective human vaccine candidate against brucellosis and developed its immunization protocol in guinea pig model. We believe that because of these studies, the proposed vaccine has achieved the best level of protection, which in turn provides a basis for its further promotion. [ABSTRACT FROM AUTHOR]

Published

2021

11. Immunological characteristics of Mycobacterium tuberculosis subunit vaccines immunized through different routes.

Author

Lu, Yanzhi, Kang, Jian, Ning, Huanhuan, Wang, Lifei, Xu, Yanhui, Xue, Ying, Xu, Zhikai, Wu, Xingan, and Bai, Yinlan

Subjects

*MYCOBACTERIUM tuberculosis, *IMMUNIZATION, *ANTIGENS, *COMMUNICABLE diseases, *IMMUNE response, *TUBERCULOSIS

Abstract

Abstract Tuberculosis is chronic infectious disease caused by Mycobacterium tuberculosis (M.tb) that is prevalent worldwide. Several specific antigens, such as Antigen 85B (Ag85B) and 6 kDa early secretory antigenic target (ESAT-6) protein of M.tb , are listed as some of the candidate subunit vaccines against M.tb. ESAT-6, as a virulent factor and differential gene in M.tb , shows insufficient immunogenicity in animal model. In order to investigate the ways to improve the immunogenicity of ESAT-6, we immunized ESAT-6 by subcutaneous and intramuscular routes with different adjuvants. We found that ESAT-6 immunized alone did not induce significant humoral immunity in both immunization routes. However, subcutaneous immunization of ESAT-6 plus incomplete Freund's adjuvant can induce a significant humoral immune response, enhanced proliferation and elevated secretion of IFN-γ from splenocytes. Intramuscular immunization of ESAT-6 plus adjuvant aluminum salt or poly(I:C) did not enhance humoral and cellular immune responses. Therefore, it is concluded that immunization of ESAT-6 subcutaneously plus incomplete Freund's adjuvant induces stronger humoral and cellular immune responses, which can be considered of ESAT-6 as a subunit vaccine in further research against tuberculosis. Highlights • ESAT-6 plus adjuvant immunized subcutaneously induces strong humoral immunity. • ESAT-6 plus adjuvant immunized subcutaneously induces strong cellular immunity. • Subcutaneous immunization of ESAT-6 is considered better than intramuscular route. [ABSTRACT FROM AUTHOR]

Published

2018

12. COMPARATIVE STUDY OF IMMUNOGENICITY AND PROTECTIVE EFFECT OF LIVE COLD-ADAPTED AND INACTIVATED VACCINES AGAINST TYPE A INFLUENZA

Author

O. S Kashirina, M. I Chernikova, and Yu. M Vasiliev

Subjects

influenza, inactivated vaccines, attenuated vaccines, cold-adapted vaccines, immunization route, immunogenicity, protective effect, Microbiology, QR1-502

Abstract

Aim. Direct comparative studies of immunogenicity and protective effect of live cold-adapted (ca) and inactivated vaccines against type A influenza. Materials and methods. Groups of mice were immunized intramuscularly (i/m) or intranasally (i/n) twice with inactivated or live ca vaccines based on wild-type parent strain A/Krasnodar/101/59 (H2N2) and the corresponding ca donor strain А/Krasnodar/101/59/30CE/5MDCK/1/7/4 (H2N2), respectively. Immunogenicity was determined by HAI antibodies in sera and lungs (extracts) against both vaccine strains. Protective effect - by the level of wild-type strain in lungs of immunized mice after the infection. Results. Live ca and inactivated vaccines based on similar strains increase immunogenicity and protective effect when administered via different routes in varying patterns. A significant increase of immunogenicity was only observed for i/m (sera antibodies) and i/n (lung antibodies) administration of the live ca vaccine, and could be determined by antigenic features of the vaccine strains. At the same time, all the vaccine variants and administration routes induced at least partial protection from infection compared with unimmunized control. However, complete protection from infection was only noted for the i/m administered live ca vaccine. Conclusion. A combination of immunization variant and vaccine type determines immunogenicity and protective effect, and their interconnection requires further studies using all the possible combinations ofpreparations and administration routes as well as determination of induction of various components of the immune system.

Published

2015

13. Perception and willingness toward various immunization routes for COVID-19 vaccines: a cross-sectional survey in China.

