FML vaccine against canine visceral leishmaniasis: from second-generation to synthetic vaccine

Palatnik-de-Sousa, Clarisa B.; Barbosa, André de Figueiredo; Oliveira, Sandra Maria de; Nico, Dirlei; Bernardo, Robson Ronney; Santos, Wania Renata dos; Rodrigues, Maurício M.; Soares, Irene da Silva; Borja-Cabrera, G.P.

doi:10.1586/14760584.7.6.833

Cited by 44 publications

(61 citation statements)

References 110 publications

(155 reference statements)

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“…F3 is then the target of the anti- Leishmania cross-specific humoral response of mice (48), and the antibody target of humans and dogs with VL (49) and of dogs vaccinated with Leishmune ® (17). Since the antibodies generated by the Leishmune ® vaccine in dogs reacted mostly with the F3 epitopes (48) and block the transmission of VL in the insect vector (18, 19), the identification of these cross-reactive immunogenic sequences in F3 might also help in blocking the transmission of CL.…”

Section: Discussionmentioning

confidence: 99%

“…Consequently, we believe that the search for cross-protective antigens is mandatory. Recently, we developed the first licensed second generation vaccine against canine VL leishmaniasis (Leishmune ® ), which contains the fucose–mannose ligand (FML) antigen of L. donovani in formulation with saponin (16–19), is a transmission blocking vaccine (18, 19) and has already determined a reduction in the incidence of the human and canine disease in Brazilian endemic areas (20). Prophylactic vaccination of dogs with Leishmune ® promoted increases in the production of NO, IgG2 antibodies against FML and L. chagasi , intradermal reactions and proportions of CD8 + lymphocytes, which secrete more IFN-γ than IL-4 (21, 22) expressing a selective pro-inflammatory pattern (IFN-γ/NO) (23).…”

Section: Introductionmentioning

confidence: 99%

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Leishmania donovani Nucleoside Hydrolase Terminal Domains in Cross-Protective Immunotherapy Against Leishmania amazonensis Murine Infection

et al. 2014

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Nucleoside hydrolases of the Leishmania genus are vital enzymes for the replication of the DNA and conserved phylogenetic markers of the parasites. Leishmania donovani nucleoside hydrolase (NH36) induced a main CD4+ T cell driven protective response against L. chagasi infection in mice which is directed against its C-terminal domain. In this study, we used the three recombinant domains of NH36: N-terminal domain (F1, amino acids 1–103), central domain (F2 aminoacids 104–198), and C-terminal domain (F3 amino acids 199–314) in combination with saponin and assayed their immunotherapeutic effect on Balb/c mice previously infected with L. amazonensis. We identified that the F1 and F3 peptides determined strong cross-immunotherapeutic effects, reducing the size of footpad lesions to 48 and 64%, and the parasite load in footpads to 82.6 and 81%, respectively. The F3 peptide induced the strongest anti-NH36 antibody response and intradermal response (IDR) against L. amazonenis and a high secretion of IFN-γ and TNF-α with reduced levels of IL-10. The F1 vaccine, induced similar increases of IgG2b antibodies and IFN-γ and TNF-α levels, but no IDR and no reduction of IL-10. The multiparameter flow cytometry analysis was used to assess the immune response after immunotherapy and disclosed that the degree of the immunotherapeutic effect is predicted by the frequencies of the CD4+ and CD8+ T cells producing IL-2 or TNF-α or both. Total frequencies and frequencies of double-cytokine CD4 T cell producers were enhanced by F1 and F3 vaccines. Collectively, our multifunctional analysis disclosed that immunotherapeutic protection improved as the CD4 responses progressed from 1+ to 2+, in the case of the F1 and F3 vaccines, and as the CD8 responses changed qualitatively from 1+ to 3+, mainly in the case of the F1 vaccine, providing new correlates of immunotherapeutic protection against cutaneous leishmaniasis in mice based on T-helper TH1 and CD8+ mediated immune responses.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Leishmania donovani Nucleoside Hydrolase Terminal Domains in Cross-Protective Immunotherapy Against Leishmania amazonensis Murine Infection

et al. 2014

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“…Various studies have been carried out in dogs using FML antigen in combination with saponin as an adjuvant and encouraging results have been observed in almost all cases [161][162][163][164][165][166]. Vaccination with FML antigen conferred effective protection with increased level of IgG2a and 79-100% delayed type hypersensitivity (DTH) response in experimentally infected [163] and naturally exposed dogs [161].…”

