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Adaptive Immunity against Leishmania Nucleoside Hydrolase Maps Its C-Terminal Domain as the Target of the CD4+ T Cell–Driven Protective Response

Author: A Moreno
A Selvapandiyan
AP Taylor
C Parra-López
Carla Claser
CB Palatnik de Sousa
CB Palatnik de Sousa
CB Palatnik-de-Sousa
CB Palatnik-de-Sousa
CB Palatnik-de-Sousa
CB Palatnik-de-Sousa
CF Alves
Christian R. Engwerda
Clarisa B. Palatnik-de-Sousa
CS Guerra
D Nico
Dirlei Nico
DJ Kao
DJ Marciani
DM Santana
DN Gopaul
E Iovane
E Oliveira-Freitas
E Paraguai de Souza
E Sanchez-Robert
EA Coelho
EM Saraiva
F De Leonardis
FY Liew
GP Borja-Cabrera
GP Borja-Cabrera
Gulnara P. Borja-Cabrera
HW Murray
I Aguilar-Be
IL Mauricio
Irene da Silva Soares
J Lukes
J Scharfetsin
L Cui
L Manna
LO Carvalho
LOP Souza
Luiz R. Travassos
MA Al-Wabel
Marcos Palatnik
Mauricio Martins Rodrigues
PA Darrah
PC Melby
PP Manna
R Basu
R Gamboa-León
R Mitterbauer
R Pellé
R Phillips
RA Seder
RL Miller
S Bertholet
SJ Todd
VO da Silva
W Shi
WG Chalé-Balboa
WR Santos
Publication venue: Public Library of Science
Publication date: 01/01/2010
Field of study

Nucleoside hydrolases (NHs) show homology among parasite protozoa, fungi and bacteria. They are vital protagonists in the establishment of early infection and, therefore, are excellent candidates for the pathogen recognition by adaptive immune responses. Immune protection against NHs would prevent disease at the early infection of several pathogens. We have identified the domain of the NH of L. donovani (NH36) responsible for its immunogenicity and protective efficacy against murine visceral leishmaniasis (VL). Using recombinant generated peptides covering the whole NH36 sequence and saponin we demonstrate that protection against L. chagasi is related to its C-terminal domain (amino-acids 199–314) and is mediated mainly by a CD4+ T cell driven response with a lower contribution of CD8+ T cells. Immunization with this peptide exceeds in 36.73±12.33% the protective response induced by the cognate NH36 protein. Increases in IgM, IgG2a, IgG1 and IgG2b antibodies, CD4+ T cell proportions, IFN-γ secretion, ratios of IFN-γ/IL-10 producing CD4+ and CD8+ T cells and percents of antibody binding inhibition by synthetic predicted epitopes were detected in F3 vaccinated mice. The increases in DTH and in ratios of TNFα/IL-10 CD4+ producing cells were however the strong correlates of protection which was confirmed by in vivo depletion with monoclonal antibodies, algorithm predicted CD4 and CD8 epitopes and a pronounced decrease in parasite load (90.5–88.23%; p = 0.011) that was long-lasting. No decrease in parasite load was detected after vaccination with the N-domain of NH36, in spite of the induction of IFN-γ/IL-10 expression by CD4+ T cells after challenge. Both peptides reduced the size of footpad lesions, but only the C-domain reduced the parasite load of mice challenged with L. amazonensis. The identification of the target of the immune response to NH36 represents a basis for the rationale development of a bivalent vaccine against leishmaniasis and for multivalent vaccines against NHs-dependent pathogens

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Universidade de São Paulo