Author

Wang H, Cui M, Li S, Wu F, Jiang S, Chen H, Yuan J, and Sun C

Subjects

Humans, Cross-Sectional Studies, Nasal Sprays, Vaccination, Immunization, China, Perception, COVID-19 Vaccines, COVID-19 prevention & control

Abstract

Background: To date, most vaccines, including the COVID-19 vaccine, are mainly administered by intramuscular injection, which might lead to vaccine hesitancy in some populations due to needle fear. Alternatively, needle-free immunization technology is extensively developed to improve the efficacy and acceptance of vaccination. However, there is no study to report the perception and willingness toward various immunization routes of the COVID-19 vaccine in the general population., Methods: A cross-sectional survey was conducted nationwide using an online questionnaire. Bivariate analyses were undertaken to assess variable associations among the participants who reported a hesitancy to receive the COVID-19 booster vaccination. Multivariable logistic regression with a backward step-wise approach was used to analyze the predicted factors associated with the willingness to receive the COVID-19 booster vaccination., Results: A total of 3,244 valid respondents were included in this survey, and 63.2% of participants thought they had a good understanding of intramuscular injection, but only 20.7, 9.2, 9.4, and 6.0% of participants had a self-perceived good understanding of inhalation vaccine, nasal spray vaccine, oral vaccine, and microneedle patch vaccine. Correspondingly, there was high acceptance for intramuscular injection (76.5%), followed by oral inhalation (64.4%) and nasal spray (43.0%). Those participants who were only willing to receive an intramuscular vaccine had less vaccine knowledge (OR = 0.78; 95% CI: 0.65-0.94) than those who were willing to receive a needle-free vaccine (OR = 1.97; 95% CI: 1.52-2.57). Some factors were found to be associated with vaccine hesitancy toward booster COVID-19 vaccination., Conclusion: Needle-free vaccination is a promising technology for the next generation of vaccines, but we found that intramuscular injection was still the most acceptable immunization route in this survey. One major reason might be that most people lack knowledge about needle-free vaccination. We should strengthen the publicity of needle-free vaccination technology, and thus improve the acceptance and coverage of vaccination in different populations., Competing Interests: The 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 © 2023 Wang, Cui, Li, Wu, Jiang, Chen, Yuan and Sun.)

Published

2023

14. A new candidate vaccine for human brucellosis based on influenza viral vectors: a preliminary investigation for the development of an immunization schedule in a guinea pig model

Author

Sholpan Ryskeldinova, Zhailaubay Kydyrbayev, Dina Bugybayeva, Kaissar Tabynov, Yerken Kozhamkulov, Bolat Yespembetov, Nurika Assanzhanova, Nadezhda Zinina, and Kunsulu Zakarya

Subjects

0301 basic medicine, Brucella Vaccine, Administration, Ophthalmic, medicine.disease_cause, Protection, biology, lcsh:Public aspects of medicine, General Medicine, Vector vaccine, Vaccination, Infectious Diseases, Vaccination dose, Female, Research Article, Bacterial Outer Membrane Proteins, Vaccine candidate, 030106 microbiology, Genetic Vectors, Administration, Sublingual, Immunization, Secondary, Brucella, Brucellosis, Viral vector, lcsh:Infectious and parasitic diseases, Guinea pig, 03 medical and health sciences, medicine, Brucella melitensis, Animals, Humans, lcsh:RC109-216, Influenza viral vectors, Administration, Intranasal, Dose-Response Relationship, Drug, Influenza A Virus, H5N1 Subtype, Human brucellosis, business.industry, Body Weight, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, biology.organism_classification, Virology, Influenza A virus subtype H5N1, Immunization route, Disease Models, Animal, 030104 developmental biology, Immunization, Guinea pigs, Nasal administration, business

Abstract

Background A new candidate vector vaccine against human brucellosis based on recombinant influenza viral vectors (rIVV) subtypes H5N1 expressing Brucella outer membrane protein (Omp) 16, L7/L12, Omp19 or Cu–Zn SOD proteins has been developed. This paper presents the results of the study of protection of the vaccine using on guinea pigs, including various options of administering, dose and frequency. Provided data of the novel vaccine candidate will contribute to its further movement into the preclinical stage study. Methods General states of guinea pigs was assessed based on behavior and dynamics of a guinea pig weight-gain test. The effectiveness of the new anti-brucellosis vector vaccine was determined by studying its protective effect after conjunctival, intranasal and sublingual administration in doses 105 EID50, 106 EID50 and 107 EID50 during prime and boost vaccinations of animals, followed by challenge with a virulent strain of B. melitensis 16 M infection. For sake of comparison, the commercial B. melitensis Rev.1 vaccine was used as a control. The protective properties of vaccines were assessed by quantitation of Brucella colonization in organs and tissues of infected animals and compared to the control groups. Results It was observed a gradual increase in body weight of guinea pigs after prime and booster immunization with the vaccine using conjunctival, intranasal and sublingual routes of administration, as well as after using various doses of vaccine. The most optimal way of using the vaccine has been established: double intranasal immunization of guinea pigs at a dose of 106 EID50, which provides 80% protection of guinea pigs from B. melitensis 16 M infection (P B. melitensis Rev.1 vaccine. Conclusions We developed effective human vaccine candidate against brucellosis and developed its immunization protocol in guinea pig model. We believe that because of these studies, the proposed vaccine has achieved the best level of protection, which in turn provides a basis for its further promotion.