Section: Fmlmentioning

confidence: 99%

“…Its gp36 glycoprotein, identified as a main component of FML, was specifically recognized by sera of rabbit [131] and used as a marker in human patients [155,166]. The use of GP36 in immunization also induced a strong and specific protection against L. donovani infection [160].…”

Section: Fmlmentioning

confidence: 99%

Vaccine candidates for leishmaniasis: A review

Nagill

Kaur

2011

International Immunopharmacology

108

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“…In Europe, there are two veterinary vaccines, one composed of the 54 kDa native excreted/secreted protein (Canileish) (6) and the other a chimera recombinant multiprotein protein Q, which contains the acidic ribosomal proteins Lip2a, Lip2b, P0, and histone H2A (7) (Latifend). In Brazil, the FML glycoprotein extract of L. (L.) donovani (Leishmune ® ) (8–11) was the first commercial vaccine in the world licensed in 2003. After that, the A2 recombinant protein of L. (L.) infantum chagasi (Leish-Tec ® ) (12) was also licensed in Brazil, in 2007 (13).…”

Section: Introductionmentioning

confidence: 99%

F1 Domain of the Leishmania (Leishmania) donovani Nucleoside Hydrolase Promotes a Th1 Response in Leishmania (Leishmania) infantum Cured Patients and in Asymptomatic Individuals Living in an Endemic Area of Leishmaniasis

et al. 2017

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The Leishmania (Leishmania) donovani nucleoside hydrolase NH36 is the main antigen of the Leishmune® vaccine and one of the promising candidates for vaccination against visceral leishmaniasis. The antigenicity of the N-terminal (F1), the central (F2), or the C-terminal recombinant domain (F3) of NH36 was evaluated using peripheral blood mononuclear cells (PBMC) from individuals infected with L. (L.) infantum from an endemic area of visceral leishmaniasis of Spain. Both NH36 and F1 domains significantly increased the PBMC proliferation stimulation index of cured patients and infected asymptomatic individuals compared to healthy controls. Moreover, F1 induced a 19% higher proliferative response than NH36 in asymptomatic exposed subjects. In addition, in patients cured from visceral leishmaniasis, proliferation in response to NH36 and F1 was accompanied by a significant increase of IFN-γ and TNF-α secretion, which was 42–43% higher, in response to F1 than to NH36. The interleukin 17 (IL-17) secretion was stronger in asymptomatic subjects, in response to F1, as well as in cured cutaneous leishmaniasis after NH36 stimulation. While no IL-10 secretion was determined by F1, a granzyme B increase was detected in supernatants from cured patients after stimulation with either NH36 or F1. These data demonstrate that F1 is the domain of NH36 that induces a recall cellular response in individuals with acquired resistance to the infection by L. (L.) infantum. In addition, F1 and NH36 discriminated the IgG3 humoral response in patients with active visceral leishmaniasis due to L. (L.) donovani (Ethiopia) and L. (L.) infantum (Spain) from that of endemic and non-endemic area controls. NH36 showed higher reactivity with sera from L. (L.) donovani-infected individuals, indicating species specificity. We conclude that the F1 domain, previously characterized as an inducer of the Th1 and Th17 responses in cured/exposed patients infected with L. (L.) infantum chagasi, may also be involved in the generation of a protective response against L. (L.) infantum and represents a potential vaccine candidate for the control of human leishmaniasis alone, or in combination with other HLA epitopes/antigens.

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FML vaccine against canine visceral leishmaniasis: from second-generation to synthetic vaccine

Cited by 44 publications

References 110 publications

Leishmania donovani Nucleoside Hydrolase Terminal Domains in Cross-Protective Immunotherapy Against Leishmania amazonensis Murine Infection

Leishmania donovani Nucleoside Hydrolase Terminal Domains in Cross-Protective Immunotherapy Against Leishmania amazonensis Murine Infection

Vaccine candidates for leishmaniasis: A review

F1 Domain of the Leishmania (Leishmania) donovani Nucleoside Hydrolase Promotes a Th1 Response in Leishmania (Leishmania) infantum Cured Patients and in Asymptomatic Individuals Living in an Endemic Area of Leishmaniasis

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