Long synthetic peptides encompassing thePlasmodium falciparum LSA3 are the target of human B and T cells and are potent inducers of B helper, T helper and cytolytic T cell responses in mice

Autor:	Blanca Liliana Perlaza, Jean-Pierre Sauzet, Karima Brahimi, Giampietro Corradin, Aissatou Toure Balde, Pierre Druilhe, Adama Tall
Rok vydání:	2001
Předmět:	Antigenicity T cell Immunology Biology Virology Molecular biology Epitope Interleukin 21 medicine.anatomical_structure Epitope mapping Antigen parasitic diseases medicine Immunology and Allergy Cytotoxic T cell Antigen-presenting cell
Zdroj:	European Journal of Immunology. 31:2200-2209
ISSN:	1521-4141 0014-2980 1026-1095
Popis:	We synthesized 17 long synthetic peptides (LSP) spanning the whole 200-kDa Plasmodium falciparum liver stage antigen-3 (LSA3), an antigen that induces protection in chimpanzee, and analyzed their immunogenicity in BALB/c mice and their antigenicity in individuals living in a hyper-endemic malaria area. Our findings show that both specific antibodies and T cell proliferation against most LSA3-LSP develop in malaria-exposed adults. All individuals studied had detectable antibodies against a minimum of 6 and a maximum of 15 polypeptides. It is noteworthy that antibody prevalence and titers were as high against non-repeat as repeat regions. Although the extent of T cell reactivity was lower than that observed for B cells, most of the sequences contained at least one T helper epitope, indicating that the majority of LSA3-LSP contain both B and T cell epitopes within the same sequence. Injection of LSA3-LSP with SBSA2 adjuvant in mice, showed strong immunogenicity for most of them, eliciting both T cell responses and specific antibody production. While all the peptides were immunogenic for B cells, different patterns of T cell responses were induced. These peptides were thus classified in three sets according to the levels of the T cell proliferative and of the IFN-gamma-specific responses. Importantly, antibodies and T cells against some of the LSP were able to recognize LSA3 native protein on P. falciparum sporozoites. Additionally, some LSP (44-119, 1026-1095, 1601-1712) also contained epitopes recognized by H-2(d) class I-restricted T cells. These results led to the identification of numerous domains that are highly antigenic and immunogenic within the LSA3 protein, and underline the value of the LSP approach for vaccine development.
Databáze:	OpenAIRE
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