Kunitz-type protease inhibitor as a vaccine candidate against schistosomiasis mansoni
[Display omitted] •The vaccination of mice with rSmKI-1 resulted in reduced numbers of parasites and eggs.•The rSmKI-1 vaccine produced a solid IgG response, with the IgG1 isotype being predominant.•The rSmKI-1 vaccine down-regulated the Th2 immune response, reducing disease pathology.•SmKI-1 has po...
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Published in | International journal of infectious diseases Vol. 66; no. C; pp. 26 - 32 |
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Main Authors | , , , |
Format | Journal Article |
Language | English |
Published |
Canada
Elsevier Ltd
01.01.2018
Elsevier |
Subjects | |
Online Access | Get full text |
ISSN | 1201-9712 1878-3511 1878-3511 |
DOI | 10.1016/j.ijid.2017.10.024 |
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Abstract | [Display omitted]
•The vaccination of mice with rSmKI-1 resulted in reduced numbers of parasites and eggs.•The rSmKI-1 vaccine produced a solid IgG response, with the IgG1 isotype being predominant.•The rSmKI-1 vaccine down-regulated the Th2 immune response, reducing disease pathology.•SmKI-1 has potential for development as part of a schistosomiasis cocktail vaccine.
The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome parasite.
SmKI-1 is a 16-kDa Kunitz-type protease inhibitor present in the excretory–secretory products and tegument of adult worms and eggs of Schistosoma mansoni. Two independent vaccine trials were performed in mice to determine the efficacy of rSmKI-1 in developing protective immunity.
The results obtained showed reductions of 23–33% in adult worms, 28–31% in intestinal eggs, 33–39% in faecal eggs, and 20–43% in liver eggs. Furthermore, rSmKI-1 significantly increased the production of interferon gamma, interleukin (IL)-10, and IL-6 in vaccinated mice, maintaining a Th1/Th2-type balanced protective response.
rSmKI-1 generated partial protection against schistosomiasis mansoni in the murine model of infection and could be developed as part of a combination vaccine with other vaccine candidates to provide an even more solid level of protection. |
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AbstractList | The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome parasite.OBJECTIVEThe aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome parasite.SmKI-1 is a 16-kDa Kunitz-type protease inhibitor present in the excretory-secretory products and tegument of adult worms and eggs of Schistosoma mansoni. Two independent vaccine trials were performed in mice to determine the efficacy of rSmKI-1 in developing protective immunity.METHODSSmKI-1 is a 16-kDa Kunitz-type protease inhibitor present in the excretory-secretory products and tegument of adult worms and eggs of Schistosoma mansoni. Two independent vaccine trials were performed in mice to determine the efficacy of rSmKI-1 in developing protective immunity.The results obtained showed reductions of 23-33% in adult worms, 28-31% in intestinal eggs, 33-39% in faecal eggs, and 20-43% in liver eggs. Furthermore, rSmKI-1 significantly increased the production of interferon gamma, interleukin (IL)-10, and IL-6 in vaccinated mice, maintaining a Th1/Th2-type balanced protective response.RESULTSThe results obtained showed reductions of 23-33% in adult worms, 28-31% in intestinal eggs, 33-39% in faecal eggs, and 20-43% in liver eggs. Furthermore, rSmKI-1 significantly increased the production of interferon gamma, interleukin (IL)-10, and IL-6 in vaccinated mice, maintaining a Th1/Th2-type balanced protective response.rSmKI-1 generated partial protection against schistosomiasis mansoni in the murine model of infection and could be developed as part of a combination vaccine with other vaccine candidates to provide an even more solid level of protection.CONCLUSIONSrSmKI-1 generated partial protection against schistosomiasis mansoni in the murine model of infection and could be developed as part of a combination vaccine with other vaccine candidates to provide an even more solid level of protection. The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome parasite. SmKI-1 is a 16-kDa Kunitz-type protease inhibitor present in the excretory-secretory products and tegument of adult worms and eggs of Schistosoma mansoni. Two independent vaccine trials were performed in mice to determine the efficacy of rSmKI-1 in developing protective immunity. The