Literature DB >> 22247289

Enhancing humoral responses to a malaria antigen with nanoparticle vaccines that expand Tfh cells and promote germinal center induction.

James J Moon1, Heikyung Suh, Adrienne V Li, Christian F Ockenhouse, Anjali Yadava, Darrell J Irvine.   

Abstract

For subunit vaccines, adjuvants play a key role in shaping immunological memory. Nanoparticle (NP) delivery systems for antigens and/or molecular danger signals are promising adjuvants capable of promoting both cellular and humoral immune responses, but in most cases the mechanisms of action of these materials are poorly understood. Here, we studied the immune response elicited by NPs composed of multilamellar "stapled" lipid vesicles carrying a recombinant Plasmodium vivax circumsporozoite antigen, VMP001, both entrapped in the aqueous core and anchored to the lipid bilayer surfaces. Immunization with these particles and monophosphoryl lipid A (MPLA), a US Food and Drug Administration-approved immunostimulatory agonist for Toll-like receptor-4, promoted high-titer, high-avidity antibody responses against VMP001, lasting more than 1 y in mice at 10-fold lower doses than conventional adjuvants. Compared to soluble VMP001 mixed with MPLA, VMP001-NPs promoted broader humoral responses, targeting multiple epitopes of the protein and a more balanced Th1/Th2 cytokine profile from antigen-specific T cells. To begin to understand the underlying mechanisms, we examined components of the B-cell response and found that NPs promoted robust germinal center (GC) formation at low doses of antigen where no GC induction occurred with soluble protein immunization, and that GCs nucleated near depots of NPs accumulating in the draining lymph nodes over time. In parallel, NP vaccination enhanced the expansion of antigen-specific follicular helper T cells (T(fh)), compared to vaccinations with soluble VMP001 or alum. Thus, NP vaccines may be a promising strategy to enhance the durability, breadth, and potency of humoral immunity by enhancing key elements of the B-cell response.

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Year:  2012        PMID: 22247289      PMCID: PMC3268296          DOI: 10.1073/pnas.1112648109

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  30 in total

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Journal:  Immunity       Date:  2010-08-05       Impact factor: 31.745

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4.  Enhanced resistance to coxsackievirus B3-induced myocarditis by intranasal co-immunization of lymphotactin gene encapsulated in chitosan particle.

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Review 5.  Vivax malaria: neglected and not benign.

Authors:  Ric N Price; Emiliana Tjitra; Carlos A Guerra; Shunmay Yeung; Nicholas J White; Nicholas M Anstey
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Review 6.  The development of the RTS,S malaria vaccine candidate: challenges and lessons.

Authors:  W R Ballou
Journal:  Parasite Immunol       Date:  2009-09       Impact factor: 2.280

Review 7.  Key gaps in the knowledge of Plasmodium vivax, a neglected human malaria parasite.

Authors:  Ivo Mueller; Mary R Galinski; J Kevin Baird; Jane M Carlton; Dhanpat K Kochar; Pedro L Alonso; Hernando A del Portillo
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8.  Process development for the production of an E. coli produced clinical grade recombinant malaria vaccine for Plasmodium vivax.

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9.  Interbilayer-crosslinked multilamellar vesicles as synthetic vaccines for potent humoral and cellular immune responses.

Authors:  James J Moon; Heikyung Suh; Anna Bershteyn; Matthias T Stephan; Haipeng Liu; Bonnie Huang; Mashaal Sohail; Samantha Luo; Soong Ho Um; Htet Khant; Jessica T Goodwin; Jenelyn Ramos; Wah Chiu; Darrell J Irvine
Journal:  Nat Mater       Date:  2011-02-20       Impact factor: 43.841

10.  Follicular B helper T cells express CXC chemokine receptor 5, localize to B cell follicles, and support immunoglobulin production.

Authors:  D Breitfeld; L Ohl; E Kremmer; J Ellwart; F Sallusto; M Lipp; R Förster
Journal:  J Exp Med       Date:  2000-12-04       Impact factor: 14.307

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  138 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2012-01-17       Impact factor: 11.205

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3.  Covalent modification of cell surfaces with TLR agonists improves & directs immune stimulation.

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6.  Nanoparticulate STING agonists are potent lymph node-targeted vaccine adjuvants.

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7.  Biomaterials at the interface of nano- and micro-scale vector-cellular interactions in genetic vaccine design.

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Review 9.  Applications of nanomaterials as vaccine adjuvants.

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Review 10.  Biomimetic and synthetic interfaces to tune immune responses.

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