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Vacunación con las proteínas ácidas ribosomales de Leishmania infantum.Respuesta inmunològica y capacidad protectiva
Author
Iborra Martín, SalvadorEntity
UAM. Departamento de Biología Molecular; Centro de Biología Molecular Severo Ochoa (CBM)Date
2005-03-01Subjects
Leishmania Infantum-Tesis doctorales; Vacunas antivirales-Tesis doctorales; Inmunogenética-Tesis doctorales; Biología y Biomedicina / BiologíaNote
Tesis Doctoral inédita leída en la Universidad Autónoma de Madrid, Facultad de Ciencias, Departamento de Biología Molecular. Fecha de lectura: 01-03-2005Abstract
Despite the evidence of acquired irnrnunity and resistance to reinfection in
natural Leishmania hosts, suggesting that a vaccine is feasible, to date there is no
vaccine for hurnan leishrnaniasis.
Recent advances in the design of vaccines are based on rnolecularly defined
antigens obtained by recornbinant rnethodologies, the socalled 'second-generation
vaccines". In this study, we have tested rnolecularly defined vaccines based on the
acidic ribosornal proteins and the histones of Leishmania infantum. These molecules
have been described as relevant irnrnunogens for the host irnrnune systern during
infection with Leishmania (Requena et al., 2000). In addition, adrninistration of a
rnulticornponent protein containing the antigenic detenninants of sorne of these
proteins (LiP2a, LiP2b, LiPO and LiH2A), using live BCG as adjuvant, confers
protection in dogs against L. infantum infection (Molano et al., 2003).
Fintly. we have deterrnined that sorne of these antigens (LiPO. LiPZb, LiH2A
and LiH3). expressed as recornbinant proteins in bacteria, stirnulate the in vitro
proliferation of splenocytes and lyrnph node cells frorn naive rnice. This mitogenic
activity is correlated with a B cell activation and cytokine synthesis (11-6 and IFNy).
Secondly, probably related with the in viho effect. we present data showing that
the adrninistration of the acidic ribosornal proteins, in the absence of any added
adjuvant, induces a humoral response. The progressive switch frorn IgM to IgG afler
the protein boosting, suggests that these are conventional secondary humoral
responses requiring the participation of T cells. Since lgGl was the predorninant
isotype, we conclude that adrninistration of these proteins elicited a Th2 response.
Further, we analysed the adrninistration of these antigens as recornbinant proteins
adjuvated with irnmunostirnulatory CpG oligodeoxynucleotides (CpG ODN). We
detected an enhanced generation of lgG2a antibodies and synthesis of IFN-y following
in vitro stirnulation with each antigen. Thus, we rnay conclude that that CpG ODN
adjuvant is able to increase the Thl irnrnune response against these antigens. On the
other hand. DNA vaccinations with either the LiPO antigen ora rnixture of four plasrnids
encoding for the L. infantum histones were perfonned. It was dernonstrated that this
DNA vaccines prirned for a Thl irnrnune response. which was associated with the
induction of lgG2a antibodies and an antigen-specific production of IFN-y.
Further, we decided to test these vaccines in the rnurine rnodel of cutaneous
leishrnaniasis (CL). Effective prirnary irnrnunity against L. major in rnouse is known to
require IL-12dependent production of 1FN-y frorn CD4' T cells (Thl response), which
rnediates NOdependent killing by infected rnacrophages. We have dernonstrated that
the adrninistration of LiPO either as protein plus CpG ODN or as a DNA vaccine.
confers partial protection against cutaneous leishrnaniasis due to L. major in BALBlc
rnice. These rnice exhibited a more controlled lesions but finally, progressive infection
and pathology was observed. On the other hand, DNA vaccination with the rnixture of
the four plasmids encoding for the L. infantum histones protects BALBlc rnice against
CL due to L. major. ln addition, these rnice were protected against the progressive
infection and disease, which correlates with an absence of the Th2 response against
the parasite proteins.
A rnodel of CL in C57BU6 rnice, that more accurately reproduces the pathology
and transrnission of the hurnan disease, was used to better undentand the potency of
the LiPO-vaccines. We dernonstrated that these vaccines confer protection against L.
major infection. consisting of a reduction of the parasite nurnber in the infected ama
and alrnost an absence of dennal pathology that correlates well with a specific Thl
response.
Finally. the LiPO-DNA vaccine was tested in two models of VL: BALBIc rnice
and hamster infected with L. infantum. No protection was 0bse~edin these two
rnodels. in spite of the fact that, at least in BALBlc rnice. a Thl response was induced
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