Published January 29, 2013 | Version v1
Publication Open

Virus-like particles as nanovaccine candidates

Creators

  • 1. Centro de Ingeniería Genética y Biotecnología

Description

The existing vaccines are mainly limited to the microorganisms we are able to culture and produce and/or to those whose killing is mediated by humoral response (antibody mediated). It has been more difficult to develop vaccines capable of inducing a functional cellular response needed to prevent or cure chronic diseases. New strategies should be taken into account in the improvement of cell-based immune responses in order to prevent and control the infections and eventually clear the virus. Preclinical and clinical results with vaccine candidates developed as a vaccine platform based on virus-like particles (VLPs) evidenced their ability to stimulate mucosal as well as systemic immunity. Particles based on envelope, membrane or nucleocapsid microbial proteins induce a strong immune response after nasal or parenteral administration in mice, non-human primates and humans. In addition, the immune response obtained was modulated in a Th1 sense. The VLPs were also able to immunoenhance the humoral and cellular immune responses against several viral pathogens. Studies in animals and humans with nasal and systemic formulations evidenced that it is possible to induce functional immune response against HBV, HCV, HIV and dengue virus.

⚠️ This is an automatic machine translation with an accuracy of 90-95%

Translated Description (Arabic)

تقتصر اللقاحات الحالية بشكل أساسي على الكائنات الحية الدقيقة التي يمكننا استزراعها وإنتاجها و/أو أولئك الذين يتم التوسط في قتلهم عن طريق الاستجابة الخلطية (التوسط في الأجسام المضادة). كان من الصعب تطوير لقاحات قادرة على إحداث استجابة خلوية وظيفية ضرورية للوقاية من الأمراض المزمنة أو علاجها. يجب مراعاة الاستراتيجيات الجديدة في تحسين الاستجابات المناعية القائمة على الخلايا من أجل الوقاية من العدوى ومكافحتها والقضاء على الفيروس في نهاية المطاف. أثبتت النتائج قبل السريرية والسريرية مع اللقاحات المرشحة التي تم تطويرها كمنصة لقاح تعتمد على الجسيمات الشبيهة بالفيروس (VLPs) قدرتها على تحفيز المناعة المخاطية والجهازية. تحفز الجسيمات القائمة على البروتينات الميكروبية المغلفة أو الغشائية أو القفيصة النووية استجابة مناعية قوية بعد الإعطاء عن طريق الأنف أو الحقن في الفئران والرئيسيات غير البشرية والبشر. بالإضافة إلى ذلك، تم تعديل الاستجابة المناعية التي تم الحصول عليها بمعنى Th1. كما تمكن VLPs من تعزيز الاستجابات المناعية الخلطية والخلوية ضد العديد من مسببات الأمراض الفيروسية. أثبتت الدراسات التي أجريت على الحيوانات والبشر الذين لديهم تركيبات أنفية وجهازية أنه من الممكن إحداث استجابة مناعية وظيفية ضد فيروس التهاب الكبد الوبائي (HBV) وفيروس التهاب الكبد الوبائي (HCV) وفيروس نقص المناعة البشرية وفيروس حمى الضنك.

Translated Description (English)

The existing vaccines are mainly limited to the microorganisms we are able to culture and produce and/or to those whose killing is mediated by humoral response (antibody mediated). It has been more difficult to develop vaccines capable of inducing a functional cellular response needed to prevent or cure chronic diseases. New strategies should be taken into account in the improvement of cell-based immune responses in order to prevent and control infections and eventually clear the virus. Preclinical and clinical results with vaccine candidates developed as a vaccine platform based on virus-like particles (VLPs) evidenced their ability to stimulate mucosal as well as systemic immunity. Particles based on envelope, membrane or nucleocapsid microbial proteins induce a strong immune response after nasal or parenteral administration in mice, non-human primates and humans. In addition, the immune response obtained was modulated in a Th1 sense. The VLPs were also able to immunoenhance the humoral and cellular immune responses against several viral pathogens. Studies in animals and humans with nasal and systemic formulations evidenced that it is possible to induce functional immune response against HBV, HCV, HIV and dengue virus.

Translated Description (French)

The existing vaccines are mainly limited to the microorganisms we are able to culture and produce and/or to those whose killing is mediated by humoral response (antibody mediated). It has been more difficult to develop vaccines capable of inducing a functional cellular response needed to prevent or cura chronic diseases. New strategies should be taken into account in the improvement of cell-based immune responses in order to prevent and control the infections and eventually clear the virus. Preclinical and clinical results with vaccine candidates developed as a vaccine platform based on virus-like particles (VLPs) evidenced their ability to stimulate mucosal as well as systemic immunity. Particles based on enveloppe, membrane or nucleocapsid microbial proteins induit strong immune response after nasal or parenteral administration in mice, non-human primates and humans. En outre, la réponse immunitaire a été modulée dans un sens Th1. The VLPs were also able to immunoenhance the humoral and cellular immune responses against several viral pathogens. Etudes in animals and humans with nasal and systemic formulations evidenced that it possible to induce functional immune response against HBV, HCV, HIV and dengue virus.

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Additional details

Additional titles

Translated title (Arabic)
جزيئات شبيهة بالفيروسات كمرشحين للقاح النانو
Translated title (English)
Virus-like particles as nanovaccine candidates
Translated title (French)
Virus-like particles as nanovaccines candidates

Identifiers

Other
https://openalex.org/W1995750797
DOI
10.1088/2043-6262/4/1/015005

Is supplement to
https://openalex.org/W573847062 (Other)
https://openalex.org/W4381570565 (Other)
https://openalex.org/W4307359803 (Other)
https://openalex.org/W4302757063 (Other)
https://openalex.org/W2909757564 (Other)
https://openalex.org/W2478580149 (Other)
https://openalex.org/W2164219360 (Other)
https://openalex.org/W2045024356 (Other)
https://openalex.org/W2031253481 (Other)
https://openalex.org/W1964985474 (Other)

GreSIS Basics Section

Is Global South Knowledge
Yes
Country
Cuba

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