Published

2021

15. A Proposed Immunoassay for T-2 Toxin

Author

O’Rear, Charles E., Lappas, Nicholas T., Dashek, William V., Llewellyn, Gerald C., Llewellyn, Gerald C., editor, and O’Rear, Charles E., editor

Published

1990

16. Subunit vaccines for Acinetobacter baumannii .

Author

Yang N, Jin X, Zhu C, Gao F, Weng Z, Du X, and Feng G

Subjects

Immunization methods, Vaccination methods, Adjuvants, Immunologic pharmacology, Vaccines, Subunit pharmacology, Acinetobacter baumannii

Abstract

Acinetobacter baumannii is a gram-negative bacterium and a crucial opportunistic pathogen in hospitals. A. baumannii infection has become a challenging problem in clinical practice due to the increasing number of multidrug-resistant strains and their prevalence worldwide. Vaccines are effective tools to prevent and control A. baumannii infection. Many researchers are studying subunit vaccines against A. baumannii . Subunit vaccines have the advantages of high purity, safety, and stability, ease of production, and highly targeted induced immune responses. To date, no A. baumannii subunit vaccine candidate has entered clinical trials. This may be related to the easy degradation of subunit vaccines in vivo and weak immunogenicity. Using adjuvants or delivery vehicles to prepare subunit vaccines can slow down degradation and improve immunogenicity. The common immunization routes include intramuscular injection, subcutaneous injection, intraperitoneal injection and mucosal vaccination. The appropriate immunization method can also enhance the immune effect of subunit vaccines. Therefore, selecting an appropriate adjuvant and immunization method is essential for subunit vaccine research. This review summarizes the past exploration of A. baumannii subunit vaccines, hoping to guide current and future research on these vaccines., Competing Interests: The 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 © 2023 Yang, Jin, Zhu, Gao, Weng, Du and Feng.)

Published

2023

17. Flower-like mesoporous silica nanoparticles as an antigen delivery platform to promote systemic immune response.

Author

Hou, Fengping, Teng, Zhidong, Ru, Jiaxi, Liu, Haiyun, Li, Jiajun, Zhang, Yun, Sun, Shiqi, and Guo, Huichen

Subjects

SILICA nanoparticles, MESOPOROUS silica, IMMUNE response, HUMORAL immunity, VIRUS-like particles

Abstract

Virus-like particles (VLPs), a kind of superior subunit vaccine, are assembled from the viral structural proteins with similar capsids to viruses. However, the efficiency of cell uptake is not satisfactory. We prepared flower-like mesoporous silica nanoparticles (SiNPs) with large pore channels and interior cavities to solve the problem. The highly loaded VLPs-SiNPs composites not only enhanced the stability of VLPs, but also delivered antigen to cells and improved the cellular uptake efficiency. Compared with naked VLPs, mice intramuscularly immunized with the VLPs-SiNPs composite induced higher specific antibodies, greater lymphocyte activation and higher level of cytokine secretion. Moreover, the VLPs-SiNPs composite as vaccine also promoted mucosal immune response through intranasal immune pathway. Therefore, the VLPs-SiNPs enable to induce strong cellular, humoral, and slight mucosal immune response through different immunization routes. These results are potentially useful for vaccine formulations and may provide further reference for vaccine design and delivery systems. Silica nanoparticles loaded with antigen virus-like-particles (VLPs) improved the cellular uptake of antigen, and even enhanced the thermostability and acid-resistance. The vaccine formulation was immunized to mice with different immune routes, intramuscular injection and intranasal immunization. Both immune routes promote immune response; however, the intramuscular injection shows better cellular immune response and humoral immune response. [Display omitted] • Flower-like mesoporous silicon nanoparticles (SiNPs) with large pore channels and interior cavities were prepared. • The highly loaded VLPs-SiNPs can enhance the resistance to acid and thermo. • The SiNPs help deliver antigen to cells and improve cellular uptake of VLPs. • The SiNPs also played a role of adjuvants which can stimulate organisms to enhance immune response through different immune routes. [ABSTRACT FROM AUTHOR]

Published

2022

18. Flower-like mesoporous silica nanoparticles as an antigen delivery platform to promote systemic immune response.

Author

Hou F, Teng Z, Ru J, Liu H, Li J, Zhang Y, Sun S, and Guo H

Subjects

Animals, Antibodies, Viral, Immunity, Mucosal, Immunization methods, Mice, Silicon Dioxide, Nanoparticles, Vaccines, Virus-Like Particle

