Induction of multifunctional broadly reactive T cell responses by a Plasmodium vivax circumsporozoite protein recombinant chimera

EmoryVaccineCenterYerkesNationalPrimateResearchCenter; LaboratoryofImmunoparasitologyOswaldoCruzInstitute; DepartmentofPathologyUniversityofMassachusettsMedicalSchoolDivisionofInfectiousDiseasesDepartmentofMedicine

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Induction of multifunctional broadly reactive T cell responses by a Plasmodium vivax circumsporozoite protein recombinant chimera

机译：间日疟原虫环孢子蛋白重组嵌合体诱导多功能广泛反应性 T 细胞反应

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Plasmodium vivax is the most widespread species of Plasmodium, causing up to 50 of the malaria cases occurring outside sub-Saharan Africa. An effective vaccine is essential for successful control and potential eradication. A well-characterized vaccine candidate is the circumsporozoite protein (CSP). Preclinical and clinical trials have shown that both antibodies and cellular immune responses have been correlated with protection induced by immunization with CSP. On the basis of our reported approach of developing chimeric Plasmodium yoelii proteins to enhance protective efficacy, we designed PvRMC-CSP, a recombinant chimeric protein based on the P. vivax CSP (PvCSP). In this engineered protein, regions of the PvCSP predicted to contain human T cell epitopes were genetically fused to an immunodominant B cell epitope derived from the N-terminal region I and to repeat sequences representing the two types of PvCSP repeats. The chimeric protein was expressed in soluble form with high yield. As the immune response to PvCSP has been reported to be genetically restricted in the murine model, we tested the immunogenicity of PvRMC-CSP in groups of six inbred strains of mice. PvRMC-CSP was able to induce robust antibody responses in all the mouse strains tested. Synthetic peptides representing the allelic forms of the P. vivax CSP were also recognized to a similar extent regardless of the mouse strain. Furthermore, the immunization regimen induced high frequencies of multifunctional CD4+ and CD8+ PvRMC-CSP-specific T cells. The depth and breadth of the immune responses elicited suggest that immunization with PvRMC-CSP can circumvent the genetic restriction of the immune response to P. vivax CSP. Interestingly, PvRMC-CSP was also recognized by naturally acquired antibodies from individuals living in areas where malaria is endemic. These features make PvRMC-CSP a promising vaccine candidate for further development.

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《Infection and immunity.》 |2015年第9期|3749-3761|共13页
作者
EmoryVaccineCenterYerkesNationalPrimateResearchCenter; LaboratoryofImmunoparasitologyOswaldoCruzInstitute; DepartmentofPathologyUniversityofMassachusettsMedicalSchoolDivisionofInfectiousDiseasesDepartmentofMedicine;
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作者单位

Emory University, Atlanta, GA, United States;

Oswaldo Cruz Foundation (FIOCRUZ), Rio de Janeiro, RJ, Brazil;

Worcester, MA, United States;

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原文格式 PDF
正文语种英语
中图分类传染病;
关键词
Apoptosis; Autophagy; Cachexia; Cell death; Muscle atrophy; Necrosis; Sarcopenia; Skeletal muscle;

机译：细胞凋亡;自噬;恶病质;细胞死亡;肌肉萎缩;坏死;肌肉减少症;骨骼肌;

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Induction of multifunctional broadly reactive T cell responses by a Plasmodium vivax circumsporozoite protein recombinant chimera

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