results obtained showed reductions of 23-33% in adult worms, 28-31% in intestinal eggs, 33-39% in faecal eggs, and 20-43% in liver eggs. Furthermore, rSmKI-1 significantly increased the production of interferon gamma, interleukin (IL)-10, and IL-6 in vaccinated mice, maintaining a Th1/Th2-type balanced protective response. rSmKI-1 generated partial protection against schistosomiasis mansoni in the murine model of infection and could be developed as part of a combination vaccine with other vaccine candidates to provide an even more solid level of protection. Objective: The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome parasite. Methods: SmKI-1 is a 16-kDa Kunitz-type protease inhibitor present in the excretory–secretory products and tegument of adult worms and eggs of Schistosoma mansoni. Two independent vaccine trials were performed in mice to determine the efficacy of rSmKI-1 in developing protective immunity. Results: The results obtained showed reductions of 23–33% in adult worms, 28–31% in intestinal eggs, 33–39% in faecal eggs, and 20–43% in liver eggs. Furthermore, rSmKI-1 significantly increased the production of interferon gamma, interleukin (IL)-10, and IL-6 in vaccinated mice, maintaining a Th1/Th2-type balanced protective response. Conclusions: rSmKI-1 generated partial protection against schistosomiasis mansoni in the murine model of infection and could be developed as part of a combination vaccine with other vaccine candidates to provide an even more solid level of protection. [Display omitted] •The vaccination of mice with rSmKI-1 resulted in reduced numbers of parasites and eggs.•The rSmKI-1 vaccine produced a solid IgG response, with the IgG1 isotype being predominant.•The rSmKI-1 vaccine down-regulated the Th2 immune response, reducing disease pathology.•SmKI-1 has potential for development as part of a schistosomiasis cocktail vaccine. The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome parasite. SmKI-1 is a 16-kDa Kunitz-type protease inhibitor present in the excretory–secretory products and tegument of adult worms and eggs of Schistosoma mansoni. Two independent vaccine trials were performed in mice to determine the efficacy of rSmKI-1 in developing protective immunity. The results obtained showed reductions of 23–33% in adult worms, 28–31% in intestinal eggs, 33–39% in faecal eggs, and 20–43% in liver eggs. Furthermore, rSmKI-1 significantly increased the production of interferon gamma, interleukin (IL)-10, and IL-6 in vaccinated mice, maintaining a Th1/Th2-type balanced protective response. rSmKI-1 generated partial protection against schistosomiasis mansoni in the murine model of infection and could be developed as part of a combination vaccine with other vaccine candidates to provide an even more solid level of protection. |
Author | Duke, Mary McManus, Donald P. Harvie, Marina Ranasinghe, Shiwanthi L. |
Author_xml | – sequence: 1 givenname: Shiwanthi L. surname: Ranasinghe fullname: Ranasinghe, Shiwanthi L. email: shiwanthi.ranasinghe@qimrberghofer.edu.au – sequence: 2 givenname: Mary surname: Duke fullname: Duke, Mary – sequence: 3 givenname: Marina surname: Harvie fullname: Harvie, Marina – sequence: 4 givenname: Donald P. surname: McManus fullname: McManus, Donald P. |
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Keywords | Schistosomiasis mansoni SmKI-1 Kunitz protein ES products |
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•The vaccination of mice with rSmKI-1 resulted in reduced numbers of parasites and eggs.•The rSmKI-1 vaccine produced a solid IgG response,... The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative schistosome... Objective: The aim of this study was to develop a vaccine against schistosomiasis, which is a major challenge due to the complex lifecycle of the causative... |
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SubjectTerms | Animals Antigens, Helminth - immunology Egg Hypersensitivity ES products Female Interferon-gamma Interleukin-10 Interleukin-6 Kunitz protein Mice Mice, Inbred C57BL Mice, Inbred CBA Protease Inhibitors - immunology Schistosoma mansoni Schistosomiasis mansoni Schistosomiasis mansoni - immunology Schistosomiasis mansoni - prevention & control SmKI-1 Vaccines - immunology |
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Title | Kunitz-type protease inhibitor as a vaccine candidate against schistosomiasis mansoni |
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