Abstract

Virus-like particles (VLPs), a kind of superior subunit vaccine, are assembled from the viral structural proteins with similar capsids to viruses. However, the efficiency of cell uptake is not satisfactory. We prepared flower-like mesoporous silica nanoparticles (SiNPs) with large pore channels and interior cavities to solve the problem. The highly loaded VLPs-SiNPs composites not only enhanced the stability of VLPs, but also delivered antigen to cells and improved the cellular uptake efficiency. Compared with naked VLPs, mice intramuscularly immunized with the VLPs-SiNPs composite induced higher specific antibodies, greater lymphocyte activation and higher level of cytokine secretion. Moreover, the VLPs-SiNPs composite as vaccine also promoted mucosal immune response through intranasal immune pathway. Therefore, the VLPs-SiNPs enable to induce strong cellular, humoral, and slight mucosal immune response through different immunization routes. These results are potentially useful for vaccine formulations and may provide further reference for vaccine design and delivery systems., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

19. Development of Vaccine Delivery Vehicles Based on Lactic Acid Bacteria.

Author

Tarahomjoo, Shirin

Abstract

Live recombinant bacteria represent attractive antigen delivery systems able to induce both mucosal and systemic immune responses against heterologous antigens. The first live recombinant bacterial vectors developed were derived from attenuated pathogenic microorganisms. In addition to the difficulties often encountered in the construction of stable attenuated mutants of pathogenic organisms, attenuated pathogens may retain a residual virulence level that renders them unsuitable for the vaccination of partially immunocompetent individuals such as infants, the elderly or immunocompromised patients. As an alternative to this strategy, non-pathogenic food-grade lactic acid bacteria (LAB) maybe used as live antigen carriers. This article reviews LAB vaccines constructed using antigens other than tetanus toxin fragment C, against bacterial, viral, and parasitic infective agents, for which protection studies have been performed. The antigens utilized for the development of LAB vaccines are briefly described, along with the efficiency of these systems in protection studies. Moreover, the key factors affecting the performance of these systems are highlighted. [ABSTRACT FROM AUTHOR]

Published

2012

20. The route of immunization with adenoviral vaccine influences the recruitment of cytotoxic T lymphocytes in the lung that provide potent protection from influenza A virus

Author

Suda, Tatsuya, Kawano, Masaaki, Nogi, Yasuhisa, Ohno, Naohito, Akatsuka, Toshitaka, and Matsui, Masanori

Subjects

*IMMUNIZATION, *ADENOVIRUSES, *VIRAL vaccines, *T cells, *LUNG diseases, *INFLUENZA A virus, *RESPIRATORY infections, *LABORATORY mice

Abstract

Abstract: Virus-specific cytotoxic T lymphocytes (CTLs) in the lung are considered to confer protection from respiratory viruses. Several groups demonstrated that the route of priming was likely to have an implication for the trafficking of antigen-specific CTLs. Therefore, we investigated whether the route of immunization with adenoviral vaccine influenced the recruitment of virus-specific CTLs in the lung that should provide potent protection from influenza A virus. Mice were immunized with recombinant adenovirus expressing the matrix (M1) protein of influenza A virus via various immunization routes involving intraperitoneal, intranasal, intramuscular, or intravenous administration as well as subcutaneous administration in the hind hock. We found that the immunization route dramatically impacted the recruitment of M1-specific IFN-γ+ CD8+ T cells both in the lung and the spleen. Surprisingly, hock immunization was most effective for the accumulation in the lung of IFN-γ-producing CD8+ T cells that possessed M1-specific cytolytic activity. Further, antigen-driven IFN-γ+ CD8+ T cells in the lung, but not in the spleen, were likely to be correlated with the resistance to challenge with influenza A virus. These results may improve our ability to design vaccines that target virus-specific CTL responses to respiratory viruses such as influenza A virus. [Copyright &y& Elsevier]

Published

2011

21. Enhanced immune response induced by BSA loaded in hydroxyethylstarch microparticles

Author

Balasse, Emilie, Odot, Johann, Gatouillat, Gregory, Andry, Marie-Christine, and Madoulet, Claudie

