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Dendritic cell engineered cTXN as new vaccine prospect against L. donovani.
Suman, Shashi S; Kumar, Akhilesh; Singh, Ashish K; Amit, Ajay; Topno, R K; Pandey, K; Das, V N R; Das, P; Ali, Vahab; Bimal, Sanjiva.
Afiliação
  • Suman SS; Department of Immunology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Kumar A; Department of Immunology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Singh AK; Department of Immunology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Amit A; Department of Forensic Science, Guru Ghasidas Vishwavidyalaya, Bilaspur (C.G.) 495009, India.
  • Topno RK; Department of Epidemiology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Pandey K; Department of Clinical Medicine, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Das VNR; Department of Clinical Medicine, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Das P; Department of Molecular Biology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Ali V; Department of Biochemistry, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India.
  • Bimal S; Department of Immunology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India. Electronic address: drsbimal24@yahoo.com.
Cytokine ; 145: 155208, 2021 09.
Article em En | MEDLINE | ID: mdl-32736961
Dendritic cells (DCs), as antigen-presenting cells, can reportedly be infected withLeishmaniaparasites and hence provide a better option to trigger T-cell primary immune responses and immunological memory. We consistently primed DCs during culture with purified recombinant cytosolic tryparedoxin (rcTXN) and then evaluated the vaccine prospect of presentation of rcTXN against VL in BALB/c mice. We reported earlier the immunogenic properties of cTXN antigen derived fromL. donovani when anti-cTXN antibody was detected in the sera of kala-azar patients. It was observed that cTXN antigen, when used as an immunogen with murine DCs acting as a vehicle, was able to induce complete protection against VL in an infected group of immunized mice. This vaccination triggered splenic macrophages to produce more IL-12 and GM-CSF, and restricted IL-10 release to a minimum in an immunized group of infected animals. Concomitant changes in T-cell responses against cTXN antigen were also noticed, which increased the release of protective cytokine-like IFN-γ under the influence of NF-κß in the indicated vaccinated group of animals. All cTXN-DCs-vaccinated BALB/c mice survived during the experimental period of 120 days. The results obtained in our study suggest that DCs primed with cTXN can be used as a vaccine prospect for the control of visceral leishmaniasis.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Leishmania donovani / Células Dendríticas / Vacinas contra Leishmaniose / Leishmaniose Visceral Limite: Animals Idioma: En Ano de publicação: 2021 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Leishmania donovani / Células Dendríticas / Vacinas contra Leishmaniose / Leishmaniose Visceral Limite: Animals Idioma: En Ano de publicação: 2021 Tipo de documento: Article