Subjects

*IMMUNE response, *DNA, *NANOPARTICLES, *PEPTIDES

Abstract

Abstract: Microparticles and nanoparticles represent promising carriers for the in vivo delivery of peptides, proteins or deoxyribonucleic acid (DNA). In this study, new hydroxyethylstarch (HES) microparticles were obtained by interfacial cross-linking with terephtaloyl chloride. These microparticles exhibit the characteristics required to improve antigen release and presentation to antigen presentating cells compared to free antigens. The adjuvant activity of HES microparticles as vaccine carrier was investigated in mice using bovine serum albumin (BSA) as model antigen. We showed HES microparticles were phagocyted by peritoneal mononuclear cells. The immunization with BSA-microparticles induced antibody synthesis that was predominantly immunoglobulin G1 (IgG1). Aluminium hydroxide remained more efficient to induce IgG synthesis. The analysis of the cytokine profile from spleen cells revealed that BSA-microparticles induced the secretion of both interferon-γ (IFN-γ) and interleukin-4 (IL-4). However, the immune responses induced by BSA-microparticles were qualitatively and quantitatively affected by the route of injection. Taken together, these results demonstrate that HES microparticles induce a mixed T helper 1/T helper 2 response against BSA and may be a suitable delivery and presentation system in the field of vaccine development. [Copyright &y& Elsevier]

Published

2008

22. Characteristics of the Protective Subcellular Coccidioidal T27K Vaccine.

Author

JOHNSON, SUZANNE M., KEREKES, KATHLEEN M., LUNETTA, JENNINE M., and PAPPAGIANIS, DEMOSTHENES

Subjects

*VACCINE research, *COCCIDIOIDOMYCOSIS, *LABORATORY mice, *LABORATORY monkeys, *SYSTEMIC mycoses, *PREVENTIVE medicine, *DISEASES, *IMMUNITY, *AGING

Abstract

While the whole killed spherule vaccine, protective in mice and monkeys, did not prevent coccidioidal disease in humans, the 27K vaccine, a soluble derivative, retains protective activity in mice with little irritant action. Gel filtration and anion exchange fractions of thimerosal-inactivated spherules (T27K), when administered with alum adjuvant, also protect mice against lethal respiratory coccidioidal challenge. However, the superb protection afforded by T27K antigens is maintained for some 3 months, but may then diminish. This appears unrelated to the aging of the mice. Prolongation of the protective action may require addition of a different adjuvant or administration of booster doses of vaccine. [ABSTRACT FROM AUTHOR]

Published

2007

23. Immunogenicity of κ-Casein and Glycomacropeptide.

Author

Mikkelsen, T. L., Rasmussen, E., Olsen, A., Barkholt, V., and Frøkiær, H.

Subjects

*PEPTIDES, *CASEINS, *PEPSIN, *PATHOGENIC microorganisms, *ANIMAL models in research, *IMMUNIZATION, *T cells, *IMMUNOGENETICS

Abstract

Glycomacropeptide (GMP), arising from the cleavage of κ-casein by chymosin or pepsin, has been correlated with a wide variety of biological activities including immunosuppression capacity, inhibition of pathogen invasion, and induction of satiety. Due to the interest in exploiting such potential of GMP, we aimed at characterizing the immunogenic properties of GMP as an indication of its potential allergenicity. Immunogenicity of κ-casein and GMP were investigated using 2 animal models based on different routes of immunization: 1) mice immunized intraperitoneally or subcutaneously with either κ-casein, polymerized GMP, GMP coupled to the immunogenic carrier ovalbumin, or GMP alone; 2) mice coadministered κ-casein or GMP and cholera toxin. The specific antibody response to GMP was evaluated as well as the antigen-specific T-cell response. The results demonstrated that immunization or feeding with κ-casein induced GMP-specific antibodies, whereas GMP per se lacked immunogenicity independently of the mode of presentation. The size of the presented form of GMP did not influence its immunogenicity. Because the results showed that GMP did not induce a specific T-cell response, we postulate that GMP lacks the ability to stimulate antigen-specific T cells. [ABSTRACT FROM AUTHOR]

Published

2006

24. DNA immunization via intramuscular and intradermal routes using a gene gun provides different magnitudes and durations on immune response

Author

Ito, Koichi, Ito, Kyoko, Shinohara, Nobukata, and Kato, Seishi

Subjects

*ANTINEOPLASTIC antibiotics, *GREEN fluorescent protein

Abstract

We investigated the antibody (Ab) and cytotoxic T lymphocyte (CTL) responses to gene gun (GG)-mediated DNA immunization via the intramuscular (i.m.) and intradermal (i.d.) routes. BALB/c mice were immunized five times at weekly intervals with plasmid DNA encoding enhanced green fluorescent protein (EGFP). EGFP production was rapidly detected in the target tissues after injection via either delivery route. There were significant differences in the magnitude and duration of the Ab and CTL responses according to the route employed. Intradermal injection elicited higher Ab and CTL responses to EGFP than i.m. injection 1 week after the last immunization. However, both immune responses were reduced rapidly 5 weeks after the last immunization via i.d. injection. In contrast, in mice injected via the i.m. routes, Ab and CTL responses 5 weeks after the last immunization remained at levels similar to those detected after 1 week. All mice generated a predominantly IgG1 Ab response via either route. These findings suggest that a combination of these two routes of DNA immunization would provide optimal conditions for induction of a broad immune response, and this information is expected to be very important for future applications of DNA vaccination. [Copyright &y& Elsevier]

Published

2003

25. Simultaneous Intramuscular And Intranasal Administration Of Chitosan Nanoparticles-Adjuvanted

Author

Yumeng, Li, Chuan, Wang, Zhenjie, Sun, Jian, Xiao, Xiaoliang, Yan, Yuqing, Chen, Jian, Yu, and Yimou, Wu

Subjects

T-Lymphocytes, chitosan nanoparticles, Injections, Intramuscular, Adjuvants, Immunologic, immunization route, respiratory infection, vaccine, Animals, Particle Size, Immunity, Mucosal, Lung, Administration, Intranasal, Original Research, Antigens, Bacterial, Chitosan, Mice, Inbred BALB C, Vaccination, Chlamydia psittaci, Psittacosis, Immunity, Humoral, Chlamydophila psittaci, Immunoglobulin G, Bacterial Vaccines, bacteria, Cytokines, Nanoparticles, Female, Spleen

Abstract

Background Chlamydia psittaci is a zoonotic bacteria closely associated with psittacosis/ornithosis. Vaccination has been recognized as the best way to inhibit the spread of C. psittaci due to the majority ignored of infections. The optimal Chlamydia vaccine was obstructed by the defect of single immunization route and the lack of availability of nontoxic and valid adjuvants. Methods In this study, we developed a novel immunization strategy, simultaneous (SIM) intramuscular (IM) and intranasal (IN) administration of a C. psittaci antigens (Ags) adjuvanted with chitosan nanoparticles (CNPs). And SIM-CNPs-Ags were used to determine the different types of immune response and the protective role in vivo. Results CNPs-Ags with zeta-potential values of 13.12 mV and of 276.1 nm showed excellent stability and optimal size for crossing the mucosal barrier with high 71.7% encapsulation efficiency. SIM-CPN-Ags mediated stronger humoral and mucosal responses by producing meaningfully high levels of IgG and secretory IgA (sIgA) antibodies. The SIM route also led to Ags-specific T-cell responses and increased IFN-γ, IL-2, TNF-α and IL-17A in the splenocyte supernatants. Following respiratory infection with C. psittaci, we found that SIM immunization remarkably reduced bacterial load and the degree of inflammation in the infected lungs and made for a lower level of IFN-γ, TNF-α and IL-6. Furthermore, SIM vaccination with CNPs-Ags had obviously inhibited C. psittaci disseminating to various organs in vivo. Conclusion SIM immunization with CNPs-adjuvanted C. psittaci Ags may present a novel strategy for the development of a vaccine against the C. psittaci infection.

Published

2019

26. Adjuvanted vaccines: Aspects of immunosafety and modes of action

Author

van Aalst, S. and van Aalst, S.

Abstract

New developments in vaccine design shift towards safe, though sometimes less immunogenic, subunit and synthetic antigens. Therefore, the majority of current vaccines require adjuvants to increase immunogenicity. Most adjuvants available were developed empirically and their mode of action is only partly elucidated. Earlier work shows that adjuvants exert their effect mainly on the innate immune system. To improve vaccines, more knowledge on adjuvants’ modes of action and their effect on innate immune responses at the site of application are required. Furthermore, immune responses that take place after vaccination are sometimes linked with the development or exacerbation of autoimmune diseases (AID). It is highly debated íf vaccines indeed induce or aggravate AID and in particular adjuvants are mentioned as potential cause. Since vaccines are given on a large scale, more research is warranted. The aim of this thesis was to study working mechanisms of vaccines and adjuvants locally (innate immune system) as well as systemically (adaptive immune system) to identify possible risks on severe side effects of vaccination and potentially improve vaccine effectiveness. A panel of human and experimental adjuvants was tested in mice for their local effects and ability to initiate adaptive responses. Rapid but transient immune-stimulatory environments were induced by most adjuvants. Antigen-uptake and -presentation by APC and maturation of APC were differentially affected by distinct adjuvants. The choice of adjuvant determined the outcome of the initiated adaptive immune response and we showed that the route of administration of vaccines (intranasal or intradermal) also influences the response induced. Two potential mechanisms on how AID could result from vaccination were explored; (1) bystander activation and (2) disturbances in regulatory T cells (Treg). During bystander activation, T cells unrelated to the antigen presented can be activated without (strong) T cell

Published

2017

27. Adjuvanted vaccines: Aspects of immunosafety and modes of action

Subjects

safety, Treg, intramuscular, adjuvant, bystander activation, immunization route, intranasal, intradermal, Vaccine

Abstract

New developments in vaccine design shift towards safe, though sometimes less immunogenic, subunit and synthetic antigens. Therefore, the majority of current vaccines require adjuvants to increase immunogenicity. Most adjuvants available were developed empirically and their mode of action is only partly elucidated. Earlier work shows that adjuvants exert their effect mainly on the innate immune system. To improve vaccines, more knowledge on adjuvants’ modes of action and their effect on innate immune responses at the site of application are required. Furthermore, immune responses that take place after vaccination are sometimes linked with the development or exacerbation of autoimmune diseases (AID). It is highly debated íf vaccines indeed induce or aggravate AID and in particular adjuvants are mentioned as potential cause. Since vaccines are given on a large scale, more research is warranted. The aim of this thesis was to study working mechanisms of vaccines and adjuvants locally (innate immune system) as well as systemically (adaptive immune system) to identify possible risks on severe side effects of vaccination and potentially improve vaccine effectiveness. A panel of human and experimental adjuvants was tested in mice for their local effects and ability to initiate adaptive responses. Rapid but transient immune-stimulatory environments were induced by most adjuvants. Antigen-uptake and -presentation by APC and maturation of APC were differentially affected by distinct adjuvants. The choice of adjuvant determined the outcome of the initiated adaptive immune response and we showed that the route of administration of vaccines (intranasal or intradermal) also influences the response induced. Two potential mechanisms on how AID could result from vaccination were explored; (1) bystander activation and (2) disturbances in regulatory T cells (Treg). During bystander activation, T cells unrelated to the antigen presented can be activated without (strong) T cell receptor (TCR) ligation, but via signals derived from the ongoing response directed against the vaccine-antigen or adjuvant at hand. Our study demonstrated that for a model vaccine (comprising the unsafe adjuvant Complete Freund’s adjuvant) not the adjuvant, but the vaccine-antigen likely induced limited bystander responses. No evidence was obtained that adjuvation of antigen specific responses is essential for bystander activation. Regulatory T cells (Treg) function in the prevention of excessive inflammation and maintenance of immunological homeostasis. However, these cells may also interfere with resolution of infections or with immune reactions following vaccination. Effects of Treg on vaccine responses are nowadays investigated, but the impact of vaccination on Treg homeostasis is still largely unknown. This may be a relevant safety aspect, since loss of tolerance through reduced Treg may trigger autoimmunity. Both in men and mice, safe vaccines were shown to have only minimal impact on Treg frequencies and characteristics and even an unsafe stimulus (CFA) did not result in significant (long term) effects on Treg of mice. More knowledge on adjuvants, both their modes of action and aspects of immunosafety, will aid in the development of new, improved and safe(r) vaccines that will provide good protection against infectious diseases without any unnecessary side effects.

Published

2017

28. Development of Vaccine Delivery Vehicles Based on Lactic Acid Bacteria

Author

Shirin Tarahomjoo

Subjects

Vaccine delivery, Virulence, Reviews, Bioengineering, Live vaccine, Applied Microbiology and Biotechnology, Biochemistry, law.invention, Microbiology, Mice, Immune system, Drug Delivery Systems, Antigen, law, Lactobacillales, Lactic acid bacteria, Animals, Humans, Antigens, Molecular Biology, Vaccines, Attenuated vaccine, biology, biology.organism_classification, Virology, Vaccination, Immunization route, Recombinant DNA, Bacteria, Biotechnology

Abstract

Live recombinant bacteria represent attractive antigen delivery systems able to induce both mucosal and systemic immune responses against heterologous antigens. The first live recombinant bacterial vectors developed were derived from attenuated pathogenic microorganisms. In addition to the difficulties often encountered in the construction of stable attenuated mutants of pathogenic organisms, attenuated pathogens may retain a residual virulence level that renders them unsuitable for the vaccination of partially immunocompetent individuals such as infants, the elderly or immunocompromised patients. As an alternative to this strategy, non-pathogenic food-grade lactic acid bacteria (LAB) maybe used as live antigen carriers. This article reviews LAB vaccines constructed using antigens other than tetanus toxin fragment C, against bacterial, viral, and parasitic infective agents, for which protection studies have been performed. The antigens utilized for the development of LAB vaccines are briefly described, along with the efficiency of these systems in protection studies. Moreover, the key factors affecting the performance of these systems are highlighted.

Published

2011

29. Recombinant Semliki Forest virus vaccine vectors: the route of injection determines the localization of vector RNA and subsequent T cell response

Author

Colmenero, P, Berglund, P, Kambayashi, T, Biberfeld, P, Liljeström, P, and Jondal, M

Published

2001

30. Immunization of hamsters against Clostridium difficile infection usingthe Cwp84 protease as an antigen

Author

Anne Collignon, Sandra Hoys, Alban Le Monnier, Claire Janoir, Cécile Denève, Séverine Péchiné, Écosystème Microbien Digestif et Santé, and Institut National de la Recherche Agronomique (INRA)-Université Paris-Sud - Paris 11 (UP11)

Subjects

Male, animal diseases, [SDV]Life Sciences [q-bio], STREPTOCOCCUS-PNEUMONIAE, VACCINE, immunization route, Cricetinae, BINDING, Immunology and Allergy, 0303 health sciences, biology, SURFACE-LAYER PROTEINS, Proteolytic enzymes, General Medicine, ANTIBODY-RESPONSE, Clostridium difficile, Antibodies, Bacterial, 3. Good health, Cysteine Endopeptidases, Infectious Diseases, Bacterial Vaccines, Cwp84, Antibody, Microbiology (medical), EXTRACELLULAR-MATRIX PROTEINS, Injections, Subcutaneous, Immunology, Hamster, chemical and pharmacologic phenomena, IMMUNE-RESPONSE, Microbiology, 03 medical and health sciences, Immune system, Antigen, PASSIVE-IMMUNIZATION, Administration, Rectal, medicine, hamster model, Animals, Colitis, Gastric Lavage, 030304 developmental biology, Antigens, Bacterial, 030306 microbiology, Clostridioides difficile, STRAINS, biochemical phenomena, metabolism, and nutrition, medicine.disease, Survival Analysis, DIARRHEA, Gastrointestinal Tract, Disease Models, Animal, Immunization, biology.protein, Clostridium Infections, bacteria

Abstract

Clostridium difficile is a pathogen responsible for diarrhoea and colitis, particularly after antibiotic treatment. We evaluated the C. difficile protease Cwp84, found to be associated with the S-layer proteins, as a vaccine antigen to limit the C. difficile intestinal colonization and therefore the development of the infection in a clindamycin-treated hamster model. First, we evaluated the immune response and the animal protection against death induced by several immunization routes: rectal, intragastric and subcutaneous. Antibody production was variable according to the immunization routes. In addition, serum Cwp84 antibody titres did not always correlate with animal protection after challenge with a toxigenic C. difficile strain. The best survival rate was observed with the rectal route of immunization. Then, in a second assay, we selected this immunization route to perform a larger immunization assay including a Cwp84 immunized group and a control group. Clostridium difficile intestinal colonization and survival rate, as well as the immune response were examined. Clostridium difficile hamster challenge resulted in a 26% weaker and slower C. difficile intestinal colonization in the immunized group. Furthermore, hamster survival in the Cwp84 immunized group was 33% greater than that of the control group, with a significant statistical difference.

Published

2011

31. Relevance of a pre-existing measles immunity prior immunization with a recombinant measles virus vector.

Author

Knuchel MC, Marty RR, Morin TN, Ilter O, Zuniga A, and Naim HY

Subjects

Administration, Intranasal, Animals, Antibodies, Neutralizing administration & dosage, Antibodies, Viral administration & dosage, Humans, Immunity, Cellular, Injections, Intramuscular, Measles virus genetics, Mice, Vaccines, Synthetic administration & dosage, Vaccines, Synthetic genetics, Vaccines, Synthetic immunology, Viral Vaccines administration & dosage, Viral Vaccines genetics, Antibodies, Viral blood, Drug Carriers, Genetic Vectors immunology, Immunization methods, Measles immunology, Measles virus immunology, Viral Vaccines immunology

Abstract

Measles virus (MV) vectors are promising candidates for designing new recombinant vaccines since the parental live vaccines have a well-known safety and efficacy record. Like all viral vectors, the MV vector efficacy in inducing a protecting immune answer could be affected by the pre-existing immunity among the human population. In order to determine the optimal immunization route and regimen, we mimicked a MV pre-immunity by passively administrating MV neutralizing antibodies (MV-nAb) prior intramuscular (i.m.) and/or intranasal (i.n.) immunization with recombinant MV expressing the SIV-gag antigen (rMV-SIVgag). Our results revealed that 500 mIU of MV-nAb allowed the induction of a humoral and cellular immune response against the vector and the transgene, while higher titers of the MV-nAb were significantly inhibitory. In a prime-boost regimen, in the presence of MV-nAb, the intranasal-intramuscular (i.n.-i.m.) or intramuscular-intramuscular (i.m.-i.m.) routes induced higher humoral immune responses against the vector and the transgene (SIV-gag). In naive animals, cellular immune response was significantly higher by i.m. immunization; however, MV pre-immunity did not seem to affect the cellular immune response after an i.n. immunization.   In summary, we show that a pre-existing immunity of up to 500 mIU anti-MV neutralizing antibodies had little effect on the replication of rMV and did not inhibit the induction of significant humoral and cellular immune responses in immune-competent mice.

Published

2013